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快速诱导 SIV Env 特异性黏膜和血清抗体可增强细胞免疫,从而保护免疫的精英控制猕猴免受高剂量异源 SIV 挑战。

Rapid SIV Env-specific mucosal and serum antibody induction augments cellular immunity in protecting immunized, elite-controller macaques against high dose heterologous SIV challenge.

机构信息

Vaccine Branch, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Virology. 2011 Mar 1;411(1):87-102. doi: 10.1016/j.virol.2010.12.033. Epub 2011 Jan 14.

DOI:10.1016/j.virol.2010.12.033
PMID:21237474
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3039060/
Abstract

Three Indian rhesus macaques, Ad-SIV primed/protein boosted and exposed twice to high-dose mucosal SIV(mac251) challenges, exhibited elite control of viremia over 6.5 years. They were negative for host factors associated with control of SIV infection. After a third intrarectal challenge with SIV(smE660), all controlled viremia, with one (macaque #5) maintaining undetectable viremia in blood. Acquisition was not blocked, but virus was contained in the jejunum and draining lymph nodes. Polyfunctional memory T cell responses and high-titered neutralizing and non-neutralizing serum and mucosal antibodies were present before and maintained post-challenge. The level of protection seen for animal #5 was predicted from analyses of gene transcription in jejunum 2 weeks post-challenge. Macaques #7 and #9, exhibiting lower pre-challenge cellular and humoral immunity, partially controlled the SIV(smE660) challenge. Initial vaccine-induced control by macaque #5 extended to the SIV(smE660) challenge due to multiple immune mechanisms that were boosted and augmented by cryptic SIV exposure.

摘要

三只印度食蟹猕猴,经 SIV 疫苗 primed/protein boosted 并两次暴露于高剂量黏膜 SIV(mac251)挑战,在超过 6.5 年的时间里表现出对病毒血症的精英控制。它们没有与控制 SIV 感染相关的宿主因素。在第三次直肠内 SIV(smE660)挑战后,所有猕猴均控制了病毒血症,其中一只(猕猴 #5)在血液中保持无法检测到的病毒血症。虽然病毒没有被完全阻断,但它被局限在空肠和引流淋巴结中。在挑战前和挑战后,多功能记忆 T 细胞反应以及高滴度的中和和非中和血清和黏膜抗体均存在。从挑战后 2 周空肠的基因转录分析中预测了动物 #5 的保护水平。猕猴 #7 和 #9,表现出较低的细胞和体液免疫前,部分控制了 SIV(smE660)挑战。由于多种免疫机制被增强和放大,猕猴 #5 最初由疫苗诱导的控制扩展到 SIV(smE660)挑战。

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