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预先存在的抗体可预防猴子的先天性巨细胞病毒感染。

Preexisting antibodies can protect against congenital cytomegalovirus infection in monkeys.

作者信息

Nelson Cody S, Cruz Diana Vera, Tran Dollnovan, Bialas Kristy M, Stamper Lisa, Wu Huali, Gilbert Margaret, Blair Robert, Alvarez Xavier, Itell Hannah, Chen Meng, Deshpande Ashlesha, Chiuppesi Flavia, Wussow Felix, Diamond Don J, Vandergrift Nathan, Walter Mark R, Barry Peter A, Cohen-Wolkowiez Michael, Koelle Katia, Kaur Amitinder, Permar Sallie R

机构信息

Human Vaccine Institute, Duke University School of Medicine, and.

Department of Biology, Duke University, Durham, North Carolina, USA.

出版信息

JCI Insight. 2017 Jul 6;2(13). doi: 10.1172/jci.insight.94002.

Abstract

Human cytomegalovirus (HCMV) is the most common congenital infection and a known cause of microcephaly, sensorineural hearing loss, and cognitive impairment among newborns worldwide. Natural maternal HCMV immunity reduces the incidence of congenital infection, but does not prevent the disease altogether. We employed a nonhuman primate model of congenital CMV infection to investigate the ability of preexisting antibodies to protect against placental CMV transmission in the setting of primary maternal infection and subsequent viremia, which is required for placental virus exposure. Pregnant, CD4+ T cell-depleted, rhesus CMV-seronegative (RhCMV-seronegative) rhesus monkeys were treated with either standardly produced hyperimmune globulin (HIG) from RhCMV-seropositive macaques or dose-optimized, potently RhCMV-neutralizing HIG prior to intravenous challenge with an RhCMV mixture. HIG passive infusion provided complete protection against fetal loss in both groups. The dose-optimized, RhCMV-neutralizing HIG additionally inhibited placental transmission of RhCMV and reduced viral replication and diversity. Our findings suggest that the presence of durable and potently neutralizing antibodies at the time of primary infection can prevent transmission of systemically replicating maternal RhCMV to the developing fetus, and therefore should be a primary target of vaccines to eliminate this neonatal infection.

摘要

人巨细胞病毒(HCMV)是最常见的先天性感染病原体,也是全球范围内新生儿小头畸形、感音神经性听力损失和认知障碍的已知病因。母体自然获得的HCMV免疫力可降低先天性感染的发生率,但不能完全预防该病。我们采用先天性CMV感染的非人灵长类动物模型,研究在原发性母体感染及随后的病毒血症(胎盘病毒暴露所必需)情况下,预先存在的抗体预防胎盘CMV传播的能力。对怀孕的、CD4 + T细胞耗竭的、恒河猴巨细胞病毒血清阴性(RhCMV血清阴性)的恒河猴,在静脉注射RhCMV混合物进行攻击之前,用来自RhCMV血清阳性猕猴的标准生产的高效价免疫球蛋白(HIG)或剂量优化的、强效RhCMV中和HIG进行治疗。HIG被动输注在两组中均提供了完全的胎儿丢失保护。剂量优化的、RhCMV中和HIG还抑制了RhCMV的胎盘传播,并减少了病毒复制和多样性。我们的研究结果表明,原发性感染时存在持久且强效中和的抗体可预防全身复制的母体RhCMV传播给发育中的胎儿,因此应成为消除这种新生儿感染的疫苗的主要靶点。

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