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    <Identifier>25dkou297</Identifier>
    <IdentifierDoi>10.3205/25dkou297</IdentifierDoi>
    <IdentifierUrn>urn:nbn:de:0183-25dkou2979</IdentifierUrn>
    <ArticleType>Meeting Abstract</ArticleType>
    <TitleGroup>
      <Title language="en">Immunological competence as a critical risk factor for implant-associated infections in hip arthroplasty</Title>
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        <PersonNames>
          <Lastname>Pourbozorg</Lastname>
          <LastnameHeading>Pourbozorg</LastnameHeading>
          <Firstname>Ghazal</Firstname>
          <Initials>G</Initials>
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          <Affiliation>Orthopa&#776;disches Forschungszentrum, Christian-Albrechts-Universita&#776;t zu Kiel, Kiel, Deutschland</Affiliation>
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        <PersonNames>
          <Lastname>M&#252;ller</Lastname>
          <LastnameHeading>M&#252;ller</LastnameHeading>
          <Firstname>Karin </Firstname>
          <Initials>K</Initials>
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        <Address>
          <Affiliation>Orthopa&#776;disches Forschungszentrum, Christian-Albrechts-Universita&#776;t zu Kiel, Kiel, Deutschland</Affiliation>
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          <Lastname>Holz</Lastname>
          <LastnameHeading>Holz</LastnameHeading>
          <Firstname>Mathias</Firstname>
          <Initials>M</Initials>
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          <Affiliation>Klinik fu&#776;r Orthopa&#776;die und Unfallchirurgie, Universita&#776;tsklinikum Schleswig-Holstein, Campus Kiel, Kiel, Deutschland</Affiliation>
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          <Lastname>Simon</Lastname>
          <LastnameHeading>Simon</LastnameHeading>
          <Firstname>Maciej</Firstname>
          <Initials>M</Initials>
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        <Address>
          <Affiliation>Klinik fu&#776;r Orthopa&#776;die und Unfallchirurgie, Universita&#776;tsklinikum Schleswig-Holstein, Campus Kiel, Kiel, Deutschland</Affiliation>
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          <Lastname>Platzer</Lastname>
          <LastnameHeading>Platzer</LastnameHeading>
          <Firstname>Hadrian</Firstname>
          <Initials>H</Initials>
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        <Address>
          <Affiliation>Orthopa&#776;disches Forschungszentrum, Christian-Albrechts-Universita&#776;t zu Kiel, Kiel, Deutschland</Affiliation>
          <Affiliation>Klinik fu&#776;r Orthopa&#776;die und Unfallchirurgie, Universita&#776;tsklinikum Schleswig-Holstein, Campus Kiel, Kiel, Deutschland</Affiliation>
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      <Creator>
        <PersonNames>
          <Lastname>Moradi</Lastname>
          <LastnameHeading>Moradi</LastnameHeading>
          <Firstname>Babak</Firstname>
          <Initials>B</Initials>
        </PersonNames>
        <Address>
          <Affiliation>Orthopa&#776;disches Forschungszentrum, Christian-Albrechts-Universita&#776;t zu Kiel, Kiel, Deutschland</Affiliation>
          <Affiliation>Klinik fu&#776;r Orthopa&#776;die und Unfallchirurgie, Universita&#776;tsklinikum Schleswig-Holstein, Campus Kiel, Kiel, Deutschland</Affiliation>
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          <Corporatename>German Medical Science GMS Publishing House</Corporatename>
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        <Address>D&#252;sseldorf</Address>
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    <SubjectGroup>
      <SubjectheadingDDB>610</SubjectheadingDDB>
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    <DatePublishedList>
      <DatePublished>20251031</DatePublished>
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    <Language>engl</Language>
    <License license-type="open-access" xlink:href="http://creativecommons.org/licenses/by/4.0/">
      <AltText language="en">This is an Open Access article distributed under the terms of the Creative Commons Attribution 4.0 License.</AltText>
      <AltText language="de">Dieser Artikel ist ein Open-Access-Artikel und steht unter den Lizenzbedingungen der Creative Commons Attribution 4.0 License (Namensnennung).</AltText>
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      <Meeting>
        <MeetingId>M0634</MeetingId>
        <MeetingSequence>297</MeetingSequence>
        <MeetingCorporation>Deutsche Gesellschaft f&#252;r Orthop&#228;die und Unfallchirurgie</MeetingCorporation>
        <MeetingCorporation>Deutsche Gesellschaft f&#252;r Orthop&#228;die und Orthop&#228;dische Chirurgie</MeetingCorporation>
        <MeetingCorporation>Deutsche Gesellschaft f&#252;r Unfallchirurgie</MeetingCorporation>
        <MeetingCorporation>Berufsverband f&#252;r Orthop&#228;die und Unfallchirurgie</MeetingCorporation>
        <MeetingName></MeetingName>
        <MeetingTitle>Deutscher Kongress f&#252;r Orthop&#228;die und Unfallchirurgie (DKOU 2025)</MeetingTitle>
        <MeetingSession>Grundlagenforschung &#124; Infekt &#38; Diagnostik 1</MeetingSession>
        <MeetingCity>Berlin</MeetingCity>
        <MeetingDate>
          <DateFrom>20251028</DateFrom>
          <DateTo>20251031</DateTo>
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    <ArticleNo>AB44-4152</ArticleNo>
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      <MainHeadline>Text</MainHeadline><Pgraph><Mark1>Objectives and questions: </Mark1>Implant-associated infections remain a major challenge in hip arthroplasty, particularly among fracture patients, who exhibit higher infection rates than those undergoing elective procedures. This study is the first to explore immune cell distribution and phenotypic variations in hip arthroplasty patients, hypothesizing that differences in immunological competence contribute to the higher infection rates in trauma surgeries compared to elective procedures.</Pgraph><Pgraph><Mark1>Material and methods: </Mark1>In this prospective study, 30 patients undergoing total hip arthroplasty were enrolled, including 17 with osteoarthritis and 13 with femoral neck fractures. Fracture patients were older (82.1 &#177; 11.2 vs. 69.1 &#177; 11.4 years) with higher leukocytes (12.3 &#177; 7.9 vs. 7.3 &#177; 2.2 cells&#47;nl) and C-reactive protein levels (30.6 &#177; 29.5 vs. 2.6 &#177; 1.59 mg&#47;L), while BMI was similar (24.5 &#177; 3.3 vs. 26.0 &#177; 4.1 kg&#47;m&#178;). Peripheral blood samples were collected preoperatively (D0) and on postoperative days 1, 3, and 7. Flow cytometry was employed to assess immune cell populations, including granulocytes (CD19&#8314;, CD56&#8314;), monocytes (CD14&#8314;), various T-helper subsets (Th1, Th2, Th9, Th17, Th22), and regulatory T cells (CD25&#8314;, CD127&#8315;). Paired t-tests were used to compare immune cell distributions over time, with statistical significance set at &#42;p &#60; 0.05, &#42;&#42;p &#60; 0.01, &#42;&#42;&#42;p &#60; 0.001.</Pgraph><Pgraph><Mark1>Results: </Mark1>Preoperative analysis revealed significant differences between the osteoarthritis and fracture groups, with fracture patients showing marked shifts in eosinophils, B cells, cytotoxic T cells, and T-helper cells. Postoperatively, the fracture group exhibited significant alterations in basophil and eosinophil counts on day 1, and sustained differences in natural killer and mast cell populations on days 3 and 7 (Figure 1 <ImgLink imgNo="1" imgType="figure" />). These findings indicate that fracture patients have distinct pre- and postoperative immune profiles that may predispose them to an increased risk of implant-associated infections.</Pgraph><Pgraph><Mark1>Discussion and conclusions: </Mark1>This is the first study to demonstrate that inherent differences in immunological competence, particularly in granulocyte and T-cell subsets, may underlie the higher incidence of implant-associated infections in trauma patients. These results provide novel insights into the role of the immune system in postoperative infection susceptibility following hip arthroplasty and suggest that preoperative immune profiling could be instrumental in risk assessment and the development of tailored clinical interventions.</Pgraph></TextBlock>
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          <Caption><Pgraph><Mark1>Figure 1: Kinetics of Immune Cell Distribution in Hip Osteoarthritis and Fracture Patients. Immune profiling of hip osteoarthritis and fracture patients at time points (pre-surgery: D0, post-surgery: D1, D3, D7) in peripheral blood, as percentages of CD45&#43; cells. Data are mean &#177; SEM.</Mark1></Pgraph></Caption>
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