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冠状病毒特异性体液免疫母胎转移中抗体种类形成的模式及功能后果。

Patterns and functional consequences of antibody speciation in maternal-fetal transfer of coronavirus-specific humoral immunity.

作者信息

Hederman Andrew P, Brookes Hannah M, Natarajan Harini, Heyndrickx Leo, Ariën Kevin K, Weiner Joshua A, Rottenstreich Amihai, Zarbiv Gila, Wolf Dana, Goetghebuer Tessa, Marchant Arnaud, Ackerman Margaret E

机构信息

Thayer School of Engineering, Dartmouth College, Hanover, New Hampshire, United States of America.

Department of Immunology and Microbiology, Geisel School of Medicine at Dartmouth, Dartmouth College, Hanover, New Hampshire, United States of America.

出版信息

PLoS Pathog. 2025 Aug 6;21(8):e1013408. doi: 10.1371/journal.ppat.1013408. eCollection 2025 Aug.

Abstract

Maternal antibodies serve as a temporary form of inherited immunity, providing humoral protection to vulnerable neonates. Whereas IgG is actively transferred up a concentration gradient via the neonatal Fc Receptor (FcRn), maternal IgA and IgM are typically excluded from fetal circulation. Further, not all IgG molecules exhibit the same transfer efficiency, being influenced by subclass, Fab and Fc domain glycosylation, antigen-specificity, and the temporal dynamics of maternal antibody responses. Here, we investigate the phenotypes and functions of maternal and cord blood antibodies induced by SARS-CoV-2 infection and compare them to those induced by mRNA vaccination, focusing on breadth of antigen recognition and antiviral functions including neutralization and effector function. While cord blood coronavirus-specific antibody functional breadth and potency appeared to be more compromised than binding breadth and potency in both groups, vaccination induced substantially greater function and breadth in cord blood than did natural infection. These functional phenotypes were associated with speciation of the maternal serum repertoires, as some IgG subpopulations were enriched while others were relatively depleted from cord blood. Relevant to the continued protection of vulnerable infants in the context of a diversifying pathogen, key observations included the greater breadth of antibody effector functions as compared to neutralization, which was associated with greater affinity for antigen and the more efficient placental transfer of IgG subclasses with better affinity to Fc receptors. This work provides new insights into the binding and functional breadth of inherited antibody responses that are likely responsible for the protection of infants born to seropositive mothers from severe SARS-CoV-2 infection despite continued viral diversification.

摘要

母体抗体作为一种遗传免疫的临时形式,为脆弱的新生儿提供体液保护。虽然IgG通过新生儿Fc受体(FcRn)以浓度梯度主动转运,但母体IgA和IgM通常被排除在胎儿循环之外。此外,并非所有IgG分子都表现出相同的转运效率,其受到亚类、Fab和Fc结构域糖基化、抗原特异性以及母体抗体反应的时间动态影响。在这里,我们研究了由SARS-CoV-2感染诱导的母体和脐带血抗体的表型和功能,并将它们与mRNA疫苗诱导的表型和功能进行比较,重点关注抗原识别广度和抗病毒功能,包括中和作用和效应功能。虽然在两组中,脐带血冠状病毒特异性抗体的功能广度和效力似乎比结合广度和效力更受影响,但与自然感染相比,疫苗接种在脐带血中诱导出的功能和广度要大得多。这些功能表型与母体血清库的种类形成有关,因为一些IgG亚群在脐带血中富集,而另一些则相对减少。在病原体多样化的背景下,与持续保护脆弱婴儿相关的关键观察结果包括,与中和作用相比,抗体效应功能的广度更大,这与对抗原的更高亲和力以及对Fc受体亲和力更好的IgG亚类更有效的胎盘转运有关。这项工作为遗传抗体反应的结合和功能广度提供了新的见解,这些反应可能是导致血清反应阳性母亲所生婴儿免受严重SARS-CoV-2感染的原因,尽管病毒持续多样化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e439/12349702/eb5790848b84/ppat.1013408.g001.jpg

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