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Properties of anti-gp41 core structure antibodies, which compete with sera of HIV-1-infected patients

机译:抗gp41核心结构抗体的特性,可与HIV-1感染患者的血清竞争

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摘要

To determine the correlation between the immunoreaction against the core structure of human immunodeficiency virus type (HIV-1) transmembrane protein gp41 epitopes and the disease progression, it is essential to evaluate the anti-core structure antibody epitopes and the humoral immunity against the epitopes. For this purpose we evaluated monoclonal antibodies (mAbs) against the gp41 core structure such as mAbs 50.69, 98.6 and T26, by Western blotting (WB) and flow cytometry. WB showed mAbs 50.69 and 98.6 bound to both monomeric and oligomeric gp41, and mAb T26 exclusively bound to oligomeric gp41. We evaluated the sera from Pneumocystis pneumonia patients (PCP; n = 7) and long-term survivors (LTS; n = 7). Competition assay with sera and mAbs for binding to H9 cells infected with HIV-1 IIIB virus was done using flow cytometry. The results revealed that PCP sera as well as LTS sera inhibited the binding of all the three mAbs, and the PCP sera inhibited mAb T26 binding more efficiently than LTS. Therefore, PCP patients retain competing immunity to antibodies against not only the shared epitopes of the core structure (binding sites of mAbs 50.69 and 98.6) but also against oligomeric gp41 specific epitope (binding site of mAb T26). (c) 2005 Elsevier SAS. All rights reserved.
机译:为了确定针对人类免疫缺陷病毒类型(HIV-1)跨膜蛋白gp41表位的核心结构的免疫反应与疾病进展之间的相关性,评估抗核心结构抗体表位和针对表位的体液免疫至关重要。为此,我们通过Western印迹(WB)和流式细胞仪评估了针对gp41核心结构的单克隆抗体(mAb),例如mAb 50.69、98.6和T26。 WB显示mAb 50.69和98.6均与单体gp41和寡​​聚gp41结合,而mAb T26仅与寡聚gp41结合。我们评估了肺孢子虫肺炎患者(PCP; n = 7)和长期幸存者(LTS; n = 7)的血清。使用流式细胞仪进行了血清和mAb与HIV-1 IIIB病毒感染的H9细胞结合的竞争测定。结果显示,PCP血清和LTS血清均抑制所有三种mAb的结合,并且PCP血清比LTS更有效地抑制mAb T26结合。因此,PCP患者不仅对核心结构的共享表位(mAb 50.69和98.6的结合位点)而且对寡聚gp41特异性表位(mAb T26的结合位点)都具有竞争性抗体免疫力。 (c)2005 Elsevier SAS。版权所有。

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