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不同的母体巨细胞病毒特异性中和及Fc受体结合反应对暴露于HIV的新生儿先天性巨细胞病毒传播的影响。

Influence of Distinct Maternal Cytomegalovirus-Specific Neutralizing and Fc Receptor-Binding Responses on Congenital Cytomegalovirus Transmission in HIV-Exposed Neonates.

作者信息

Miller Itzayana G, Mahant Aakash Mahant, Jenks Jennifer A, Semmes Eleanor C, Rochat Eric, Herbek Savannah L, Andy Caroline, Rodgers Nicole S, Pollara Justin, Gerber Linda M, Herold Betsy C, Permar Sallie R

机构信息

Department of Pediatrics, Weill Cornell Medicine, New York, NY 10065, USA.

Immunology and Microbial Pathogenesis Program, Weill Cornell Medicine Graduate School of Medical Sciences, New York, NY 10065, USA.

出版信息

Viruses. 2025 Feb 26;17(3):325. doi: 10.3390/v17030325.

Abstract

Congenital cytomegalovirus (cCMV) is the most common infectious cause of birth defects worldwide, affecting approximately 1 in every 200 live-born infants globally. Recent work has identified potential immune correlates of protection against cCMV transmission including maternal and placentally transferred antibody levels and their function, which may inform the development of maternal active (vaccine) and passive (mono/polyclonal antibody) immunizations. However, these correlates need to also be assessed in diverse cohorts, including women living with HIV who have increased risk of cCMV transmission. Using a case-control design, we investigated whether the magnitude, specificity, function and placental transfer of maternal IgG responses are associated with protection against and/or risk of cCMV transmission in HIV/HCMV co-infection. Within 3 historical cohorts of pregnant women with HIV/HCMV co-infection, we identified 16 cCMV transmitting cases that were matched to 29 cCMV non-transmitting controls. Using a systems serology approach, we found that normalized HCMV-specific IgG binding to FcγR1α was higher in non-transmitting dyads, whereas HCMV-neutralizing antibody responses were higher in transmitting dyads. These findings suggest that engagement of FcγR1α by HCMV-specific IgG may help confer protection against cCMV transmission. Building upon previous research, our study reinforces the critical role of validating maternal humoral immune correlates of cCMV transmission risk across diverse seropositive cohorts, providing essential insights to inform and accelerate the development of effective HCMV vaccines.

摘要

先天性巨细胞病毒(cCMV)是全球范围内出生缺陷最常见的感染原因,全球每200名活产婴儿中约有1人受其影响。最近的研究确定了针对cCMV传播的潜在免疫保护相关因素,包括母体和胎盘转移的抗体水平及其功能,这可能为母体主动(疫苗)和被动(单克隆/多克隆抗体)免疫的发展提供信息。然而,这些相关因素还需要在不同队列中进行评估,包括感染HIV且cCMV传播风险增加的女性。我们采用病例对照设计,研究了HIV/HCMV合并感染的母体IgG反应的强度、特异性、功能和胎盘转移是否与预防cCMV传播及/或cCMV传播风险相关。在3个HIV/HCMV合并感染的孕妇历史队列中,我们确定了16例cCMV传播病例,并与29例cCMV未传播对照进行匹配。我们采用系统血清学方法发现,在未传播组中,标准化的HCMV特异性IgG与FcγR1α的结合更高,而在传播组中,HCMV中和抗体反应更高。这些发现表明,HCMV特异性IgG与FcγR1α的结合可能有助于预防cCMV传播。基于先前的研究,我们的研究强化了在不同血清阳性队列中验证cCMV传播风险的母体体液免疫相关因素的关键作用,为有效HCMV疫苗的研发提供了重要见解并加速其进程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a138/11946089/aa0ac85e15ce/viruses-17-00325-g001.jpg

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