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低传播环境下恶性疟原虫和间日疟原虫抗体的母婴转移

Maternal-foetal transfer of Plasmodium falciparum and Plasmodium vivax antibodies in a low transmission setting.

作者信息

Charnaud Sarah C, McGready Rose, Herten-Crabb Asha, Powell Rosanna, Guy Andrew, Langer Christine, Richards Jack S, Gilson Paul R, Chotivanich Kesinee, Tsuboi Takafumi, Narum David L, Pimanpanarak Mupawjay, Simpson Julie A, Beeson James G, Nosten François, Fowkes Freya J I

机构信息

Macfarlane Burnet Institute of Medical Research, Melbourne, Australia.

Shoklo Malaria Research Unit, Mahidol-Oxford Tropical Medicine Research Unit, Faculty of Tropical Medicine, Mahidol University, Mae Sot, Thailand.

出版信息

Sci Rep. 2016 Feb 10;6:20859. doi: 10.1038/srep20859.

Abstract

During pregnancy immunoglobulin G (IgG) antibodies are transferred from mother to neonate across the placenta. Studies in high transmission areas have shown transfer of P. falciparum-specific IgG, but the extent and factors influencing maternal-foetal transfer in low transmission areas co-endemic for both P. falciparum and P. vivax are unknown. Pregnant women were screened weekly for Plasmodium infection. Mother-neonate paired serum samples at delivery were tested for IgG to antigens from P. falciparum, P. vivax and other infectious diseases. Antibodies to malarial and non-malarial antigens were highly correlated between maternal and neonatal samples (median [range] spearman ρ = 0.78 [0.57-0.93]), although Plasmodium spp. antibodies tended to be lower in neonates than mothers. Estimated gestational age at last P. falciparum infection, but not P. vivax infection, was positively associated with antibody levels in the neonate (P. falciparum merozoite, spearman ρ median [range] 0.42 [0.33-0.66], PfVAR2CSA 0.69; P. vivax ρ = 0.19 [0.09-0.3]). Maternal-foetal transfer of anti-malarial IgG to Plasmodium spp. antigens occurs in low transmission settings. P. vivax IgG acquisition is not associated with recent exposure unlike P. falciparum IgG, suggesting a difference in acquisition of antibodies. IgG transfer is greatest in the final weeks of pregnancy which has implications for the timing of future malaria vaccination strategies in pregnant women.

摘要

在孕期,免疫球蛋白G(IgG)抗体通过胎盘从母亲转移至新生儿体内。在高传播地区开展的研究已表明恶性疟原虫特异性IgG会发生转移,但在同时存在恶性疟原虫和间日疟原虫的低传播地区,母婴转移的程度及影响因素尚不清楚。对孕妇每周进行疟原虫感染筛查。在分娩时采集母婴配对的血清样本,检测针对恶性疟原虫、间日疟原虫及其他传染病抗原的IgG。母婴样本中针对疟疾和非疟疾抗原的抗体高度相关(中位数[范围]斯皮尔曼ρ = 0.78[0.57 - 0.93]),不过疟原虫属抗体在新生儿中往往低于母亲。末次感染恶性疟原虫而非间日疟原虫时的估计孕周与新生儿抗体水平呈正相关(恶性疟原虫裂殖子,斯皮尔曼ρ中位数[范围]0.42[0.33 - 0.66],PfVAR2CSA为0.69;间日疟原虫ρ = 0.19[0.09 - 0.3])。在低传播环境中会发生抗疟疾IgG从母亲到胎儿的转移。与恶性疟原虫IgG不同,间日疟原虫IgG的获得与近期暴露无关,这表明抗体获得存在差异。IgG转移在妊娠最后几周最为显著,这对未来孕妇疟疾疫苗接种策略的时机具有启示意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4875/4748262/380aef23eb83/srep20859-f1.jpg

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