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VH1-69 Utilizing Antibodies Are Capable of Mediating Non-neutralizing Fc-Mediated Effector Functions Against the Transmitted/Founder gp120

机译:VH1-69利用抗体能够介导非中和的Fc介导的效应子功能对抗传递的/基础gp120

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摘要

Multiple antibody effector functions arise in HIV-1 infection that could be harnessed to protect against infection or clear the persistent reservoir. Here, we have investigated the genetic and functional memory B cell and antibody landscape present during early infection in six individuals infected with either subtype A, C, or an A/C recombinant HIV-1. These individuals demonstrated varying levels of plasma autologous neutralization (nAb) against the transmitted/founder envelope (T/F Env) pseudovirus and non-neutralizing Fc-mediated effector function (nnFc) antibody-dependent cell-mediated cytotoxicity (ADCC) against the T/F Env gp120 protein at ~7 months after infection. Genetic analysis of the immunoglobulin heavy (VH) and light (VL) chain variable domain gene segments from 352 autologous T/F Env gp120-specific single B cells recovered at this same 7-month time-point revealed an over-representation of the VH1-69 germline in five of six individuals. A defining feature of the VH1-69 utilizing gp120-specific antibodies was their significantly more hydrophobic complementarity-determining region-2 (CDRH2) regions compared to other VH CDRH2 sequences from each individual. While none of the VH1-69 antibodies possessed strong neutralizing activity against virions pseudotyped with the autologous T/F Env, almost a third were capable of mediating high ADCC activity, as assayed by intracellular granzyme B activity in CEM.NKr.CCR5 target cells coated with autologous T/F Env gp120. High ADCC mediating VH1-69 antibodies exhibited shorter complementarity-determining region-3 (CDRH3) lengths and a more neutral isoelectric point than antibodies lacking this function. In the individual that developed the highest autologous ADCC responses, the high granzyme B producing antibodies bound to surface expressed envelope in the absence of CD4 and were not enhanced by the addition of soluble CD4. Overall, VH1-69 utilizing antibodies are commonly induced against gp120 in diverse HIV-1 infections and a subset of these antibodies can mediate ADCC functions, serving as a bridge between the innate and adaptive immune response to HIV-1.
机译:在HIV-1感染中会出现多种抗体效应子功能,可以利用这些功能来保护自己免受感染或清除持久性宿主。在这里,我们调查了在感染A,C或A / C重组HIV-1亚型的六名个体早期感染过程中存在的遗传和功能记忆B细胞和抗体的情况。这些个体表现出针对传播/基础包膜(T / F Env)假病毒的血浆自体中和水平(nAb)和针对T的非中和Fc介导的效应子功能(nnFc)抗体依赖性细胞介导的细胞毒性(ADCC)感染后约7个月/ F Env gp120蛋白。在同一7个月的时间点回收的352个自体T / F Env gp120特异性单B细胞的免疫球蛋白重链(VH)和轻链(VL)可变域基因片段的遗传分析显示,VH1的表达过多在六个个体中的五个个体中拥有-69种系。与来自每个个体的其他VH CDRH2序列相比,利用gp120特异性抗体的VH1-69的主要特征是它们的疏水性互补决定区域2(CDRH2)区域明显更强。尽管VH1-69抗体均不具有针对用自体T / F Env假型化的病毒体的强中和活性,但通过CEM.NKr.CCR5靶细胞包被的细胞内颗粒酶B活性检测,几乎有三分之一的病毒能够介导高ADCC活性。与自体T / F Env gp120。与缺乏此功能的抗体相比,介导高ADCC的VH1-69抗体表现出更短的互补决定区3(CDRH3)长度和更中性的等电点。在产生最高自体ADCC反应的个体中,在不存在CD4的情况下,高粒酶B产生抗体与表面表达的包膜结合,并且不会通过添加可溶性CD4来增强。总体而言,利用VH1-69的抗体通常会在各种HIV-1感染中针对gp120诱导,这些抗体的一部分可以介导ADCC功能,充当对HIV-1的先天性和适应性免疫应答之间的桥梁。

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