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High Cell-Free Virus Load and Robust Autologous Humoral Immune Responses in Breast Milk of Simian Immunodeficiency Virus-Infected African Green Monkeys

机译:猿猴免疫缺陷病毒感染非洲绿猴的母乳中的高无细胞病毒载量和强大的自体体液免疫反应

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摘要

The design of immunologic interventions to prevent postnatal transmission of human immunodeficiency virus (HIV) will require identification of protective immune responses in this setting. Simian immunodeficiency virus (SIV)-infected rhesus monkeys (RMs), a species that develops an AIDS-like illness following experimental infection, transmit the virus at a high rate during breastfeeding. In contrast, postnatal transmission of SIV occurs rarely or not at all in natural, asymptomatic primate hosts of SIV. These contrasting transmission patterns provide a unique opportunity to study mechanisms that evolved to protect suckling infants from SIV infection. We compared the virologic and immunologic properties of milk of SIV-infected and uninfected natural hosts of SIV, African green monkeys (AGMs), to that of RMs. Interestingly, despite a low number of milk CD4+ T lymphocytes in uninfected AGMs, milk virus RNA load in SIV-infected AGMs was comparable to that of SIV-infected RMs and that in AGM plasma. This observation is in contrast to the relatively low virus load in milk compared to that in plasma of SIV-infected RMs and HIV-infected women. Milk of SIV-infected AGMs also displayed robust virus-specific cellular immune responses. Importantly, an autologous challenge virus-specific neutralization response was detected in milk of five of six SIV-infected AGMs that was comparable in magnitude to that in plasma. In contrast, autologous challenge virus neutralization was not detectable in milk of SIV-infected RMs. The autologous virus-specific adaptive immune responses in breast milk of AGMs may contribute to impedance of virus transmission in the infant oral/gastrointestinal tract and the rarity of postnatal virus transmission in natural hosts of SIV.
机译:为防止出生后人类免疫缺陷病毒(HIV)传播的免疫干预措施的设计,需要在这种情况下鉴定保护性免疫应答。受猿猴免疫缺陷病毒(SIV)感染的恒河猴(RM),是一种在实验性感染后会发展成AIDS样疾病的物种,在母乳喂养期间会以很高的速度传播该病毒。相反,在自然,无症状的SIV宿主中,SIV的产后传播很少或根本没有发生。这些截然不同的传播方式为研究为保护哺乳期婴儿免受SIV感染而进化的机制提供了独特的机会。我们比较了SIV感染和未感染的SIV自然宿主(非洲绿猴(AGM))与RM的牛奶的病毒学和免疫学特性。有趣的是,尽管未感染的AGM中的牛奶CD4 + T淋巴细胞数量很少,但SIV感染的AGM中的牛奶病毒RNA载量与SIV感染的RM和血浆中的RM相当。该观察结果与牛奶中的病毒载量相对较低,而牛奶中的病毒载量与SIV感染的RM和HIV感染的女性血浆中的病毒载量相比较低。被SIV感染的AGM的牛奶也表现出强大的病毒特异性细胞免疫反应。重要的是,在牛奶中检测到六种SIV感染的AGM中有五种发生了自体攻击病毒特异性中和反应,其大小与血浆相当。相反,在牛奶中未检测到自体激发病毒中和的SIV感染RM。 AGMs母乳中的自体病毒特异性适应性免疫应答可能会导致婴儿口腔/胃肠道中病毒传播的阻抗增加,以及SIV天然宿主中出生后病毒传播的罕见性。

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