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HIV Type 1 Env Precursor Cleavage State Affects Recognition by Both Neutralizing and Nonneutralizing gp41 Antibodies

机译：HIV 1型Env前体裂解状态通过中和和非中和gp41抗体影响识别。

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摘要

HIV-1 is relatively resistant to antibody-mediated neutralization; however, rare antibodies to the exterior envelope glycoprotein, gp120, and the transmembrane glycoprotein, gp41, can neutralize a broad array of isolates. Two antibodies, 2F5 and 4E10, are directed against the gp41 membrane proximal external region (MPER); however, the kinetic neutralization signature of these antibodies remains unresolved. Previously, we reported that the fully cleaved, cell surface envelope glycoproteins (Env) derived from the primary isolate, JR-FL, are well recognized exclusively by gp120-directed neutralizing ligands and not by nonneutralizing gp120 antibodies. However, the gp120 nonneutralizing antibodies can recognize HIV spikes that are rendered fully cleavage defective by site-directed mutagenesis. Here, we extended such analysis to gp41 neutralizing and nonneutralizing antibodies and, relative to the rules of gp120-specific antibody recognition, we observed marked contrasts. Similar to gp120 recognition, the nonneutralizing gp41 cluster 1 or cluster 2 antibodies bound much more efficiently to cleavage-defective spikes when compared to their recognition of cleaved spikes. In contrast to gp120 neutralizing antibody recognition, the broadly neutralizing gp41 antibodies 2F5 and 4E10, like the nonneutralizing gp41 antibodies, did not efficiently recognize the predominantly cleaved, primary isolate JR-FL spikes. However, if the spikes were rendered cleavage defective, recognition by both the neutralizing and nonneutralizing ligand markedly increased. CD4 interaction with the cleaved spikes markedly increased recognition by most nonneutralizing gp41 antibodies, whereas such treatment had a minimal increase of 2F5 and 4E10 recognition. These data indicate again the profound influence that cleavage imposes on the quaternary packing of primary isolate spikes and have important implications for soluble trimer candidate immunogens.

机译：HIV-1对抗体介导的中和具有相对抗性。然而，针对外部包膜糖蛋白gp120和跨膜糖蛋白gp41的罕见抗体可以中和多种分离物。两种抗体2F5和4E10针对gp41膜近端外部区域（MPER）；然而，这些抗体的动力学中和特征仍未解决。先前，我们报道了源自主要分离物JR-FL的完全切割的细胞表面包膜糖蛋白（Env）仅被定向于gp120的中和配体而不是未被中和的gp120抗体很好地识别。但是，gp120非中和抗体可以识别通过定点诱变使其完全裂解为缺陷的HIV峰值。在这里，我们将这种分析扩展到gp41中和和非中和抗体，并且相对于gp120特异性抗体识别的规则，我们观察到了明显的对比。与gp120识别类似，与识别裂解的尖峰相比，非中和性gp41簇1或簇2抗体与裂解缺陷的尖峰的结合效率更高。与gp120中和抗体识别相反，广泛中和的gp41抗体2F5和4E10与未中和的gp41抗体一样，不能有效识别主要切割的初级分离物JR-FL尖峰。但是，如果使尖峰的切割缺陷，则中和和非中和配体的识别度都会明显提高。 CD4与裂解的尖峰的相互作用通过大多数非中和性gp41抗体显着增加了识别，而这种处理的2F5和4E10识别增加最小。这些数据再次表明，裂解对初级分离物突突的四级堆积施加了深远影响，并对可溶性三聚体候选免疫原具有重要意义。

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期刊名称 AIDS Research and Human Retroviruses
作者
Bimal K. Chakrabarti; Marie Pancera; Sanjay Phogat; Sijy ODell; Krisha McKee; Javier Guenaga; James Robinson; John Mascola; Richard T. Wyatt;
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年(卷),期 -1(27),8
年度 -1
页码 877–887
总页数 12
原文格式 PDF
正文语种
中图分类免疫学;病毒传染病;人体病毒学（致病病毒）;病毒（滤过性病毒）;
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专利

1. HIV type 1 Env precursor cleavage state affects recognition by both neutralizing and nonneutralizing gp41 antibodies. [J] . Chakrabarti BK, Pancera M, Phogat S, AIDS Research and Human Retroviruses . 2011,第8期

机译：HIV 1型Env前体的裂解状态会通过中和gp41抗体和不中和gp41抗体来影响识别。
2. Modulation of nonneutralizing HIV-1 gp41 responses by an MHC-restricted TH epitope overlapping those of membrane proximal external region broadly neutralizing antibodies [J] . ZhangJ., AlamS.M., Bouton-VervilleH., The Journal of Immunology: Official Journal of the American Association of Immunologists . 2014,第4期

机译：通过重叠膜近端外部区域的MHC限制的TH表位对非线性阈值的反应的非对外区域宽度中和抗体的反应的调节
3. Modulation of Nonneutralizing HIV-1 gp41 Responses by an MHC-Restricted TH Epitope Overlapping Those of Membrane Proximal External Region Broadly Neutralizing Antibodies [J] . Jinsong Zhang, S. Munir Alam, Hilary Bouton-Verville, The journal of immunology . 2014,第4期

机译：MHC限制TH抗原决定簇重叠膜近端外部区域广泛中和抗体的非中和HIV-1 gp41反应的调制。
4. Synthesis of HIV Gp41 Trimer Mimics Inducing Neutralizing Antibodies Based on Remodeling of Dynamic Structures of HIV-1 Envelope Proteins [C] . Wataru Nomera, Toru Nakahara, Chie Hashimoto American Peptide Symposium . 2011

机译：基于HIV-1包络蛋白动态结构的重塑诱导中和抗体的HIV GP41三聚体模拟物的合成
5. The HIV-1 Env Gp41 Cytoplasmic Tail: Key Functions During Cell-to-Cell Infection and Neutralization. [D] . Durham, Natasha D. 2016

机译：HIV-1 Env Gp41细胞质尾巴：细胞间感染和中和过程中的关键功能。
6. Nonneutralizing Antibodies Induced by the HIV-1 gp41 NHR Domain Gain Neutralizing Activity in the Presence of the HIV Fusion Inhibitor Enfuvirtide: a Potential Therapeutic Vaccine Strategy [O] . Qian Wang, Wenwen Bi, Xiaojie Zhu, 2015

机译：HIV-1 gp41 NHR域诱导的非中和抗体在存在HIV融合抑制剂恩夫韦肽的情况下获得中和活性：一种潜在的治疗性疫苗策略
7. Functional characterization of two scFv-Fc antibodies from an HIV controller selected on soluble HIV-1 Env complexes : a neutralizing V3- and a trimer-specific gp41 antibody [O] . Trott, Maria, Weiβ, Svenja, Antoni, Sascha, 2014

机译：从可溶性HIV-1 Env复合物上选择的HIV控制器中的两种scFv-Fc抗体的功能表征：中和性V3-和三聚体特异性gp41抗体

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