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在感染动物源性泡沫病毒的人类中发现的强效中和抗体针对位于表面包膜蛋白二聚体结构域中的保守表位。

Potent neutralizing antibodies in humans infected with zoonotic simian foamy viruses target conserved epitopes located in the dimorphic domain of the surface envelope protein.

机构信息

Unité d'Épidémiologie et Physiopathologie des Virus Oncogènes, Institut Pasteur, Paris, France.

UMR CNRS 3569, Institut Pasteur, Paris, France.

出版信息

PLoS Pathog. 2018 Oct 8;14(10):e1007293. doi: 10.1371/journal.ppat.1007293. eCollection 2018 Oct.

Abstract

Human diseases of zoonotic origin are a major public health problem. Simian foamy viruses (SFVs) are complex retroviruses which are currently spilling over to humans. Replication-competent SFVs persist over the lifetime of their human hosts, without spreading to secondary hosts, suggesting the presence of efficient immune control. Accordingly, we aimed to perform an in-depth characterization of neutralizing antibodies raised by humans infected with a zoonotic SFV. We quantified the neutralizing capacity of plasma samples from 58 SFV-infected hunters against primary zoonotic gorilla and chimpanzee SFV strains, and laboratory-adapted chimpanzee SFV. The genotype of the strain infecting each hunter was identified by direct sequencing of the env gene amplified from the buffy coat with genotype-specific primers. Foamy virus vector particles (FVV) enveloped by wild-type and chimeric gorilla SFV were used to map the envelope region targeted by antibodies. Here, we showed high titers of neutralizing antibodies in the plasma of most SFV-infected individuals. Neutralizing antibodies target the dimorphic portion of the envelope protein surface domain. Epitopes recognized by neutralizing antibodies have been conserved during the cospeciation of SFV with their nonhuman primate host. Greater neutralization breadth in plasma samples of SFV-infected humans was statistically associated with smaller SFV-related hematological changes. The neutralization patterns provide evidence for persistent expression of viral proteins and a high prevalence of coinfection. In conclusion, neutralizing antibodies raised against zoonotic SFV target immunodominant and conserved epitopes located in the receptor binding domain. These properties support their potential role in restricting the spread of SFV in the human population.

摘要

人畜共患病是一个主要的公共卫生问题。猴泡沫病毒(SFV)是一种复杂的逆转录病毒,目前正在溢出到人类中。复制能力强的 SFV 在其人类宿主的一生中持续存在,而不会传播给次级宿主,这表明存在有效的免疫控制。因此,我们旨在对感染人畜共患 SFV 的人类产生的中和抗体进行深入表征。我们量化了 58 名 SFV 感染猎人的血浆样本对原发性人猿和黑猩猩 SFV 株以及实验室适应的黑猩猩 SFV 的中和能力。通过使用针对 env 基因的特异性引物从 buffy coat 中扩增,用直接测序鉴定感染每个猎人的毒株的基因型。用野生型和嵌合大猩猩 SFV 包裹的泡沫病毒载体颗粒(FVV)用于定位抗体靶向的包膜区域。在这里,我们显示了大多数 SFV 感染个体的血浆中中和抗体的高滴度。中和抗体针对包膜蛋白表面结构域的二态部分。在 SFV 与其非人类灵长类宿主共同进化过程中,中和抗体识别的表位得到了保守。SFV 感染人类的血浆样本中更大的中和广度在统计学上与较小的 SFV 相关的血液学变化相关。中和模式为病毒蛋白的持续表达和高比例的合并感染提供了证据。总之,针对人畜共患 SFV 产生的中和抗体针对位于受体结合域的免疫显性和保守表位。这些特性支持它们在限制 SFV 在人类中的传播中的潜在作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ffc0/6193739/cd7f2cd32191/ppat.1007293.g001.jpg

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