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    <titleInfo>
      <title>Correlations between treatment outcome and both anti-MSP1(19) antibody response and erythrocyte-related genetic factors in Plasmodium falciparum malaria</title>
    </titleInfo>
    <name type="personnal">
      <namePart type="family">Aubouy</namePart>
      <namePart type="given">Agnès</namePart>
      <role>
        <roleTerm type="text">auteur</roleTerm>
        <roleTerm type="code" authority="marcrelator">aut</roleTerm>
      </role>
      <affiliation>IRD</affiliation>
    </name>
    <name type="personnal">
      <namePart type="family">Migot Nabias</namePart>
      <namePart type="given">Florence</namePart>
      <role>
        <roleTerm type="text">auteur</roleTerm>
        <roleTerm type="code" authority="marcrelator">aut</roleTerm>
      </role>
      <affiliation>IRD</affiliation>
    </name>
    <name type="personnal">
      <namePart type="family">Deloron</namePart>
      <namePart type="given">Philippe</namePart>
      <role>
        <roleTerm type="text">auteur</roleTerm>
        <roleTerm type="code" authority="marcrelator">aut</roleTerm>
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      <languageTerm type="code" authority="iso639-2b">eng</languageTerm>
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    <abstract>Treatment efficacy is related to the interaction of three parameters: drug, parasites, and human factors. The role of human factors in treatment outcome has been poorly documented to date, although human genetic factors and specific immunity have been related to protection against malaria. This study aimed to evaluate a possible cooperation between drug efficacy and host factors in treatment success. The contribution of host factors to treatment efficacy was studied in Gabonese children with a non-severe malaria attack. Children (n = 232) aged under 10 years were treated with either sulfadoxine-pyrimethamine or amodiaquine. The influence of erythrocyte-related genetic factors and humoral immune responses (IgG and subclasses) against MSPI19 on anti-malarial treatment outcome during a 28-day follow-up was studied. Sickle-cell trait carriage and anti-MSPI19 IgG3 levels were related to lower parasite densities at enrolment (multiple linear regression analysis, P &lt;= 0.005). Strikingly, early failures after AQ or SP treatment were associated with decreased anti-MSPI19 IgG, lgG1 and IgG3 levels at enrolment. However, this finding was achieved in a low number of children presenting with an early failure. Kinetics of anti-MSPI19 IgG and subclasses between Days 0 and 28 were also related to treatment efficacy, as the most effective treatment (sulfadoxine-pyrimethamine) was characterised by a higher elevation of antibody titres by Day 28. No effect of erythrocyte-related genetic factors on treatment outcome was shown, although the protective role of sickle-cell trait against higher parasitaemias was confirmed at enrolment. Our data suggest that anti-MSPI19 IgGI may have a supportive role during the first days of treatment to prevent early failures. The interference between drug efficacy, immunity and human genetic factors needs further investigation to be elucidated.</abstract>
    <targetAudience authority="marctarget">specialized</targetAudience>
    <subject>
      <topic>Plasmodium falciparum</topic>
      <topic>treatment efficacy</topic>
      <topic>human genetic factors</topic>
      <topic>anti MSP119 IgG</topic>
    </subject>
    <classification authority="local">052</classification>
    <relatedItem type="host">
      <titleInfo>
        <title>Infection Genetics and Evolution</title>
      </titleInfo>
      <part>
        <detail type="volume">
          <number>7</number>
        </detail>
        <detail type="volume">
          <number>2</number>
        </detail>
        <extent unit="pages">
          <list> 147-154</list>
        </extent>
      </part>
      <originInfo>
        <dateIssued>2007</dateIssued>
      </originInfo>
      <identifier type="issn">1567-1348</identifier>
    </relatedItem>
    <identifier type="uri">https://www.documentation.ird.fr/hor/fdi:010037887</identifier>
    <identifier type="doi">10.1016/j.meegid.2006.07.001</identifier>
    <identifier type="issn">1567-1348</identifier>
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      <shelfLocator>[F A010037887]</shelfLocator>
      <url usage="primary display" access="object in context">https://www.documentation.ird.fr/hor/fdi:010037887</url>
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      <recordContentSource>IRD - Base Horizon / Pleins textes</recordContentSource>
      <recordCreationDate encoding="w3cdtf">2007-04-27</recordCreationDate>
      <recordChangeDate encoding="w3cdtf">2017-08-23</recordChangeDate>
      <recordIdentifier>fdi:010037887</recordIdentifier>
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        <languageTerm authority="iso639-2b">fre</languageTerm>
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