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B cell responses to HIV and the development of human monoclonal antibodies.

机译:B细胞对HIV的反应和人类单克隆抗体的发展。

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摘要

In this review B cell responses in HIV-infected individuals are summarized together with the techniques used to date to produce human monoclonals to HIV and the properties of these antibodies. Profound disturbances in B cell responses are apparent both in vivo and in vitro. While there is evidence in vivo of marked polyclonal B cell activation, primary and secondary antibody responses are impaired. Similarly these cells exhibit spontaneous immunoglobulin secretion upon in vitro culture but do not readily respond to B cell mitogens and recall antigens including HIV. Furthermore, certain of these defects can be reproduced in normal B cells in vitro by incubation with HIV or HIV coded peptides. Individuals infected with HIV develop antibodies to HIV structural proteins (e.g. p17, p24, gp41 and gp120) and regulatory proteins (e.g. vif, nef, RT). Autoantibodies against a number of immunologically important molecules are also frequently observed. The anti-HIV antibodies are predominantly of the IgG1 isotype and exhibit a variety of effects on the virus in vitro. To date, using conventional immortalization strategies, an appreciable number of human monoclonals to HIV have been developed. These have been specific for gp41, gp120 and gag with antibodies of the former specificity predominating. The majority of these antibodies have been of the IgG1 isotype. Only a small number of the antibodies neutralize virus in vitro and most of these react with gp120. The neutralizing antibodies recognize conformational and carbohydrate epitopes or epitopes in amino acid positions 306-322. The predominant epitopes recognized by the anti-gp41 antibodies were in amino acid positions 579-620 and 644-662. A high percentage (congruent to 25%) of these antibodies enhance viral growth in vitro. The problems relating to the production of human monoclonals to HIV are discussed together with strategies that could be used in the future.
机译:在这篇综述中,总结了HIV感染者的B细胞反应,以及迄今为止用于产生HIV单克隆抗体和这些抗体特性的技术。在体内和体外,B细胞反应的深刻紊乱是显而易见的。尽管体内有明显的多克隆B细胞活化证据,但一抗和二抗反应受到损害。类似地,这些细胞在体外培养后表现出自发的免疫球蛋白分泌,但不容易对B细胞的促细胞分裂剂产生反应,并无法召回包括HIV在内的抗原。此外,这些缺陷中的某些可以通过与HIV或HIV编码的肽一起孵育,在体外正常B细胞​​中复制。感染了HIV的个体会产生针对HIV结构蛋白(例如p17,p24,gp41和gp120)和调节蛋白(例如vif,nef,RT)的抗体。还经常观察到针对许多具有免疫学意义的分子的自身抗体。抗HIV抗体主要是IgG1同种型,并且在体外对病毒表现出多种作用。迄今为止,使用常规的永生化策略,已经开发了相当数量的针对HIV的人单克隆抗体。这些对gp41,gp120和gag具有特异性,而前者的特异性抗体占优势。这些抗体大多数是IgG1同种型。仅有少量抗体在体外中和病毒,其中大多数与gp120反应。中和抗体识别构象表位和碳水化合物表位或氨基酸位置306-322中的表位。抗gp41抗体识别的主要表位位于氨基酸位置579-620和644-662。这些抗体的高百分比(相当于25%)可增强体外病毒的生长。讨论了与人类单克隆抗体的生产有关的问题,以及将来可能使用的策略。

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