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疟疾易感性:IgG3 Gm 同种异型和 Fcγ 受体 IIA、IIIA 和 IIIB 联合多态性的影响。

Susceptibility to Malaria: Influence of Combined Polymorphisms of IgG3 Gm Allotypes and Fc Gamma Receptors IIA, IIIA, and IIIB.

机构信息

Université de Paris, Institut de Recherche pour le Développement (IRD), UMR 261 MERIT, Paris, France.

CNRS UMR 5288 Laboratoire d'Anthropologie Moléculaire et d'Imagerie de Synthèse (AMIS), Université Paul Sabatier Toulouse III, Toulouse, France.

出版信息

Front Immunol. 2020 Dec 23;11:608016. doi: 10.3389/fimmu.2020.608016. eCollection 2020.

Abstract

The binding of immunoglobulin (Ig) to Fc gamma receptors (FcgR) at the immune cell surface is an important step to initiate immunological defense against malaria. However, polymorphisms in receptors and/or constant regions of the IgG heavy chains may modulate this binding. Here, we investigated whether polymorphisms located in FcgR and constant regions of the heavy chain of IgG are associated with susceptibility to malaria. For this purpose, a clinical and parasitological follow-up on malaria was conducted among 656 infants in southern Benin. G3m allotypes (from total IgG3) were determined by a serological method of hemagglutination inhibition. FcgRIIA 131R/H and FcgRIIIA 176F/V genotypes were determined using the TaqMan method and FcgRIIIB NA1/NA2 genotypes were assessed by polymerase chain reaction using allele-specific primers. Association analyses between the number of malaria infections during the follow-up and polymorphisms in IgG G3m allotypes and FcgR were studied independently by zero inflated binomial negative regression. The influence of combinations of G3m allotypes and FcgRIIA/FcgRIIIA/FcgRIIIB polymorphisms on the number of infections, and their potential interaction with environmental exposure to malaria was assessed by using the generalized multifactor dimensionality reduction (GMDR) method. Results showed that individual carriage of G3m24 single allotype and of G3m5,6,10,11,13,14,24 phenotype was independently associated with a high risk of malaria infection. A risk effect for G3m6 was observed only under high environmental exposure. FcgRIIIA 176VV single genotype and combined carriage of FcgRIIA 131RH/FcgRIIIA 176VV/FcgRIIIB NA1NA2, FcgRIIA 131HH/FcgRIIIA 176FF/FcgRIIIB NA1NA1, FcgRIIA 131HH/FcgRIIIA 176VV/FcgRIIIB NA2NA2 and FcgRIIA 131HH/FcgRIIIA 176VV/FcgRIIIB NA1NA2 genotypes were related to a high number of malaria infections. The risk was accentuated for FcgRIIIA 176VV when considering the influence of environmental exposure to malaria. Finally, the GMDR analysis including environmental exposure showed strengthened associations with a malaria risk when FcgRIIA/FcgRIIIA/FcgRIIIB genotypes were combined to G3m5,6,11,24 and G3m5,6,10,11,13,15,24 phenotypes or G3m10 and G3m13 single allotypes. Our results highlight the relevance of studying IgG heavy chain and FcgR polymorphisms, independently as well as in combination, in relation to the individual susceptibility to infection. The intensity of individual exposure to mosquito bites was demonstrated to impact the relationships found.

摘要

免疫球蛋白(Ig)与免疫细胞表面 Fc 受体(FcgR)的结合是启动针对疟疾的免疫防御的重要步骤。然而,受体和/或 IgG 重链恒定区的多态性可能会调节这种结合。在这里,我们研究了 FcgR 和 IgG 重链恒定区中位于的多态性是否与疟疾易感性有关。为此,我们在贝宁南部对 656 名婴儿进行了疟疾的临床和寄生虫学随访。通过红细胞凝集抑制的血清学方法确定 G3m 同种型(来自总 IgG3)。使用 TaqMan 方法确定 FcgRIIA 131R/H 和 FcgRIIIA 176F/V 基因型,使用等位基因特异性引物的聚合酶链反应评估 FcgRIIIB NA1/NA2 基因型。通过零膨胀二项负回归,分别独立研究 IgG G3m 同种型和 FcgR 之间的随访期间疟疾感染次数与多态性之间的关联。使用广义多因素降维(GMDR)方法评估 G3m 同种型和 FcgRIIA/FcgRIIIA/FcgRIIIB 多态性组合对感染数量的影响及其与疟疾环境暴露的潜在相互作用。结果表明,携带 G3m24 单一同种型和 G3m5、6、10、11、13、14、24 表型的个体,疟疾感染的风险独立增加。仅在高环境暴露下才观察到 G3m6 的风险效应。FcgRIIIA 176VV 单一基因型以及 FcgRIIA 131RH/FcgRIIIA 176VV/FcgRIIIB NA1NA2、FcgRIIA 131HH/FcgRIIIA 176FF/FcgRIIIB NA1NA1、FcgRIIA 131HH/FcgRIIIA 176VV/FcgRIIIB NA2NA2 和 FcgRIIA 131HH/FcgRIIIA 176VV/FcgRIIIB NA1NA2 基因型与疟疾感染数量增加有关。当考虑到疟疾环境暴露的影响时,FcgRIIIA 176VV 的风险会增加。最后,当将 FcgRIIA/FcgRIIIA/FcgRIIIB 基因型与 G3m5、6、11、24 和 G3m5、6、10、11、13、15、24 表型或 G3m10 和 G3m13 单一同种型结合,并纳入环境暴露因素的 GMDR 分析显示,与疟疾风险的关联得到了加强。我们的结果强调了研究 IgG 重链和 FcgR 多态性的相关性,包括独立研究以及组合研究,与个体对感染的易感性有关。个体暴露于蚊子叮咬的强度被证明会影响所发现的关系。

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