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    <title>An agnostic study of associations between ABO and RhD blood group and phenome-wide
      disease risk</title>
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      <article itemscope="" itemtype="http://schema.org/Article" data-itemscope="root">
        <h1 itemprop="headline">An agnostic study of associations between ABO and RhD blood group
          and phenome-wide disease risk</h1>
        <meta itemprop="image"
          content="https://via.placeholder.com/1200x714/dbdbdb/4a4a4a.png?text=An%20agnostic%20study%20of%20associations%20between%20ABO%20and%20RhD%20blood%20group%20and%20phenome-wide%20disease%20risk">
        <ol data-itemprop="authors">
          <li itemscope="" itemtype="http://schema.org/Person" itemprop="author">
            <meta itemprop="name" content="Torsten Dahlén"><span data-itemprop="givenNames"><span
                itemprop="givenName">Torsten</span></span><span data-itemprop="familyNames"><span
                itemprop="familyName">Dahlén</span></span><span data-itemprop="emails"><a
                itemprop="email"
                href="mailto:torsten.dahlen@ki.se">torsten.dahlen@ki.se</a></span><span
              data-itemprop="affiliations"><a itemprop="affiliation"
                href="#author-organization-1">1</a><a itemprop="affiliation"
                href="#author-organization-2">2</a></span>
          </li>
          <li itemscope="" itemtype="http://schema.org/Person" itemprop="author">
            <meta itemprop="name" content="Mark Clements"><span data-itemprop="givenNames"><span
                itemprop="givenName">Mark</span></span><span data-itemprop="familyNames"><span
                itemprop="familyName">Clements</span></span><span data-itemprop="affiliations"><a
                itemprop="affiliation" href="#author-organization-3">3</a></span>
          </li>
          <li itemscope="" itemtype="http://schema.org/Person" itemprop="author">
            <meta itemprop="name" content="Jingcheng Zhao"><span data-itemprop="givenNames"><span
                itemprop="givenName">Jingcheng</span></span><span data-itemprop="familyNames"><span
                itemprop="familyName">Zhao</span></span><span data-itemprop="affiliations"><a
                itemprop="affiliation" href="#author-organization-2">2</a></span>
          </li>
          <li itemscope="" itemtype="http://schema.org/Person" itemprop="author">
            <meta itemprop="name" content="Martin L Olsson"><span data-itemprop="givenNames"><span
                itemprop="givenName">Martin</span><span itemprop="givenName">L</span></span><span
              data-itemprop="familyNames"><span itemprop="familyName">Olsson</span></span><span
              data-itemprop="affiliations"><a itemprop="affiliation"
                href="#author-organization-4">4</a></span>
          </li>
          <li itemscope="" itemtype="http://schema.org/Person" itemprop="author">
            <meta itemprop="name" content="Gustaf Edgren"><span data-itemprop="givenNames"><span
                itemprop="givenName">Gustaf</span></span><span data-itemprop="familyNames"><span
                itemprop="familyName">Edgren</span></span><span data-itemprop="affiliations"><a
                itemprop="affiliation" href="#author-organization-2">2</a><a itemprop="affiliation"
                href="#author-organization-5">5</a></span>
          </li>
        </ol>
        <ol data-itemprop="affiliations">
          <li itemscope="" itemtype="http://schema.org/Organization" itemid="#author-organization-1"
            id="author-organization-1"><span itemprop="name">Hematology Department, Karolinska
              University Hospital</span><address itemscope=""
              itemtype="http://schema.org/PostalAddress" itemprop="address"><span
                itemprop="addressLocality">Stockholm</span><span
                itemprop="addressCountry">Sweden</span></address></li>
          <li itemscope="" itemtype="http://schema.org/Organization" itemid="#author-organization-2"
            id="author-organization-2"><span itemprop="name">Department of Medicine Solna, Clinical
              Epidemiology Division, Karolinska Institutet</span><address itemscope=""
              itemtype="http://schema.org/PostalAddress" itemprop="address"><span
                itemprop="addressLocality">Stockholm</span><span
                itemprop="addressCountry">Sweden</span></address></li>
          <li itemscope="" itemtype="http://schema.org/Organization" itemid="#author-organization-3"
            id="author-organization-3"><span itemprop="name">Department of Medical Epidemiology and
              Biostatistics, Karolinska Institutet</span><address itemscope=""
              itemtype="http://schema.org/PostalAddress" itemprop="address"><span
                itemprop="addressLocality">Stockholm</span><span
                itemprop="addressCountry">Sweden</span></address></li>
          <li itemscope="" itemtype="http://schema.org/Organization" itemid="#author-organization-4"
            id="author-organization-4"><span itemprop="name">Division of Hematology and Transfusion
              Medicine, Department of Laboratory Medicine, Lund University &amp; Department of
              Clinical Immunology and Transfusion Medicine, Office of Medical Services, Region
              Skåne</span><address itemscope="" itemtype="http://schema.org/PostalAddress"
              itemprop="address"><span itemprop="addressLocality">Lund</span><span
                itemprop="addressCountry">Sweden</span></address></li>
          <li itemscope="" itemtype="http://schema.org/Organization" itemid="#author-organization-5"
            id="author-organization-5"><span itemprop="name">Cardiology Department,
              Södersjukhuset</span><address itemscope="" itemtype="http://schema.org/PostalAddress"
              itemprop="address"><span itemprop="addressLocality">Stockholm</span><span
                itemprop="addressCountry">Sweden</span></address></li>
        </ol><span itemscope="" itemtype="http://schema.org/Organization" itemprop="publisher">
          <meta itemprop="name" content="Unknown"><span itemscope=""
            itemtype="http://schema.org/ImageObject" itemprop="logo">
            <meta itemprop="url"
              content="https://via.placeholder.com/600x60/dbdbdb/4a4a4a.png?text=Unknown">
          </span>
        </span><time itemprop="datePublished" datetime="2021-04-27">2021-04-27</time>
        <ul data-itemprop="genre">
          <li itemprop="genre">Research Article</li>
        </ul>
        <ul data-itemprop="about">
          <li itemscope="" itemtype="http://schema.org/DefinedTerm" itemprop="about"><span
              itemprop="name">Epidemiology and Global Health</span></li>
          <li itemscope="" itemtype="http://schema.org/DefinedTerm" itemprop="about"><span
              itemprop="name">Medicine</span></li>
        </ul>
        <ul data-itemprop="keywords">
          <li itemprop="keywords">ABO blood group</li>
          <li itemprop="keywords">RhD blood group</li>
          <li itemprop="keywords">agnostic</li>
          <li itemprop="keywords">all disease</li>
          <li itemprop="keywords">None</li>
        </ul>
        <ul data-itemprop="identifiers">
          <li itemscope="" itemtype="http://schema.org/PropertyValue" itemprop="identifier">
            <meta itemprop="propertyID"
              content="https://registry.identifiers.org/registry/publisher-id"><span
              itemprop="name">publisher-id</span><span itemprop="value"
              data-itemtype="http://schema.org/Number">65658</span>
          </li>
          <li itemscope="" itemtype="http://schema.org/PropertyValue" itemprop="identifier">
            <meta itemprop="propertyID" content="https://registry.identifiers.org/registry/doi">
            <span itemprop="name">doi</span><span itemprop="value">10.7554/eLife.65658</span>
          </li>
          <li itemscope="" itemtype="http://schema.org/PropertyValue" itemprop="identifier">
            <meta itemprop="propertyID"
              content="https://registry.identifiers.org/registry/elocation-id"><span
              itemprop="name">elocation-id</span><span itemprop="value">e65658</span>
          </li>
        </ul>
        <section data-itemprop="description">
          <h2 data-itemtype="http://schema.stenci.la/Heading">Abstract</h2>
          <meta itemprop="description"
            content="Background: There are multiple known associations between the ABO and RhD blood groups and disease. No systematic population-based studies elucidating associations between a large number of disease categories and blood group have been conducted. Methods: Using SCANDAT3-S, a comprehensive nationwide blood donation-transfusion database, we modeled outcomes for 1217 disease categories including 70 million person-years of follow-up, accruing from 5.1 million individuals. Results: We discovered 49 and 1 associations between a disease and ABO and RhD blood groups, respectively, after adjustment for multiple testing. We identified new associations such as a decreased risk of kidney stones and blood group B as compared to blood group O. We also expanded previous knowledge on other associations such as pregnancy-induced hypertension and blood groups A and AB as compared to blood group O and RhD positive as compared to negative. Conclusions: Our findings generate strong further support for previously known associations, but also indicate new interesting relations. Funding: Swedish Research Council.">
          <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Background: There are
            multiple known associations between the ABO and RhD blood groups and disease. No
            systematic population-based studies elucidating associations between a large number of
            disease categories and blood group have been conducted.</p>
          <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Methods: Using SCANDAT3-S, a
            comprehensive nationwide blood donation-transfusion database, we modeled outcomes for
            1217 disease categories including 70 million person-years of follow-up, accruing from
            5.1 million individuals.</p>
          <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Results: We discovered 49 and
            1 associations between a disease and ABO and RhD blood groups, respectively, after
            adjustment for multiple testing. We identified new associations such as a decreased risk
            of kidney stones and blood group B as compared to blood group O. We also expanded
            previous knowledge on other associations such as pregnancy-induced hypertension and
            blood groups A and AB as compared to blood group O and RhD positive as compared to
            negative.</p>
          <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Conclusions: Our findings
            generate strong further support for previously known associations, but also indicate new
            interesting relations.</p>
          <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Funding: Swedish Research
            Council.</p>
        </section>
        <h2 itemscope="" itemtype="http://schema.stenci.la/Heading" id="introduction">Introduction
        </h2>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">The blood group antigens of the
          ABO and RhD systems play a pivotal role in transfusion medicine because of their role in
          the safe administration of blood transfusions. In addition, these cell surface antigens
          have been demonstrated to have direct effects on the susceptibility for several diseases
          <span itemscope="" itemtype="http://schema.stenci.la/CiteGroup"><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib9"><span>9</span><span>Franchini
                  et al.</span><span>2012</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib23"><span>23</span><span>Stowell
                  and Stowell</span><span>2019</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib24"><span>24</span><span>Stowell
                  and Stowell</span><span>2019</span></a></cite></span>. One of the first such
          studies was published in 1962, demonstrating a relationship between the ABO system and
          ischemic heart disease <cite itemscope="" itemtype="http://schema.stenci.la/Cite"><a
              href="#bib3"><span>3</span><span>Bronte-Stewart et
                al.</span><span>1962</span></a></cite>. Multiple subsequent studies have revealed
          associations with a range of diseases, with a prominent example being a decreased risk of
          thromboembolic events and increased risks of some hemorrhagic events in individuals with
          blood group O <span itemscope="" itemtype="http://schema.stenci.la/CiteGroup"><cite
              itemscope="" itemtype="http://schema.stenci.la/Cite"><a
                href="#bib9"><span>9</span><span>Franchini et
                  al.</span><span>2012</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib8"><span>8</span><span>Edgren et
                  al.</span><span>2010</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib27"><span>27</span><span>Vasan et
                  al.</span><span>2016</span></a></cite></span>. The difference in thrombotic and
          hemorrhagic phenotypes has been attributed to variability in levels of <em itemscope=""
            itemtype="http://schema.stenci.la/Emphasis">Factor VIII</em> and <em itemscope=""
            itemtype="http://schema.stenci.la/Emphasis">von Willebrand factor</em>, where ABO status
          may explain as much as 30% of this variability <span itemscope=""
            itemtype="http://schema.stenci.la/CiteGroup"><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib9"><span>9</span><span>Franchini
                  et al.</span><span>2012</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib19"><span>19</span><span>Orstavik
                  et al.</span><span>1985</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib12"><span>12</span><span>Germain
                  et al.</span><span>2015</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a
                href="#bib16"><span>16</span><span>Lindström et
                  al.</span><span>2019</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a
                href="#bib18"><span>18</span><span>O'Donnell et
                  al.</span><span>2002</span></a></cite></span> Other prominent examples include
          associations with risks of a number of infectious diseases, to the extent that the allele
          distribution of the blood group antigens has evolved to reflect some areas endemic to
          these infectious diseases <cite itemscope="" itemtype="http://schema.stenci.la/Cite"><a
              href="#bib11"><span>11</span><span>Franchini and
                Bonfanti</span><span>2015</span></a></cite>. This is in part true for infectious
          disease such as <em itemscope="" itemtype="http://schema.stenci.la/Emphasis">Plasmodium
            falciparum</em> malaria, <em itemscope=""
            itemtype="http://schema.stenci.la/Emphasis">Helicobacter pylori</em>, and <em
            itemscope="" itemtype="http://schema.stenci.la/Emphasis">Vibrio cholera</em>, where ABO
          blood groups are involved in different aspects of pathogenesis, from microbe attachment
          and entry into cells to subsequent disease development and severity of disease <span
            itemscope="" itemtype="http://schema.stenci.la/CiteGroup"><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib23"><span>23</span><span>Stowell
                  and Stowell</span><span>2019</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a
                href="#bib11"><span>11</span><span>Franchini and
                  Bonfanti</span><span>2015</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib6"><span>6</span><span>Cserti and
                  Dzik</span><span>2007</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib7"><span>7</span><span>Degarege
                  et al.</span><span>2019</span></a></cite></span>. Surface antigens of the ABO
          blood groups are defined by the immunodominant, terminal sugar residues on certain
          glycolipids and glycoproteins anchored to the membrane of red blood cells and exposed
          extracellularly. Even if expressed from a single-gene locus, the <em itemscope=""
            itemtype="http://schema.stenci.la/Emphasis">ABO</em> gene on chromosome 9, A and B
          antigens are present not only on erythroid cells but also in many other tissues, and due
          to the diverse tissue, expression may result in differences in disease occurrence <cite
            itemscope="" itemtype="http://schema.stenci.la/Cite"><a
              href="#bib13"><span>13</span><span>Harmening</span><span>2012</span></a></cite>. The
          <em itemscope="" itemtype="http://schema.stenci.la/Emphasis">A</em> and <em itemscope=""
            itemtype="http://schema.stenci.la/Emphasis">B</em> allelic variants of the <em
            itemscope="" itemtype="http://schema.stenci.la/Emphasis">ABO</em> locus encode the A and
          B glycosyltransferases, which differ only by a few amino acid residues, add the donor
          substrates UDP-<em itemscope=""
            itemtype="http://schema.stenci.la/Emphasis">N</em>-acetylgalactosamine or UDP-galactose,
          respectively, to a common acceptor substrate, namely a carbohydrate chain terminating with
          the so-called H antigen, in turn dependent on fucosyltransferase activity expressed from
          the <em itemscope="" itemtype="http://schema.stenci.la/Emphasis">FUT1</em> and <em
            itemscope="" itemtype="http://schema.stenci.la/Emphasis">FUT2</em> genes on chromosome
          19. In blood group O, the H antigen is left unaltered due to lack of ABO enzyme activity,
          most commonly by a single-nucleotide deletion in the <em itemscope=""
            itemtype="http://schema.stenci.la/Emphasis">ABO</em> coding region <cite itemscope=""
            itemtype="http://schema.stenci.la/Cite"><a href="#bib22"><span>22</span><span>Storry and
                Olsson</span><span>2009</span></a></cite>.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">The RhD antigen, on the other
          hand, has a less clear link to health outcomes. RhD status has mainly been linked to
          alloimmunization of the pregnant women with hemolytic disease of the fetus and newborn as
          a consequence <cite itemscope="" itemtype="http://schema.stenci.la/Cite"><a
              href="#bib25"><span>25</span><span>Urbaniak and
                Greiss</span><span>2000</span></a></cite>. Beyond these direct effects, little is
          known about its role in disease pathogenesis. The difference between RhD-positive and
          -negative blood group is the presence or absence of the RhD protein on the red blood cell
          surface. However, both individuals with and without RhD possess the homologous RhCE
          protein and Rh-associated glycoprotein (RhAG) on their red cells. Thus, functions carried
          out by RhD are likely performed RhCE and RhAG in RhD-negative individuals, and this
          redundancy may in part explain the scarcity of findings related to RhD status <cite
            itemscope="" itemtype="http://schema.stenci.la/Cite"><a
              href="#bib1"><span>1</span><span>Avent and Reid</span><span>2000</span></a></cite>.
        </p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Using the Scandinavian Donation
          and Transfusion (SCANDAT) database, we have previously studied associations between ABO
          blood groups and cancer subtypes, cardiovascular and thromboembolic disease, the
          occurrence of dementia and degradation of bioprosthetic aortic valves in relation to ABO
          blood group <span itemscope="" itemtype="http://schema.stenci.la/CiteGroup"><cite
              itemscope="" itemtype="http://schema.stenci.la/Cite"><a
                href="#bib27"><span>27</span><span>Vasan et
                  al.</span><span>2016</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib20"><span>20</span><span>Persson
                  et al.</span><span>2019</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib28"><span>28</span><span>Vasan et
                  al.</span><span>2016</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib26"><span>26</span><span>Vasan et
                  al.</span><span>2015</span></a></cite></span>. However, these and most other prior
          studies into the association between ABO blood group and disease outcomes have been
          limited by potentially misdirected a priori hypotheses and phenome-wide disease
          associations have not been thoroughly explored in a systematic manner. Therefore, in the
          current study, we aimed to agnostically investigate the association between ABO and RhD
          blood group and disease occurrence for a large number of disease phenotypes using
          large-scale population-based Swedish healthcare registries.</p>
        <h2 itemscope="" itemtype="http://schema.stenci.la/Heading" id="materials-and-methods">
          Materials and methods</h2>
        <h3 itemscope="" itemtype="http://schema.stenci.la/Heading"
          id="study-population-and-study-design">Study population and study design</h3>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Individuals in the study were
          identified using an updated version of the Scandinavian donations and transfusion database
          (SCANDAT3-S). This database includes close to 8 million individuals who have donated
          blood, received a blood transfusion, or have had blood group testing done for other
          reasons. Other reasons for blood group testing would typically be pre-emptive testing
          for example, before surgery or in antenatal care. The database contains detailed
          information on blood donations, transfusions, as well as blood group antigen and antibody
          testing results and is thoroughly described elsewhere <cite itemscope=""
            itemtype="http://schema.stenci.la/Cite"><a href="#bib29"><span>29</span><span>Zhao et
                al.</span><span>2020</span></a></cite>. It is nationally complete since 1995, but
          information dates back to 1968 with various levels of completeness, mainly depending on
          the geographical region. Using unique national registration numbers assigned to all
          inhabitants of Sweden, the SCANDAT3-S database has been linked to a range of national
          health outcomes registers, for hospital care, cancer, cause of death, and drug
          prescriptions . From SCANDAT3-S, we extracted information on ABO and RhD blood group and
          created a main cohort and a validation cohort. The main cohort consisted of all
          individuals who were born in Sweden where at least one parent was born in Sweden and who,
          for any reason, had undergone ABO and RhD blood group typing with a conclusive result, but
          who did not donate blood within 90 days of the test. Person-time for blood donors were
          excluded from the main cohort to maximize the representativeness of the study population.
          In the validation cohort, we included all individuals in the SCANDAT3-S database who had
          ever donated blood. As such, an individual could contribute person-time in both cohorts,
          such as in the case a person started to donate blood more than 90 days later from a blood
          grouping test that was initially performed for other reasons. The person-time before blood
          donation would contribute to the main cohort censoring at entry in the validation cohort
          starting at the time of blood grouping before the blood donation.</p>
        <h3 itemscope="" itemtype="http://schema.stenci.la/Heading" id="outcomes">Outcomes</h3>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">We defined and studied a large
          number of disease categories. Non-cancer disease categories were based on discharge
          diagnoses from the national patient register, which covers all hospital inpatient care in
          Sweden since 1987 and all specialist outpatient care since 1997, and from the Cause of
          Death register, which records underlying causes of death for all persons in Sweden since
          1964 <span itemscope="" itemtype="http://schema.stenci.la/CiteGroup"><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib4"><span>4</span><span>Brooke et
                  al.</span><span>2017</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a
                href="#bib17"><span>17</span><span>Ludvigsson et
                  al.</span><span>2011</span></a></cite></span>. Because the 10th revision of the
          International Classification of Disease (ICD) was implemented in 1997, we limited outcomes
          ascertainment to events from 1997 or later to avoid inconsistencies between ICD revisions.
          Cancer outcomes were based on the Cancer Register, which records all incident cancer cases
          in Sweden since 1958 <cite itemscope="" itemtype="http://schema.stenci.la/Cite"><a
              href="#bib2"><span>2</span><span>Barlow et al.</span><span>2009</span></a></cite>. All
          of these registries are held and maintained by the Swedish National Board of Health and
          Welfare and have a high level of completeness and accuracy. Dates of death and emigration
          were obtained from population registers kept by Statistics Sweden.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Details of non-cancerous
          disease categories are presented in <a href="#supp3" itemscope=""
            itemtype="http://schema.stenci.la/Link">Supplementary file 3</a>. Non-cancer diseases
          were classified into disease categories based on the first three codes of the diagnosis,
          according to the ICD-10 codebook. We did not consider external causes of disease,
          traumatic injuries, or symptom-based codes as these were deemed unlikely to be related to
          blood group antigens. Cancer disease categories were based on anatomical coding using the
          7th revision of the ICD for all non-hematological malignancies and the 8th revision of the
          ICD for hematological malignancies. For details of cancer categories, see <a href="#supp4"
            itemscope="" itemtype="http://schema.stenci.la/Link">Supplementary file 4</a> (SAS code
          for cancer disease grouping is available upon request).</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">In total, we considered 1217
          distinct disease categories. After database construction, we excluded disease categories
          with fewer than 50 events before analysis as we would be unlikely to detect sufficient
          events in the validation cohort in categories with fewer than 50 events in the main
          cohort.</p>
        <h3 itemscope="" itemtype="http://schema.stenci.la/Heading" id="statistical-methods">
          Statistical methods</h3>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">All persons were followed from
          the date of the first blood grouping test, from their 18th birthday, or from January 1,
          1997, whichever occurred last. Follow-up was extended until the first incident event in
          each disease category, emigration, death or December 31, 2017, whichever occurred first. A
          person could thus be included in follow-up for all disease categories investigated.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Descriptive statistics were
          presented for cohort baseline data. For the main analysis, we used a Poisson regression
          model. In the model, we incorporated the following covariates: ABO blood group (A, AB, B
          or O), RhD status (weak or category expression variants were excluded), sex,
          calendar-period, and age. A restricted cubic spline functions with four or five knots
          placed according to Harrell’s method were applied to the age and calendar-period
          covariates <cite itemscope="" itemtype="http://schema.stenci.la/Cite"><a
              href="#bib14"><span>14</span><span>Harrell</span><span>2015</span></a></cite>. The
          regression model was fitted separately to each disease category resulting in incidence
          rate ratios (IRR) for each ABO blood group and RhD status using blood group O and RhD
          negative as reference, respectively. Wald’s method was used to construct 95% confidence
          intervals (CI). Equi-dispersion was tested using a Lagrange multiplier test. For disease
          categories where data demonstrated significant over- or under-dispersion after also
          performing the same analysis but reducing the number of knots from 5 to 4, analyses were
          instead run using quasi-Poisson regression.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Multiple testing was handled
          using a two-stage approach. First, in the exploratory analysis using the main cohort, we
          applied a false discovery rate (FDR) adjustment of raw p-values assuming positive
          dependency of stochastic ordering between outcomes. Second, in the confirmatory analysis
          using the validation cohort, we used the disease categories with significant effects from
          explorative analysis, with results presented both without adjustment and using a
          Bonferroni adjustment. In effect, this allowed us to limit type one errors presenting
          confirmed associations with high certainty, but still not to compromise type two errors
          for future confirmatory analysis in other cohorts.</p>
        <h2 itemscope="" itemtype="http://schema.stenci.la/Heading" id="results">Results</h2>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Characteristics of the main and
          validation cohorts are presented in <a href="#table1" itemscope=""
            itemtype="http://schema.stenci.la/Link">Table 1</a>. When combining the main and
          validation cohort, there were a total of 5.1 million unique individuals. The main cohort
          consisted of 4.2 million individuals who at any point had undertaken an ABO and RhD blood
          antigen test. The distribution of A, AB, B, and O were 47%, 5%, 10%, and 38%,
          respectively, and 84% of individuals were RhD positive. Women constituted 60% of the
          cohort. The median age at cohort entry was 52 years (interquartile range [IQR], 30–71) and
          the median year of birth was 1949 (IQR, 1931–1971).</p>
        <table id="table1" itemscope="" itemtype="http://schema.org/Table">
          <caption><label data-itemprop="label">Table 1.</label>
            <div itemprop="caption">
              <h3 itemscope="" itemtype="http://schema.stenci.la/Heading"
                id="baseline-characteristics-of-main-and-validation-cohort">Baseline characteristics
                of main and validation cohort.</h3>
            </div>
          </caption>
          <thead>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell">Main cohort</th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell">Validation cohort</th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
            </tr>
          </thead>
          <tbody>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Number</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">4,204,234</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1,197,522</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Age, median (IQR)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Age, median (IQR)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">52</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">(30-71)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">30</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">(23-41)</td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Year of birth, median
                (IQR)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">1949</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">(1931–1971)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">1966</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">(1953–1978)</td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Sex, %</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">60</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">49</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Blood group, %</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">A</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">47</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">45</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">AB</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">5</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">5</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">B</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">10</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">11</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">O</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">38</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">39</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">RhD positive, %</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">84</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">82</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
          </tbody>
        </table>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Not accounting for censoring
          due to disease events, the main cohort accrued a total of 49.9 million person-years of
          follow-up, 23.7 million in blood group A, 2.3 million in blood group AB, 4.9 million in
          blood group B, and 18.9 million in blood group O.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Of the original 1217 disease
          categories, 1090 remained available for analyses after excluding disease categories with
          fewer than 50 events. The median number of events per disease category in the main cohort
          was 4748 (IQR, 869–231,166). A meta-summary of results of regression analyses is presented
          in <a href="#table2" itemscope="" itemtype="http://schema.stenci.la/Link">Table 2</a>, and
          graphically in the form of a volcano plot in <a href="#fig1" itemscope=""
            itemtype="http://schema.stenci.la/Link">Figure 1</a> (also, as an interactive, online
          variant as <a href="#supp1" itemscope=""
            itemtype="http://schema.stenci.la/Link">Supplementary file 1</a>). Alternatively,
          results are also presented as an ICD chapter-based, variant Manhattan plot in <a
            href="#fig2" itemscope="" itemtype="http://schema.stenci.la/Link">Figure 2</a> (also as
          an interactive, online variant as <a href="#supp2" itemscope=""
            itemtype="http://schema.stenci.la/Link">Supplementary file 2</a>). Overall, in the main
          cohort and before FDR adjustment for multiple testing, there were 343 and 98 statistically
          significant associations for the ABO and RhD blood group systems and unique disease
          categories, respectively. Of these, a total of 143 (41%) and 13 (13%) associations between
          blood group and unique outcome remained statistically significant for ABO and RhD blood
          group systems, respectively, after FDR adjustment. For the ABO system, IRRs for
          statistically significant associations after FDR adjustment ranged from 0.57 to 0.99 for
          negative associations and from 1.01 to 1.52 for positive associations. For RhD status,
          IRRs ranged from 0.90 to 0.97 for negative associations and from 1.02 to 1.08 for positive
          associations. Details of all associations identified after FDR are presented in <a
            href="#supp5" itemscope="" itemtype="http://schema.stenci.la/Link">Supplementary file
            5</a> (for ABO blood groups) and <a href="#supp6" itemscope=""
            itemtype="http://schema.stenci.la/Link">Supplementary file 6</a> (for RhD).</p>
        <stencila-code-chunk itemscope="" itemtype="http://schema.stenci.la/CodeChunk"
          data-execution_count="1" data-programminglanguage="python">
          <pre class="language-python" itemscope="" itemtype="http://schema.stenci.la/CodeBlock"
            slot="text"><code>import numpy as np
import pandas as pd
import plotly.graph_objects as go
from plotly.subplots import make_subplots</code></pre>
        </stencila-code-chunk>
        <figure itemscope="" itemtype="http://schema.stenci.la/Figure" id="fig1" title="Figure 1.">
          <label data-itemprop="label">Figure 1.</label>
          <stencila-code-chunk itemscope="" itemtype="http://schema.stenci.la/CodeChunk"
            data-execution_count="2" data-programminglanguage="python">
            <pre class="language-python" itemscope="" itemtype="http://schema.stenci.la/CodeBlock"
              slot="text"><code>df = pd.read_csv(&#39;df.csv&#39;)
df_r = pd.read_csv(&#39;df_r.csv&#39;)
concordant = pd.read_csv(&#39;concordant.csv&#39;)

fig = go.Figure()
fdr_p=df[&#39;fdr_p&#39;]


grp=df[&#39;bg&#39;].unique().tolist()
for groups in grp:
        data_filtered=df[(df.bg==groups) &amp; (df.fdr_p &lt; 0.05)]
        fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=data_filtered[&#39;y&#39;], 
                         mode=&#39;markers&#39;,
                             opacity=0.5,
                         marker=dict(color=data_filtered[&#39;color&#39;],line=dict(color=&#39;white&#39;,width=0)),
                         text=data_filtered[&#39;bg_cat&#39;],
                         customdata=data_filtered[&#39;event_pyrs&#39;],
                         hovertext=data_filtered[&#39;fdr_p&#39;],
                        meta=data_filtered[&#39;combined&#39;],
                        hovertemplate = &quot;&lt;b&gt;%{text}&lt;/b&gt;&quot; +
                         &quot;&lt;br&gt;FDR-P: %{hovertext:,.2g}:&quot; +
                         #&quot;&lt;br&gt;IRR: %{marker.size:,.2f}&quot;+
                         &quot;&lt;br&gt;IRR (95% CI): %{meta}&quot; +
                         &quot;&lt;br&gt;Events/Person-years: %{customdata}&quot; +
                         &quot;&lt;extra&gt;&lt;/extra&gt;&quot;,
                         marker_size=(8*data_filtered[&#39;irr&#39;]),
                         name=groups
                        )
              )



df_r2=df_r[df_r.fdr_p&lt;0.05]
fig.add_trace(go.Scatter(x=df_r2[&#39;x&#39;], 
                         y=df_r2[&#39;y&#39;], 
                         mode=&#39;markers&#39;,
                             opacity=0.5,
                         marker=dict(color=df_r2[&#39;color&#39;],opacity=df_r2[&#39;opacity&#39;],line=dict(color=&#39;white&#39;,width=0)),
                         text=df_r2[&#39;bg_cat&#39;],
                         customdata=df_r2[&#39;event_pyrs&#39;],
                         hovertext=df_r2[&#39;fdr_p&#39;],
                        meta=df_r2[&#39;combined&#39;],
                        hovertemplate = &quot;&lt;b&gt;%{text}&lt;/b&gt;&quot; +
                         &quot;&lt;br&gt;FDR-P: %{hovertext:,.2g}:&quot; +
                         #&quot;&lt;br&gt;IRR: %{marker.size:,.2f}&quot;+
                         &quot;&lt;br&gt;IRR (95% CI): %{meta}&quot; +
                         &quot;&lt;br&gt;Events/Person-years: %{customdata}&quot; +
                         &quot;&lt;extra&gt;&lt;/extra&gt;&quot;,
                         marker_size=(8*df_r2[&#39;irr&#39;]),
                         name=&#39;RhD positive&#39;
                        )
              )
              
fig.add_trace(go.Scatter(x=pd.concat([df_r.x[(df_r.fdr_p&gt;=0.05)],df.x[(df.fdr_p&gt;=0.05)]]), 
                         y=pd.concat([df_r.y[(df_r.fdr_p&gt;=0.05)],df.y[(df.fdr_p&gt;=0.05)]]), 
                         mode=&#39;markers&#39;,
                             opacity=0.7,
                         marker=dict(color=pd.concat([df_r.color[(df_r.fdr_p&gt;=0.05)],df.color[(df.fdr_p&gt;=0.05)]]),opacity=0.7,line=dict(color=&#39;white&#39;,width=0)),
                         name=&#39;Non-significant ABO and RhD&#39;,
                         showlegend=True,
                        )
              )
    
    

fig.add_trace(go.Scatter(x=concordant.x, 
                         y=concordant.y, 
                         mode=&#39;markers&#39;,
                             opacity=0.8,
                         marker=dict(color=&#39;black&#39;,opacity=0.8,line=dict(color=&#39;white&#39;,width=0)),
                         text=concordant[&#39;bg_cat&#39;],
                         customdata=concordant[&#39;event_pyrs&#39;],
                         hovertext=concordant[&#39;pvalue&#39;],
                        meta=concordant[&#39;combined&#39;],
                        hovertemplate = &quot;&lt;b&gt;%{text}&lt;/b&gt;&quot; +
                         &quot;&lt;br&gt;P-value: %{hovertext:,.2g}:&quot; +
                         &quot;&lt;br&gt;IRR: %{marker.size:,.2f}&quot;+
                         &quot;&lt;br&gt;IRR (95% CI): %{meta}&quot; +
                         &quot;&lt;br&gt;Events/Person-years: %{customdata}&quot; +
                         &quot;&lt;extra&gt;&lt;/extra&gt;&quot;,
                         marker_size=(5*concordant[&#39;irr&#39;]),
                         name=&#39;Concordant between Main and Donor cohort, ABO and RhD&#39;
                        )
              )


fig.add_shape(
       # Line Horizontal
          type=&quot;line&quot;,
         x0=-0.8,
        x1=0.8,
        y0=-(np.log10(0.05)),
        y1=-(np.log10(0.05)),
           line=dict(
              color=&quot;black&quot;,
             width=0.5,
            dash=&quot;dot&quot;
       ), opacity=1,
)
   
    
#Layout
fig.update_layout(title=&#39;&lt;b&gt;Volcanoplot showing Incidence Rate Ratios/False Discovery Rate Adjusted P-Values Depending On ABO Blood Group and RhD Status&#39;
                  &#39;&#39;
                  &#39;&lt;br&gt;&#39;,
                  title_font_color = &#39;#333333&#39;,
                  title_font_size = 14,
                  
                  font=dict(family=&quot;helvetica&quot;),
                  
                  xaxis_title=&#39;&lt;b&gt;IRR&#39;,
                  xaxis_visible=True,
                  xaxis_showline=True,

                  #xaxis_type=&#39;category&#39;,
                  xaxis_gridcolor=&#39;white&#39;,
                  #xaxis_tickangle = 90,
                  xaxis_range=[-0.8,0.8],
                  xaxis_showgrid=False,
                  xaxis_tickvals=[-0.5, 0, 0.5],
                  xaxis_linecolor=&#39;black&#39;,
                  
                  plot_bgcolor=&#39;white&#39;,
                  showlegend=True,
                  legend= {&#39;itemsizing&#39;: &#39;constant&#39;},
                  hoverlabel=dict(
                        bgcolor=&quot;white&quot;, 
                        font_size=18, 
                        font_family=&quot;helvetica&quot;),
                  
                  yaxis_ticks=(&#39;outside&#39;),
                  yaxis_tickwidth=1,
                  yaxis_ticklen=5,
                  yaxis_title=&#39;&lt;b&gt;-log10(FDR-adjusted p-value)&#39;,
                  yaxis_showline=True,
                  yaxis_showgrid=False,
                  yaxis_visible=True,
                  yaxis_linewidth=1,
                  yaxis_linecolor=&#39;black&#39;,
                  yaxis_range=[-5,140],
                  #yaxis_tickangle = 90,
                  yaxis_tickvals=[-(np.log10(0.05)),50, 100],
                  yaxis_ticktext=[&#39;FDR-P 0.05&#39;,50,100],
                  #yaxis_ticksuffix=&#39;%&#39;,
                  
                  width=1000,
                  height=900
                  )

fig.show()</code></pre>
            <figure slot="outputs">
              <stencila-image-plotly>
                <picture>
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showing Incidence Rate Ratios/False Discovery Rate Adjusted P-Values Depending On ABO Blood Group and RhD Status<br>"},"width":1000,"xaxis":{"gridcolor":"white","linecolor":"black","range":[-0.8,0.8],"showgrid":false,"showline":true,"tickvals":[-0.5,0,0.5],"title":{"text":"<b>IRR"},"visible":true},"yaxis":{"linecolor":"black","linewidth":1,"range":[-5,140],"showgrid":false,"showline":true,"ticklen":5,"ticks":"outside","ticktext":["FDR-P 0.05",50,100],"tickvals":[1.3010299956639813,50,100],"tickwidth":1,"title":{"text":"<b>-log10(FDR-adjusted p-value)"},"visible":true}}}
                  </script><img src="index.html.media/0" alt="" itemscope=""
                    itemtype="http://schema.org/ImageObject">
                </picture>
              </stencila-image-plotly>
            </figure>
          </stencila-code-chunk>
          <figcaption>
            <h4 itemscope="" itemtype="http://schema.stenci.la/Heading"
              id="volcano-plot-of-all-findings-from-main-and-validation-cohort">Volcano plot of all
              findings from main and validation cohort.</h4>
            <p itemscope="" itemtype="http://schema.stenci.la/Paragraph"> Volcano plot depicting
              spread of p-values of significant and non-significant ABO and RhD blood groups for
              main cohort and validated results. The labels represent the nine findings with the
              lowest p-value in the validation cohort.</p>
          </figcaption>
        </figure>
        <figure itemscope="" itemtype="http://schema.stenci.la/Figure" id="fig2" title="Figure 2.">
          <label data-itemprop="label">Figure 2.</label>
          <stencila-code-chunk itemscope="" itemtype="http://schema.stenci.la/CodeChunk"
            data-execution_count="3" data-programminglanguage="python">
            <pre class="language-python" itemscope="" itemtype="http://schema.stenci.la/CodeBlock"
              slot="text"><code>df = pd.read_csv(&#39;df_man.csv&#39;)
df_r = pd.read_csv(&#39;df_r_man.csv&#39;)
concordant = pd.read_csv(&#39;concordant_man.csv&#39;)
mchap = pd.read_csv(&#39;mchap.csv&#39;)

fig = go.Figure()
fdr_p=df[&#39;fdr_p&#39;]

grp=df[&#39;bg&#39;].unique().tolist()
for groups in grp:
        data_filtered=df[(df.bg==groups) &amp; (df.fdr_p &lt; 0.05)]
        fig.add_trace(go.Scatter(x=data_filtered[&#39;row&#39;], 
                         y=data_filtered[&#39;y&#39;], 
                         mode=&#39;markers&#39;,
                             opacity=0.5,
                         marker=dict(color=data_filtered[&#39;color&#39;],line=dict(color=&#39;white&#39;,width=0)),
                         text=data_filtered[&#39;bg_cat&#39;],
                         customdata=data_filtered[&#39;event_pyrs&#39;],
                         hovertext=data_filtered[&#39;fdr_p&#39;],
                     
                        meta=data_filtered[&#39;combined&#39;],
                        hovertemplate = &quot;&lt;b&gt;%{text}&lt;/b&gt;&quot; +
                         &quot;&lt;br&gt;FDR-P: %{hovertext:,.2g}:&quot; +
                         &quot;&lt;br&gt;IRR (95% CI): %{meta}&quot; +
                         &quot;&lt;br&gt;Events/Person-years: %{customdata}&quot; +
                         &quot;&lt;extra&gt;&lt;/extra&gt;&quot;,
                         marker_size=(9*data_filtered[&#39;irr&#39;]),
                         name=groups
                        )
              )



df_r2=df_r[df_r.fdr_p&lt;0.05]
fig.add_trace(go.Scatter(x=df_r2[&#39;x&#39;], 
                         y=df_r2[&#39;y&#39;], 
                         mode=&#39;markers&#39;,
                             opacity=0.5,
                         marker=dict(color=df_r2[&#39;color&#39;],opacity=df_r2[&#39;opacity&#39;],line=dict(color=&#39;white&#39;,width=0)),
                         text=df_r2[&#39;bg_cat&#39;],
                         customdata=df_r2[&#39;event_pyrs&#39;],
                         hovertext=df_r2[&#39;fdr_p&#39;],
                        meta=df_r2[&#39;combined&#39;],
                        hovertemplate = &quot;&lt;b&gt;%{text}&lt;/b&gt;&quot; +
                         &quot;&lt;br&gt;FDR-P: %{hovertext:,.2g}:&quot; +
                         &quot;&lt;br&gt;IRR (95% CI): %{meta}&quot; +
                         &quot;&lt;br&gt;Events/Person-years: %{customdata}&quot; +
                         &quot;&lt;extra&gt;&lt;/extra&gt;&quot;,
                         name=&#39;RhD positive&#39;
                        )
              )
              
fig.add_trace(go.Scatter(x=pd.concat([df_r.x[(df_r.fdr_p&gt;=0.05)],df.x[(df.fdr_p&gt;=0.05)]]), 
                         y=pd.concat([df_r.y[(df_r.fdr_p&gt;=0.05)],df.y[(df.fdr_p&gt;=0.05)]]), 
                         mode=&#39;markers&#39;,
                             opacity=0.7,
                         marker=dict(color=pd.concat([df_r.color[(df_r.fdr_p&gt;=0.05)],df.color[(df.fdr_p&gt;=0.05)]]),opacity=0.7,line=dict(color=&#39;white&#39;,width=0)),

                         marker_size=2,
                         name=&#39;Non-significant ABO and RhD&#39;,
                         showlegend=True,
                        )
              )
    
    


fig.add_trace(go.Scatter(x=concordant.x, 
                         y=concordant.y, 
                         mode=&#39;markers&#39;,
                             opacity=0.8,
                         marker=dict(color=concordant[&#39;color&#39;],opacity=0.8,line=dict(color=&#39;white&#39;,width=0)),
                         text=concordant[&#39;bg_cat&#39;],
                        customdata=concordant[&#39;event_pyrs&#39;],
                         hovertext=concordant[&#39;bon_p&#39;],
                        meta=concordant[&#39;combined&#39;],
                        hovertemplate = &quot;&lt;b&gt;%{text}&lt;/b&gt;&quot; +
                         &quot;&lt;br&gt;BON-P: %{hovertext:,.2g}:&quot; +
                         &quot;&lt;br&gt;IRR (95% CI): %{meta}&quot; +
                         &quot;&lt;br&gt;Events/Person-years: %{customdata}&quot; +
                         &quot;&lt;extra&gt;&lt;/extra&gt;&quot;,
                         marker_size=(5*concordant[&#39;irr&#39;]),
                         name=&#39;Concordant in validation cohort, after bonferroni-adjustment&#39;
                        )
              )

fig.add_trace(go.Scatter(x=[], 
                         y=[],
                        mode=&#39;markers&#39;,
                         xaxis=&#39;x2&#39;
                        )
             )

fig.add_shape(
       # Line Horizontal
          type=&quot;line&quot;,
         x0=0,
        x1=df.x.max()+1,
        y0=-(np.log10(0.05)),
        y1=-(np.log10(0.05)),
           line=dict(
              color=&quot;black&quot;,
             width=0.5,
            dash=&quot;dot&quot;
       ), opacity=1,
)

    
#Layout
fig.update_layout(
    title=&#39;&lt;b&gt;Manhattanplot - Disease catagories/False Discovery Rate Adjusted P-Values In Main Cohort Depending On ABO Blood Group. &lt;/b&gt; &lt;br&gt;&#39;
                  &#39;&#39;
                  &#39;&#39;,
                  title_font_color = &#39;#333333&#39;,
                  title_font_size = 14,
                  
                  font=dict(family=&quot;helvetica&quot;),
                  
                  xaxis=dict(
                      anchor=&#39;y&#39;,
                      title=&#39;&lt;b&gt;&#39;,
                      visible=True,
                      showline=True,
                      gridcolor=&#39;white&#39;,
                      tickangle = 300,
                      range=[0,df.x.max()],
                      showgrid=False,
                      ticks=(&#39;inside&#39;),
                      ticklen=0,
                     # tickangle=0,
                      tickvals=mchap[&#39;median&#39;],
                      ticktext=mchap[&#39;names&#39;].tolist(),
                      linecolor=&#39;black&#39;,
                      linewidth=1),

                  xaxis2=dict(
                      anchor=&#39;y&#39;,
                      overlaying=&#39;x&#39;,
                      title=&#39;&lt;b&gt;&#39;,
                      visible=True,
                      showline=True,
                      gridcolor=&#39;white&#39;,
                      tickangle = 0,
                      range=[0,df.x.max()],
                      showgrid=False,
                      ticklen=5,
                      tickvals=mchap[&#39;mins&#39;],
                      showticklabels=False,
                   #   ticktext=[&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,&quot;&quot;,],
                      linecolor=&#39;black&#39;,
                      tickcolor=&#39;black&#39;,
                      ticks=(&#39;outside&#39;),
                      linewidth=1),

                  plot_bgcolor=&#39;white&#39;,
                  showlegend=True,
                  legend= {&#39;itemsizing&#39;: &#39;constant&#39;},
                  hoverlabel=dict(
                        bgcolor=&quot;white&quot;, 
                        font_size=18, 
                        font_family=&quot;helvetica&quot;),
                  
                  yaxis_ticks=(&#39;outside&#39;),
                  yaxis_tickwidth=1,
                  yaxis_ticklen=5,
                  yaxis_title=&#39;&lt;b&gt;-log10(FDR-adjusted p-value)&#39;,
                  yaxis_showline=True,
                  yaxis_showgrid=False,
                  yaxis_visible=True,
                  yaxis_linewidth=1,
                  yaxis_linecolor=&#39;black&#39;,
                  #yaxis_range=[-5,190],
                  #yaxis_tickangle = 90,
                  yaxis_tickvals=[-(np.log10(0.05)),50, 100],
                  yaxis_ticktext=[&#39;P 0.05&#39;,50,100],
                               #yaxis_ticksuffix=&#39;%&#39;,
                  yaxis_range=[-0.5,130],
                  
                  width=1200,
                  height=1200
                  )

    

fig.show()</code></pre>
            <figure slot="outputs">
              <stencila-image-plotly>
                <picture>
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                  </script><img src="index.html.media/1" alt="" itemscope=""
                    itemtype="http://schema.org/ImageObject">
                </picture>
              </stencila-image-plotly>
            </figure>
          </stencila-code-chunk>
          <figcaption>
            <h4 itemscope="" itemtype="http://schema.stenci.la/Heading"
              id="manhattan-plot-of-all-findings-from-main-and-validation-cohort-mapped-by-icd-chapter">
              Manhattan plot of all findings from main and validation cohort mapped by ICD chapter.
            </h4>
            <p itemscope="" itemtype="http://schema.stenci.la/Paragraph"> Manhattan plot depicting
              distribution of p-values for significant and non-significant associations between ABO
              and RhD blood groups and available outcomes for main cohort and validated results
              mapped by disease chapter in ICD.</p>
          </figcaption>
        </figure>
        <table id="table2" itemscope="" itemtype="http://schema.org/Table">
          <caption><label data-itemprop="label">Table 2.</label>
            <div itemprop="caption">
              <h3 itemscope="" itemtype="http://schema.stenci.la/Heading"
                id="meta-summary-of-results">Meta-summary of results.</h3>
            </div>
          </caption>
          <thead>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell">Main cohort</th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell">Validation cohort</th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
              <th itemscope="" itemtype="http://schema.stenci.la/TableCell"></th>
            </tr>
          </thead>
          <tbody>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Individuals</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">4,204,234</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1,197,522</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Person-years, sum</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">50 M</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">22 M</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Events, median (IQR)
              </td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">4748 (869–23,166)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">7129 (2464–19,973)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">A</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">AB</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">B</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">ABO total</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">RhD positive</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">A</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">AB</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">B</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">ABO total</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">RhD positive</td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Before adjustment</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">229</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">129</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">179</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">537</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">106</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">64</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">37</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">42</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">143</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">5</span></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Positive effects, N</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">150</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">79</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">107</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">336</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">61</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">47</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">23</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">22</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">92</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">3</span></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Negative effects, N</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">79</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">50</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">72</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">201</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">45</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">17</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">14</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">20</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">51</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">2</span></td>
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            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">After adjustment*</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">108</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">56</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">70</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">234</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">13</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">26</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">13</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">10</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">49</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">1</span></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Positive effects, N</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">66</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">38</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">36</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">140</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">10</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">19</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">10</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">6</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">35</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">1</span></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Negative effects, N</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">42</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">18</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">34</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">94</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">3</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">7</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">3</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">4</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">14</span></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"><span
                  data-itemtype="http://schema.org/Number">0</span></td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Positive IRR, median
                (range)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1.05 (1.01–1.72)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1.09 (1.03–1.52)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1.09 (1.02–1.39)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1.05 (1.02–1.08)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1.1 (1.03–1.57)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1.32 (1.07–1.89)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1.5 (1.07–1.64)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">1.12 (1.12–1.12)</td>
            </tr>
            <tr itemscope="" itemtype="http://schema.stenci.la/TableRow">
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">Negative IRR, median
                (range)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">0.95 (0.77–0.99)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">0.92 (0.74–0.97)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">0.92 (0.57–0.98)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">0.97 (0.9–0.97)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">0.92 (0.86–0.95)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">0.84 (0.81–0.87)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">0.88 (0.83–0.93)</td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell"></td>
              <td itemscope="" itemtype="http://schema.stenci.la/TableCell">-</td>
            </tr>
          </tbody>
        </table>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">In our validation cohort,
          consisting of almost 1.2 million blood donors accruing 22 million person-years of
          follow-up, we validated the findings from the significant disease categories from the
          first analysis. Among the 143 and 5 significant disease categories for ABO and RhD,
          respectively, the median number of events was 7129 (IQR 2464–19,973). Before multiple
          testing adjustment, we identified 160 associations between a blood group in 143 and 5
          disease categories, for the ABO and RhD blood group, respectively. After
          Bonferroni adjustment, there were 49 and 1 associations remaining between ABO and RhD
          blood group, respectively (<a href="#table2" itemscope=""
            itemtype="http://schema.stenci.la/Link">Table 2</a> and <a href="#fig3" itemscope=""
            itemtype="http://schema.stenci.la/Link">Figure 3</a>).</p>
        <figure itemscope="" itemtype="http://schema.stenci.la/Figure" id="fig3" title="Figure 3.">
          <label data-itemprop="label">Figure 3.</label>
          <stencila-code-chunk itemscope="" itemtype="http://schema.stenci.la/CodeChunk"
            data-execution_count="4" data-programminglanguage="python">
            <pre class="language-python" itemscope="" itemtype="http://schema.stenci.la/CodeBlock"
              slot="text"><code>df = pd.read_csv(&#39;fig3.csv&#39;)
concordant = pd.read_csv(&#39;concor_engcat.csv&#39;)


fig = make_subplots(cols=7, 
                    shared_yaxes=&#39;rows&#39;, 
                    column_widths=[0.20,0.08,0.20,0.08,0.20,0.08,0.01], 
                    horizontal_spacing = 0.01,
                    subplot_titles=(&quot;&lt;b&gt;A&quot;, &quot;&lt;i&gt;P&quot;, &quot;&lt;b&gt;AB&quot;, &quot;&lt;i&gt;P&quot;,&quot;&lt;b&gt;B&quot;,&quot;&lt;i&gt;P&quot;),
                  # column_titles=(&quot;A&quot;, &quot;&quot;, &quot;B&quot;, &quot;&quot;,&quot;AB&quot;,&quot;&quot;)
                   )


dfa=df[df[&#39;bg&#39;]==&quot;A&quot;]
engcat=dfa[&#39;engcat&#39;].tolist()

for cat in engcat:
    data_filtered=dfa[(dfa.engcat==cat)]
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=10,
                        marker=dict(color=data_filtered[&#39;color&#39;],size=10,symbol=&#39;square&#39;, opacity=0.5),
                        opacity=0.5,
                         
                         error_x=dict(type=&#39;data&#39;,
                                     symmetric=False,
                                     array=data_filtered[&#39;up&#39;]-data_filtered[&#39;x&#39;],
                                     arrayminus=data_filtered[&#39;x&#39;]-data_filtered[&#39;lo&#39;],
                                     color=data_filtered[&#39;color&#39;].min(),
                           
                                     thickness=10,
                                     width=0)
                       
                ), row=1, col=1
              )
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=7,
                        marker=dict(color=data_filtered[&#39;color&#39;],size=8,symbol=&#39;line-ns-open&#39;, opacity=1),
                        
                       
                ), row=1, col=1
              )

    
    fig.add_trace(go.Scatter(x=[0.05], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;text&#39;,
                             text=(data_filtered[&#39;pvalue&#39;].map(&#39;{:.2g}&#39;.format)),
                             textposition=&quot;middle right&quot;,
                         marker_symbol=&#39;square&#39;,
                         marker_size=10,
                         marker_color=data_filtered[&#39;color&#39;],
                         opacity=1,                     
                       
                ), row=1, col=2
              )
    databon=data_filtered[data_filtered[&#39;bon_p&#39;]&lt;0.05]
    fig.add_trace(go.Heatmap(
                   z=databon[&#39;bon_p&#39;],
                   x=[0.5,1.5,2.5,3.5],
                   y=[databon[&#39;names&#39;],databon[&#39;engcat&#39;]],
                showscale=False,
                text=databon[&#39;pvalue&#39;],
                opacity=0.2,
                 ygap=4,
                xgap=4,
                colorscale=[[0.0, &quot;white&quot;], [1,np.where(pd.isna(databon[&#39;color&#39;].min()),&#39;white&#39;,databon[&#39;color&#39;].min()).tolist()]],

                            ), row=1, col=2,
                )

    
dfb=df[df[&#39;bg&#39;]==&quot;AB&quot;]
engcat=dfb[&#39;engcat&#39;].tolist()

for cat in engcat:
    data_filtered=dfb[(dfb.engcat==cat)]
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=10,
                        marker=dict(color=data_filtered[&#39;color&#39;],size=10,symbol=&#39;square&#39;, opacity=0.5),
                        opacity=0.5,
                         
                         error_x=dict(type=&#39;data&#39;,
                                     symmetric=False,
                                     array=data_filtered[&#39;up&#39;]-data_filtered[&#39;x&#39;],
                                     arrayminus=data_filtered[&#39;x&#39;]-data_filtered[&#39;lo&#39;],
                                     color=data_filtered[&#39;color&#39;].min(),
                           
                                     thickness=10,
                                     width=0)
                       
                ), row=1, col=3
              )
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=7,
                        marker=dict(color=data_filtered[&#39;color&#39;],size=8,symbol=&#39;line-ns-open&#39;, opacity=1),
                        
                       
                ), row=1, col=3
              )
    
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=10,
                        marker=dict(color=&#39;lightgrey&#39;,size=10,symbol=&#39;square&#39;, opacity=0.5),
                        opacity=0.5,
                         
                         error_x=dict(type=&#39;data&#39;,
                                     symmetric=False,
                                     array=data_filtered[&#39;up&#39;]-data_filtered[&#39;x&#39;],
                                     arrayminus=data_filtered[&#39;x&#39;]-data_filtered[&#39;lo&#39;],
                                     color=&#39;lightgrey&#39;,
                           
                                     thickness=10,
                                     width=0)
                       
                ), row=1, col=3
              )
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=7,
                        marker=dict(color=&#39;black&#39;,size=8,symbol=&#39;line-ns-open&#39;, opacity=0.5),
                        
                       
                ), row=1, col=3
              )

    fig.add_trace(go.Scatter(x=[0.05], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;text&#39;,
                             text=(data_filtered[&#39;pvalue&#39;].map(&#39;{:.2g}&#39;.format)),
                             textposition=&quot;middle right&quot;,
                         marker_symbol=&#39;square&#39;,
                         marker_size=10,
                         marker_color=data_filtered[&#39;color&#39;],
                         opacity=1,                     
                       
                ), row=1, col=4
              )
    databon=data_filtered[data_filtered[&#39;bon_p&#39;]&lt;0.05]
    fig.add_trace(go.Heatmap(
                   z=databon[&#39;bon_p&#39;],
                   x=[0.5],
                   y=[databon[&#39;names&#39;],databon[&#39;engcat&#39;]],
                showscale=False,
                text=databon[&#39;pvalue&#39;],
                opacity=0.5,
                 ygap=4,
                xgap=4,
                colorscale=[[0.0, &quot;white&quot;], [1,np.where(pd.isna(databon[&#39;color&#39;].min()),&#39;white&#39;,databon[&#39;color&#39;].min()).tolist()]],
                            ), row=1, col=4,
                )
    
dfc=df[df[&#39;bg&#39;]==&quot;B&quot;]
engcat=dfc[&#39;engcat&#39;].tolist()

for cat in engcat:
    data_filtered=dfc[(dfc.engcat==cat)]
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=10,
                        marker=dict(color=data_filtered[&#39;color&#39;],size=10,symbol=&#39;square&#39;, opacity=0.5),
                        opacity=0.5,
                         
                         error_x=dict(type=&#39;data&#39;,
                                     symmetric=False,
                                     array=data_filtered[&#39;up&#39;]-data_filtered[&#39;x&#39;],
                                     arrayminus=data_filtered[&#39;x&#39;]-data_filtered[&#39;lo&#39;],
                                     color=data_filtered[&#39;color&#39;].min(),
                           
                                     thickness=10,
                                     width=0)
                       
                ), row=1, col=5
              )
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=7,
                        marker=dict(color=data_filtered[&#39;color&#39;],size=8,symbol=&#39;line-ns-open&#39;, opacity=1),
                        
                       
                ), row=1, col=5
              )    
    
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=10,
                        marker=dict(color=&#39;lightgrey&#39;,size=10,symbol=&#39;square&#39;, opacity=0.5),
                        opacity=0.5,
                         
                         error_x=dict(type=&#39;data&#39;,
                                     symmetric=False,
                                     array=data_filtered[&#39;up&#39;]-data_filtered[&#39;x&#39;],
                                     arrayminus=data_filtered[&#39;x&#39;]-data_filtered[&#39;lo&#39;],
                                     color=&#39;lightgrey&#39;,
                           
                                     thickness=10,
                                     width=0)
                       
                ), row=1, col=5
              )
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=7,
                        marker=dict(color=&#39;black&#39;,size=8,symbol=&#39;line-ns-open&#39;, opacity=0.5),
                        
                       
                ), row=1, col=5
              )

    fig.add_trace(go.Scatter(x=[0.05], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;text&#39;,
                             text=(data_filtered[&#39;pvalue&#39;].map(&#39;{:.2g}&#39;.format)),
                             textposition=&quot;middle right&quot;,
                         marker_symbol=&#39;square&#39;,
                         marker_size=10,
                         marker_color=data_filtered[&#39;color&#39;],
                         opacity=1,                     
                       
                ), row=1, col=6
              )
    databon=data_filtered[data_filtered[&#39;bon_p&#39;]&lt;0.05]
    fig.add_trace(go.Heatmap(
                   z=databon[&#39;bon_p&#39;],
                   x=[0.5,1.5,2.5,3.5],
                   y=[databon[&#39;names&#39;],databon[&#39;engcat&#39;]],
                showscale=False,
                text=databon[&#39;pvalue&#39;],
                opacity=0.5,
                 ygap=4,
                xgap=4,
                colorscale=[[0.0, &quot;white&quot;], [1,np.where(pd.isna(databon[&#39;color&#39;].min()),&#39;white&#39;,databon[&#39;color&#39;].min()).tolist()]],

                            ), row=1, col=6,
                )

    
    
dfc=df[df[&#39;bg&#39;]==&quot;AB&quot;]
engcat=dfc[&#39;engcat&#39;].tolist()

for cat in engcat:
    data_filtered=dfc[(dfc.engcat==cat)]
    fig.add_trace(go.Scatter(x=data_filtered[&#39;x&#39;], 
                         y=[data_filtered[&#39;names&#39;],data_filtered[&#39;engcat&#39;]], 
                         mode=&#39;markers&#39;,
                        marker_symbol=&#39;line-ns-open&#39;,
                        marker_size=7,
                        marker=dict(color=&#39;white&#39;,size=8,symbol=&#39;line-ns-open&#39;, opacity=1),
                        
                       
                ), row=1, col=7
              )    
                                                                

        

         
fig.add_shape(
       # Line Horizontal
          type=&quot;line&quot;,
         x0=0,
        x1=0,
        y0=-0.5,
        y1=(df.engcat.nunique()-0.5),
           line=dict(
              color=&quot;black&quot;,
             width=0.5,
            dash=&quot;dot&quot;
       ), opacity=1,row=1, col=1,
)      

fig.add_shape(
       # Line Horizontal
          type=&quot;line&quot;,
         x0=0,
        x1=0,
        y0=-0.5,
        y1=(df.engcat.nunique()-0.5),
           line=dict(
              color=&quot;black&quot;,
             width=0.5,
            dash=&quot;dot&quot;
       ), opacity=1,row=1, col=3,
)      

fig.add_shape(
       # Line Horizontal
          type=&quot;line&quot;,
         x0=0,
        x1=0,
        y0=-0.5,
        y1=(df.engcat.nunique()-0.5),
           line=dict(
              color=&quot;black&quot;,
             width=0.5,
            dash=&quot;dot&quot;
       ), opacity=1,row=1, col=5,
)      
 

fig.add_annotation(
            x=1,
            y=(df.engcat.nunique()),
            yshift=20,
            text=&quot;&lt;b&gt;FDR-p&quot;,
            yref=&quot;paper&quot;,
            showarrow=False,
            row=1, col=4
            )


fig.add_annotation(
            x=2.4,
            y=(df.engcat.nunique()),
            yshift=20,
            #xshift=3,
            text=&quot;&lt;b&gt;Events&quot;,
            yref=&quot;paper&quot;,
            showarrow=False,
            row=1, col=4
            )
   

fig.add_annotation(
            x=1,
            y=(df.engcat.nunique()),
            yshift=20,
            text=&quot;&lt;b&gt;FDR-p&quot;,
            yref=&quot;paper&quot;,
            showarrow=False,
            row=1, col=6
            )



fig.add_shape(type=&quot;line&quot;,xref=&quot;paper&quot;, x0=-0.915,x1=-0.915,y0=-0.5,y1=(concordant.engcat.nunique()-0.5),line=dict(color=&quot;black&quot;,width=1))      




#Layout
fig.update_layout(
#     title=&#39;&lt;b&gt;Concordant Results Between Main and Donor Cohort&lt;/b&gt;&#39; 
#                      &#39;&lt;br&gt;Black Marker And Corresponding Interval Represents Validation Cohort&#39;
#                       &#39;&lt;br&gt;FDR-adjusted P-Values In Column&#39;,
                  
                  title_font_color = &#39;#333333&#39;,
                  title_font_size = 16,
                  
                  font=dict(family=&quot;helvetica&quot;),
                  
                  coloraxis=dict(showscale=False, colorscale=&quot;RdBu&quot;,cmid=1.00, cmin=0.01,cmax=1.99),
                  
                  xaxis_title=&#39;&lt;b&gt;Incidence rate ratios&#39;,
                  xaxis_visible=True,
                  xaxis_showline=True,
                  xaxis_zeroline=False,

                  yaxis_type=&#39;multicategory&#39;,
                  xaxis_gridcolor=&#39;white&#39;,
                  #xaxis_tickangle = 90,
                  xaxis_range=[-0.5,10],
                  xaxis_tickvals=[1,2,3,4,5,6,7,8,9],
                  xaxis_mirror=&quot;allticks&quot;,
                  xaxis_showgrid=False,
      #            xaxis_tickvals=[0, 1, 2],
                  xaxis_linecolor=&#39;black&#39;,
                  
                  plot_bgcolor=&#39;white&#39;,
                  showlegend=False,
                 # legend= {&#39;itemsizing&#39;: &#39;constant&#39;},
                 # hoverlabel=dict(
                 #       bgcolor=&quot;white&quot;, 
                 #       font_size=18, 
                 #       font_family=&quot;helvetica&quot;),
                #  yaxis_anchor=&#39;free&#39;,
               #   yaxis_fixedrange=True,
                  yaxis_range=[-0.5,(df.engcat.nunique()-0.5)],
      #            yaxis_position=0,
                 # yaxis_ticks=(&#39;outside&#39;),
       #           yaxis_tickwidth=1,
        #          yaxis_ticklen=5,
                  #yaxis_title=&#39;&lt;b&gt;-log10(False discovery rate p-value)&#39;,
                  yaxis_showline=True,
                  yaxis_showdividers=True,
                  yaxis_dividerwidth=2,
                 # yaxis_tickson=&quot;boundaries&quot;,

                  yaxis_showgrid=False,
                  yaxis_visible=True,
                  yaxis_linewidth=1,
                  yaxis_linecolor=&#39;black&#39;,
  
                  width=1200,
                  height=1550,
                margin=dict(
        l=550,
        r=50,
        b=20,
        t=20,
        pad=4
    ),
                  )

# yaxis
fig.update_yaxes(title_text=&quot;&quot;,linecolor=&#39;black&#39;,visible=True,showline=True,dividerwidth=2,showgrid=False,showdividers=True,row=1, col=5)
fig.update_yaxes(title_text=&quot;&quot;,linecolor=&#39;black&#39;,visible=True,showline=True,dividerwidth=2,showgrid=False,showdividers=True,row=1, col=7)

fig.update_yaxes(title_text=&quot;&quot;,linecolor=&#39;black&#39;,visible=True,showline=True,showgrid=False,dividerwidth=2,showdividers=True,row=1, col=3)
fig.update_yaxes(title_text=&quot;&quot;,linecolor=&#39;black&#39;,visible=True,showline=True,dividerwidth=2,showdividers=True,row=1, col=2)
fig.update_yaxes(title_text=&quot;&quot;,linecolor=&#39;black&#39;,visible=True,showline=True,dividerwidth=2,showdividers=True,row=1, col=4)
fig.update_yaxes(title_text=&quot;&quot;,linecolor=&#39;black&#39;,visible=True,showline=True,dividerwidth=2,showdividers=True,row=1, col=6)


# xaxis
fig.update_xaxes(title_text=&#39;&#39;,visible=True,showline=False,tickfont_size = 9,range=[-np.log10(2),np.log10(2)],tickvals=[-np.log10(2),0,np.log10(2)],ticktext=[&#39;-2&#39;,&#39;0&#39;,&#39;2&#39;],gridcolor=&#39;lightgrey&#39;,showgrid=False,linewidth=3,linecolor=&#39;black&#39;,row=1, col=1)
fig.update_xaxes(title_text=&#39;&#39;,visible=False,showline=True,tickfont_size = 9,range=[0,1],gridcolor=&#39;black&#39;,tickangle = 300,ticklen=0,showgrid=False,linecolor=&#39;black&#39;,row=1, col=2)
fig.update_xaxes(title_text=&#39;&lt;b&gt;log(Incidence Rate Ratio)&#39;,visible=True,showline=False,tickfont_size = 9,range=[-np.log10(2),np.log10(2)],tickvals=[-np.log10(2),0,np.log10(2),np.log10(3),np.log10(4),np.log10(5)],ticktext=[&#39;-2&#39;,&#39;0&#39;,&#39;2&#39;,&#39;3&#39;,&#39;4&#39;,&#39;5&#39;],gridcolor=&#39;black&#39;,showgrid=False,linewidth=3,linecolor=&#39;black&#39;,row=1, col=3)
fig.update_xaxes(title_text=&#39;&#39;,visible=False,showline=True,tickfont_size = 9,range=[0,1],gridcolor=&#39;black&#39;,tickangle = 300,ticklen=0,showgrid=False,linecolor=&#39;black&#39;,row=1, col=4)
fig.update_xaxes(title_text=&#39;&#39;,visible=True,showline=False,tickfont_size = 9,range=[-np.log10(2),np.log10(2)],tickvals=[-np.log10(2),0,np.log10(2),np.log10(3)],ticktext=[&#39;-2&#39;,&#39;0&#39;,&#39;2&#39;,&#39;3&#39;],gridcolor=&#39;black&#39;,gridwidth=2,showgrid=False,linewidth=3,linecolor=&#39;black&#39;,row=1, col=5)
fig.update_xaxes(title_text=&#39;&#39;,visible=False,showline=True,tickfont_size = 9,range=[0,1],gridcolor=&#39;black&#39;,tickangle = 300,ticklen=0,showgrid=False,linecolor=&#39;black&#39;,row=1, col=6)
fig.update_xaxes(title_text=&#39;&#39;,visible=False,showline=True,type=&#39;category&#39;,tickfont_size = 9,range=[0,3],gridcolor=&#39;white&#39;,tickangle = 300,ticklen=0,showgrid=False,linecolor=&#39;black&#39;,row=1, col=7)




fig.show()</code></pre>
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          </stencila-code-chunk>
          <figcaption>
            <h4 itemscope="" itemtype="http://schema.stenci.la/Heading"
              id="all-significant-un-adjusted-findings-from-the-validation-cohort">All significant
              un-adjusted findings from the validation cohort.</h4>
            <p itemscope="" itemtype="http://schema.stenci.la/Paragraph"> Significant disease
              categories in the validation cohort. Blood group as compared to blood group O and
              log10(IRR) displayed with 95% confidence bands. All p-values are raw, highlighted
              p-value indicates associations that remained statistically significant also after
              Bonferroni adjustment.</p>
          </figcaption>
        </figure>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">A number of previously
          well-established associations were seen among the Bonferroni-adjusted results. For
          thrombosis, blood group A had a higher risk as compared to blood group O (e.g., pulmonary
          embolism, IRR 1.57 [95% CI, 1.51–1.64] and portal vein thrombosis, IRR 1.51 [95% CI,
          1.25–1.83]). Bleeding disorders were more frequent in blood group O as compared to blood
          group A (e.g., gastric ulcer, IRR 0.92 [95% CI, 0.88–0.95] and duodenal ulcer, IRR 0.86
          [95% CI, 0.82–0.9]). Thyrotoxicosis was also less common in blood groups A and AB as
          compared to blood group O (with IRRs of 0.90 [95% CI, 0.86–0.93] and 0.84 [95% CI,
          0.77–0.92], for A and AB, respectively). Pregnancy-induced hypertension was less common in
          blood groups A and AB, as compared to blood group O (with IRRs of 0.95 [95% CI, 0.92–0.97]
          and 0.87 [95% CI, 0.83–0.92] for A and AB, respectively). Pancreatic cancer was the only
          malignancy that remained associated with a blood group, specifically blood group A as
          compared to blood group O (IRR, 1.29; 95% CI, 1.19–1.40). A new finding was that of
          calculus of the kidney and ureter, which were found to be less common in blood group B as
          compared to blood group O (IRR 0.93 [95% CI, 0.89–0.96]). Cholelithiasis, which has been
          disputed, was more common in blood groups A and AB as compared to blood group O (with IRRs
          of 1.07 [95% CI, 1.05–1.09] and 1.09 [95% CI, 1.05–1.13] for A and AB, respectively).</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">In disease categories not
          significant after Bonferroni adjustment, some findings exhibited particularly strong
          effects, such as for viral and other specified intestinal infections, where blood group AB
          had a significantly lower risk, as compared to blood group O (IRR 0.74; 95% CI,
          0.62–0.87). There was a lower risk for ankylosing spondylitis in blood group AB as
          compared to blood group O (IRR 0.79; 95% CI, 0.67–0.94), and for acute pancreatitis, again
          with a lower risk in blood group AB as compared to blood group O (IRR 1.14; 95% CI,
          1.04–1.24). For the RhD positive as compared to RhD negative, only one disease category
          remained statistically significant after Bonferroni adjustment, namely pregnancy-induced
          hypertension (IRR 1.12; 95% CI, 1.09–1.16). Strong effects identified in the main cohort,
          but not in the validation cohort were hereditary factor VIII deficiency in blood group B
          (IRR 0.57; 95% CI, 0.42–0.77), well-differentiated thyroid cancer in blood groups AB (IRR
          0.74; 95% CI, 0.62–0.88) and B (IRR 0.79; 95% CI, 0.70–0.90), measles in blood group A
          (IRR 1.72; 95% CI, 1.23–2.39), as well as both erythema nodosum (IRR 1.32; 95% CI,
          1.15–1.53) and sarcoidosis in blood group B (IRR 1.15; 95% CI, 1.08–1.23), as compared to
          blood group O.</p>
        <h2 itemscope="" itemtype="http://schema.stenci.la/Heading" id="discussion">Discussion</h2>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">In this large cohort study of
          5.1 million unique persons followed over 70 million person-years, we performed an agnostic
          analysis of associations between the ABO and RhD blood groups and the risk of 1217
          distinct disease categories. After multiple testing adjustment and comparison with a
          validation cohort, 49 and 1 associations between disease categories and blood group for
          ABO and RhD remained significant, respectively. Overall, we were able to confirm a number
          of previously known associations such as risk of thrombosis and hemorrhagic events. In
          addition, we also identified novel associations, some with firm evidence and valid even
          after conservative Bonferroni adjustment, in the validation cohort, including calculus of
          the kidney and ureter. Furthermore, being the largest study so far, we also found that
          blood groups A and AB had a lower risk of gestational hypertension, compared to blood
          group O, which has previously been disputed <span itemscope=""
            itemtype="http://schema.stenci.la/CiteGroup"><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib5"><span>5</span><span>Clark and
                  Wu</span><span>2008</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a
                href="#bib10"><span>10</span><span>Franchini et
                  al.</span><span>2016</span></a></cite><cite itemscope=""
              itemtype="http://schema.stenci.la/Cite"><a href="#bib15"><span>15</span><span>Lee et
                  al.</span><span>2012</span></a></cite></span>. Of the identified associations, we
          speculate that some associations may be driven by increased screening due to other
          concomitant diseases that are associated with blood groups, which might be the case for
          hyperlipidemias that are screened for in heart disease. Most of the investigated disease
          or disease groups, however, do not seem to be strongly influenced by the ABO blood group
          of the individual. As to possible mechanisms explaining the associations identified, we
          may only generate hypothesis to be further tested. It is however peculiar to identify a
          condition, such as renal caliculi, with highly variable distribution, in regard to
          geographic region, to have an association to blood group. A possible mechanism could be,
          when considering the full spectrum of disease categories investigated, that lower urine pH
          in diabetic patients, a disease category associated with an increased incidence in blood
          group B, may result in altered stone formation <cite itemscope=""
            itemtype="http://schema.stenci.la/Cite"><a href="#bib21"><span>21</span><span>Sorokin et
                al.</span><span>2017</span></a></cite>.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">In previous studies, intending
          to dissect the association between blood groups and disease, there is diversity in
          findings and non-findings, something that may be a consequence of ethnic or geographic
          group, sample size, complexity of statistical modeling, or disease classifications used.
          This, however, imposes difficulties when comparing our results to the vast number of
          studies available concentrating the mentioned discoveries to a select few disease
          categories.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">This is hitherto the largest
          study investigating blood group antigens and disease occurrence in an effort to find novel
          and confirm previously known associations. There are some particular strengths to our
          approach and data. Most notably, the study was based on a very large study population,
          representing one third of the Swedish population, with long-term and unbiased follow-up.
          This ensures both the reliability and the generalizability of the results. The agnostic
          approach also has the advantage of not being based on specific pre-set conceptions of
          specific disease categories and possible associations of blood group. All disease
          categories are treated equally and investigated using the same principles effectively
          removing researcher bias. Moreover, the data has been collected prospectively in various
          high-quality healthcare registries during a long time period with almost complete
          coverage. In addition, the fact that all blood group data in the SCANDAT3-S database were
          collected from clinical transfusion registers – the quality of which is essential for the
          safe administration of blood transfusions – ensures that there should be little or no
          errors in the blood group coding. Similarly, while the validity of the outcomes
          registration certainly varies between the different disease categories, the degree of such
          misclassification is unlikely to vary between blood groups, and so it should not affect
          the magnitude of point estimates.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">The current study is limited by
          several factors. One such factor is the disease classification scheme used, based
          primarily on ICD revision 10 categories that in some instances may lack precision. Smaller
          disease entities were not accounted for and thus there may be true associations that were
          missed. It is thus possible that some of the associations that we reported were driven by
          multiple unknown associations within a specific disease category that may have unequal, or
          even detrimental, effects on the outcome. However, we believe that this limitation is an
          opportunity for further sub-categorized investigations in the future when even more events
          and follow-up time are available.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Another limitation that
          prevents strong casual inference is the possibility some of the observed associations
          between ABO blood group and disease categories were driven by other disease associations
          with ABO blood group. This might, for example, be the case for the associations between
          blood group A and diabetes as well as hyperlipidemia, which are potentially driven not by
          a causal association but possibly instead by an association between blood group A and
          ischemic heart disease, at the occurrence of which diabetes and lipid disorders are
          screened for and thus frequently diagnosed. We cannot exclude the possibility that some of
          the other associations were driven by similar non-causal mechanisms.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">To limit the possibility of
          false-positive findings, we handled over-dispersed Poisson models using Quasi-Poisson and
          also in the main cohort applied the FDR approach, described by Benjamini and Hochberg, and
          then utilized a Bonferroni adjustment on the sub-grouped outcomes in the validation
          cohort. The aim of this approach was to reduce type one errors without being overly
          conservative by first conducting an explorative analysis in the main cohort. We also
          employed a confirmatory analysis with a validation cohort to further limit the possibility
          of false-positive findings. However, because the validation cohort was both smaller and
          consisted only of blood donors, who were selected for their good health, the ensuing
          smaller number of events may result in failure to detect potentially interesting
          associations. Furthermore, selecting explicitly healthy donors with no known serious
          health issue at time of start of donation may result in failure to detect less common or
          specifically non-acquired or early acquired disease. However, in the validation cohort,
          only approximately 1% of the categories had fewer events than 50 and all findings from the
          main cohort can be seen in <a href="#fig1" itemscope=""
            itemtype="http://schema.stenci.la/Link">Figures 1 and </a><a href="#fig2" itemscope=""
            itemtype="http://schema.stenci.la/Link"><span
              data-itemtype="http://schema.org/Number">2</span></a> and Supplementary files 5–8. It
          may still be informative to consider also some of the associations from the main cohort
          that were not corroborated in the validation cohort. This is exemplified by pancreatic
          cancer where we saw an increased risk in blood groups AB and B in the main cohort (IRR
          1.37 and 1.129, p&lt;0.00001 and p&lt;0.00001 for AB and B, respectively) and a similar,
          yet non-significant effect in the validation cohort (IRR 1.14 and 1.26, p-value 0.8 and
          0.6 for B and AB, respectively). This also expands to the non-findings in terms of
          cancerous disease were multiple relationships that have previously been demonstrated, but
          not in the validation cohort after Bonferroni adjustment <cite itemscope=""
            itemtype="http://schema.stenci.la/Cite"><a href="#bib28"><span>28</span><span>Vasan et
                al.</span><span>2016</span></a></cite>. This strengthens our decision to not limit
          the presentation of findings to only disease categories identified in the conservative
          Bonferroni-adjusted analysis.</p>
        <p itemscope="" itemtype="http://schema.stenci.la/Paragraph">Still, after these limitations
          we believe that our findings support and generate strong further evidence for previously
          known associations and indicate new and interesting relationships for disease such as
          calculus of the kidney and ureter, pregnancy-induced hypertension, well-differentiated
          thyroid cancer, and sarcoidosis. The new set of associations should be validated in other
          cohorts but also investigated using a mechanistic approach for a possible causal and
          biological interaction.</p>
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        </section>
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