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免疫调节性妊娠特异性糖蛋白进化迅速,它们的存在与灵长类动物的血绒毛膜胎盘形成相关。

The immune-modulating pregnancy-specific glycoproteins evolve rapidly and their presence correlates with hemochorial placentation in primates.

作者信息

Zimmermann Wolfgang, Kammerer Robert

机构信息

Tumor Immunology Laboratory, LIFE Center, Department of Urology, University Hospital, LMU Munich, Germany.

Institute of Immunology, Friedrich-Loeffler-Institut, Federal Research Institute for Animal Health, Greifswald, Insel Riems, Germany.

出版信息

BMC Genomics. 2021 Feb 18;22(1):128. doi: 10.1186/s12864-021-07413-8.

Abstract

BACKGROUND

Pregnancy-specific glycoprotein (PSG) genes belong to the carcinoembryonic antigen (CEA) gene family, within the immunoglobulin gene superfamily. In humans, 10 PSG genes encode closely related secreted glycoproteins. They are exclusively expressed in fetal syncytiotrophoblast cells and represent the most abundant fetal proteins in the maternal blood. In recent years, a role in modulation of the maternal immune system possibly to avoid rejection of the semiallogeneic fetus and to facilitate access of trophoblast cells to maternal resources via the blood system has been suggested. Alternatively, they could serve as soluble pathogen decoy receptors like other members of the CEA family. Despite their clearly different domain organization, similar functional properties have also been observed for murine and bat PSG. As these species share a hemochorial type of placentation and a seemingly convergent formation of PSG genes during evolution, we hypothesized that hemochorial placentae support the evolution of PSG gene families.

RESULTS

To strengthen this hypothesis, we have analyzed PSG genes in 57 primate species which exhibit hemochorial or epitheliochorial placentation. In nearly all analyzed apes some 10 PSG genes each could be retrieved from genomic databases, while 6 to 24 PSG genes were found in Old World monkey genomes. Surprisingly, only 1 to 7 PSG genes could be identified in New World monkeys. Interestingly, no PSG genes were found in more distantly related primates with epitheliochorial placentae like lemurs and lorises. The exons encoding the putative receptor-binding domains exhibit strong selection for diversification in most primate PSG as revealed by rapid loss of orthologous relationship during evolution and high ratios of nonsynonymous and synonymous mutations.

CONCLUSION

The distribution of trophoblast-specific PSGs in primates and their pattern of selection supports the hypothesis that PSG are still evolving to optimize fetal-maternal or putative pathogen interactions in mammals with intimate contact of fetal cells with the immune system of the mother like in hemochorial placentation.

摘要

背景

妊娠特异性糖蛋白(PSG)基因属于癌胚抗原(CEA)基因家族,位于免疫球蛋白基因超家族内。在人类中,10个PSG基因编码密切相关的分泌型糖蛋白。它们仅在胎儿合体滋养层细胞中表达,是母血中最丰富的胎儿蛋白。近年来,有人提出其在调节母体免疫系统中发挥作用,可能是为了避免对半同种异体胎儿的排斥,并促进滋养层细胞通过血液系统获取母体资源。或者,它们可以像CEA家族的其他成员一样作为可溶性病原体诱饵受体。尽管它们的结构域组织明显不同,但在小鼠和蝙蝠的PSG中也观察到了类似的功能特性。由于这些物种在进化过程中共享血绒毛膜型胎盘形成以及PSG基因看似趋同的形成,我们推测血绒毛膜胎盘支持PSG基因家族的进化。

结果

为了强化这一假设,我们分析了57种具有血绒毛膜或上皮绒毛膜胎盘的灵长类物种中的PSG基因。在几乎所有分析的猿类中,每个基因组数据库中都能检索到约10个PSG基因,而在旧世界猴基因组中发现了6至24个PSG基因。令人惊讶的是,在新世界猴中仅能鉴定出1至7个PSG基因。有趣的是,在关系更远的具有上皮绒毛膜胎盘的灵长类动物如狐猴和懒猴中未发现PSG基因。编码假定受体结合域的外显子在大多数灵长类PSG中表现出强烈的多样化选择,这在进化过程中直系同源关系的快速丧失以及非同义突变与同义突变的高比例中得以体现。

结论

滋养层特异性PSG在灵长类中的分布及其选择模式支持了以下假设:在具有胎儿细胞与母体免疫系统密切接触的哺乳动物中,如血绒毛膜胎盘形成的情况下,PSG仍在不断进化以优化胎儿 - 母体或假定的病原体相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/29d0/7893922/82a300048c49/12864_2021_7413_Fig1_HTML.jpg

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