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针对棒状体相关膜抗原的抗体可预测对恶性疟原虫的抗性。

Antibodies to rhoptry-associated membrane antigen predict resistance to Plasmodium falciparum.

作者信息

Nixon Christian P, Friedman Jennifer, Treanor Kristina, Knopf Paul M, Duffy Patrick E, Kurtis Jonathan D

机构信息

International Health Institute, Brown University, Providence, Rhode Island 02912, USA.

出版信息

J Infect Dis. 2005 Sep 1;192(5):861-9. doi: 10.1086/432550. Epub 2005 Jul 29.

Abstract

Previously, we collected plasma from 143 male volunteers residing in an area of western Kenya where Plasmodium falciparum is holoendemic. Volunteers were cured of current malaria infection by use of drugs, blood was collected 2 weeks after treatment, and blood films were collected weekly for 18 weeks. We identified and pooled plasma from the 10 most resistant individuals (RP) and the 7 most susceptible individuals (SP) and used these pools in a differential screen of a P. falciparum cDNA expression library. We screened 550,000 clones and identified 7 clones that were uniquely recognized by RP but not by SP. Two clones encoded a C-terminal region polypeptide from rhoptry-associated membrane antigen (RAMA-pr), a recently described RAMA. We measured anti-RAMA-pr antibody levels in plasma obtained 2 weeks after treatment. Individuals with detectable immunoglobulin G1 anti-RAMA-pr (n = 24) had fewer positive blood films (odds ratio, 1.7 [95% confidence interval, 1.21-2.44]; P < .003), 43% lower density of parasitemia (P < .02), and prolonged time to reinfection (P < .0027), compared with individuals without detectable antibody levels (n = 115), after known determinants of resistance were accounted for. In summary, RAMA-pr is a rationally identified vaccine candidate that is preferentially recognized by antibodies produced by humans with a high level of naturally acquired resistance to P. falciparum infection.

摘要

此前,我们从居住在肯尼亚西部一个恶性疟原虫高度流行地区的143名男性志愿者身上采集了血浆。志愿者通过药物治愈了当前的疟疾感染,在治疗后2周采集血液,并在18周内每周采集血涂片。我们从10名抗性最强的个体(RP)和7名易感性最强的个体(SP)中鉴定并汇集了血浆,并将这些血浆池用于恶性疟原虫cDNA表达文库的差异筛选。我们筛选了550,000个克隆,鉴定出7个仅被RP识别而不被SP识别的克隆。两个克隆编码来自最近描述的一种与棒状体相关膜抗原(RAMA-pr)的C末端区域多肽。我们测量了治疗后2周获得的血浆中抗RAMA-pr抗体水平。与抗体水平不可检测的个体(n = 115)相比,在考虑了已知的抗性决定因素后,可检测到免疫球蛋白G1抗RAMA-pr的个体(n = 24)的阳性血涂片较少(优势比,1.7 [95%置信区间,1.21 - 2.44];P <.003),寄生虫血症密度低43%(P <.02),再感染时间延长(P <.0027)。总之,RAMA-pr是一种经过合理鉴定的疫苗候选物,优先被对恶性疟原虫感染具有高水平自然获得性抗性的人产生的抗体识别。

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