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首页> 外文期刊>Scandinavian journal of immunology. >Determinants of variant surface antigen antibody response in severe Plasmodium falciparum malaria in an area of low and unstable malaria transmission.
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Determinants of variant surface antigen antibody response in severe Plasmodium falciparum malaria in an area of low and unstable malaria transmission.

机译:在疟疾传播低且不稳定的地区,严重恶性疟原虫疟疾中各种表面抗原抗体应答的决定因素。

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摘要

The variant surface antigens (VSA) of infected erythrocytes are important pathogenic markers, a set of variants (VSA(SM)), were assumed to be associated with severe malaria (SM), while SM constitutes clinically diverse forms, such as, severe malarial anemia (SMA) and cerebral malaria (CM). This study was conducted in Eastern Sudan, an area of seasonal and unstable malaria transmission. Parasites and plasma were obtained from patients with different clinical grades of malaria, and flow cytometry was used for analysis of VSA antibody (Ab) response. We found that individuals recognized a broader range of isolates had a higher level of VSA Ab against the recognized isolates (correlation coefficient, 0.727, P<0.001). Unexpectedly, at the time of malaria diagnosis, plasma from patients with CM recognized a significantly larger number of isolates than did the plasma from patients with SMA (P<0.001). Parasites obtained from patients with SMA or from children were better recognized than isolates obtained from patients with uncomplicated malaria or from adults, P<0.001, P=0.021, respectively. Taken together, the above findings suggest that the limitations in the VSA immunoglobulin G repertoire were most probably contributing to the pathogenesis of SMA but not to that of CM.
机译:被感染红细胞的变异表面抗原(VSA)是重要的致病标记,一组变异(VSA(SM))被认为与严重疟疾(SM)相关,而SM构成临床上多种形式,例如严重疟疾贫血(SMA)和脑疟疾(CM)。这项研究是在苏丹东部(季节性和不稳定疟疾传播地区)进行的。从具有不同临床等级的疟疾的患者中获取寄生虫和血浆,并使用流式细胞仪分析VSA抗体(Ab)反应。我们发现,认识到更广泛的分离株的个体相对于公认的分离株具有更高水平的VSA Ab(相关系数,0.727,P <0.001)。出乎意料的是,在进行疟疾诊断时,来自CM患者的血浆比来自SMA患者的血浆能识别出更多的分离株(P <0.001)。从SMA患者或儿童中获得的寄生虫比从单纯性疟疾患者或成人中获得的分离物更好地被识别,分别为P <0.001,P = 0.021。综上所述,以上发现表明,VSA免疫球蛋白G库的局限性很可能是SMA的发病机理,而不是CM的发病机理。

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