首页> 美国卫生研究院文献>Journal of Virology >Signature for Long-Term Vaccine-Mediated Control of a Simian and Human Immunodeficiency Virus 89.6P Challenge: Stable Low-Breadth and Low-Frequency T-Cell Response Capable of Coproducing Gamma Interferon and Interleukin-2
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Signature for Long-Term Vaccine-Mediated Control of a Simian and Human Immunodeficiency Virus 89.6P Challenge: Stable Low-Breadth and Low-Frequency T-Cell Response Capable of Coproducing Gamma Interferon and Interleukin-2

机译:猿和人类免疫缺陷病毒89.6P挑战的长期疫苗介导控制的签名:稳定的低广度和低频T细胞反应能力可同时产生γ干扰素和白介素-2。

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摘要

In 2001, we reported 20 weeks of control of challenge with the virulent 89.6P chimera of simian and human immunodeficiency viruses (SHIV-89.6P) by a Gag-Pol-Env vaccine consisting of DNA priming and modified vaccinia virus Ankara boosting. Here we report that 22 out of 23 of these animals successfully controlled their viremia until their time of euthanasia at 200 weeks postchallenge. At euthanasia, all animals had low to undetectable viral loads and normal CD4 counts. During the long period of viral control, gamma interferon (IFN-γ)-producing antiviral T cells were present at unexpectedly low breadths and frequencies. Most animals recognized two CD8 and one CD4 epitope and had frequencies of IFN-γ-responding T cells from 0.01 to 0.3% of total CD8 or CD4 T cells. T-cell responses were remarkably stable over time and, unlike responses in most immunodeficiency virus infections, maintained good functional characteristics, as evidenced by coproduction of IFN-γ and interleukin-2. Overall, high titers of binding and neutralizing antibody persisted throughout the postchallenge period. Encouragingly, long-term control was effective in macaques of diverse histocompatibility types.
机译:在2001年,我们报道了Gag-Pol-Env疫苗对猿猴和人类免疫缺陷病毒(SHIV-89.6P)的强毒89.6P嵌合体控制攻击的20周,该疫苗由DNA引发和修饰的痘苗病毒安卡拉加强免疫。在这里,我们报告说,其中23只动物中有22只成功控制了病毒血症,直到攻击后200周安乐死为止。安乐死时,所有动物的病毒载量低至无法检测,且CD4计数正常。在长期的病毒控制期间,产生γ-干扰素(IFN-γ)的抗病毒T细胞以出乎意料的低广度和低频率存在。大多数动物能识别2个CD8和1个CD4表位,对IFN-γ应答的T细胞的频率为总CD8或CD4 T细胞的0.01%至0.3%。 T细胞反应随着时间的推移非常稳定,并且与大多数免疫缺陷病毒感染中的反应不同,它保持了良好的功能特性,这是由IFN-γ和白介素2的共同产生所证明的。总体而言,在攻击后的整个过程中,高滴度的结合抗体和中和抗体持续存在。令人鼓舞的是,长期控制对各种组织相容性类型的猕猴均有效。

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