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红细胞表面的自然选择。

Natural selection on the erythrocyte surface.

作者信息

Baum Jake, Ward Ryk H, Conway David J

机构信息

Department of Infectious and Tropical Diseases, London School of Hygiene and Tropical Medicine. Institute of Biological Anthropology, University of Oxford.

出版信息

Mol Biol Evol. 2002 Mar;19(3):223-9. doi: 10.1093/oxfordjournals.molbev.a004075.

Abstract

Surface glycoproteins are principal receptors used by pathogens to invade target cells. It has been suggested that mammalian erythrocyte surface glycoproteins function as decoy receptors attracting pathogens to the anucleated erythrocyte and away from their target tissues. Glycophorin A (GYPA) is solely expressed on the erythrocyte surface where it is the most abundant sialoglycoprotein, although its function is unknown. The pathogen decoy hypothesis may be relevant here, as GYPA has been shown in vitro to bind numerous viruses and bacteria, which do not infect erythrocytes. However, it is also a receptor for erythrocyte invasion by the malarial parasite Plasmodium falciparum. Analyses of gypa sequence variation among six higher primates and within a human population show that there is a large excess of replacement (nonsynonymous) substitutions along each primate lineage (particularly on exons 2-4 encoding the extracellular glycosylated domain of GYPA) and a significant excess of polymorphisms in exon 2 (encoding the terminal portion of the extracellular domain) within humans. These two signatures suggest that there has been exceptionally strong positive selection on this receptor driving GYPA divergence during primate evolution and balancing selection maintaining allelic variation within human populations. The pathogen decoy hypothesis alone is adequate to explain both these signatures of between-species and within-species diversifying selection. This has implications for understanding the functions of erythrocyte surface components and their roles in health and disease.

摘要

表面糖蛋白是病原体用来侵入靶细胞的主要受体。有人提出,哺乳动物红细胞表面糖蛋白起着诱饵受体的作用,将病原体吸引到无核红细胞,使其远离靶组织。血型糖蛋白A(GYPA)仅在红细胞表面表达,是红细胞表面最丰富的唾液酸糖蛋白,但其功能尚不清楚。病原体诱饵假说可能适用于此,因为体外研究表明GYPA能结合多种病毒和细菌,而这些病原体并不感染红细胞。然而,它也是疟原虫恶性疟原虫侵入红细胞的受体。对六种高等灵长类动物以及人类群体中gypa序列变异的分析表明,每个灵长类谱系中都有大量的替换(非同义)突变(特别是在编码GYPA细胞外糖基化结构域的外显子2-4上),并且人类外显子2(编码细胞外结构域的末端部分)中的多态性显著过量。这两个特征表明,在灵长类动物进化过程中,该受体受到了异常强烈的正选择,推动了GYPA的分化;而在人类群体中,则存在平衡选择以维持等位基因变异。仅病原体诱饵假说就足以解释种间和种内多样化选择的这两个特征。这对于理解红细胞表面成分的功能及其在健康和疾病中的作用具有重要意义。

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