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人类免疫缺陷病毒碳水化合物表位的肽模拟

Peptide mimicry of carbohydrate epitopes on human immunodeficiency virus.

作者信息

Agadjanyan M, Luo P, Westerink M A, Carey L A, Hutchins W, Steplewski Z, Weiner D B, Kieber-Emmons T

机构信息

Department of Pathology and Laboratory Medicine, University of Pennsylvania, Philadelphia 19104-6082, USA.

出版信息

Nat Biotechnol. 1997 Jun;15(6):547-51. doi: 10.1038/nbt0697-547.

Abstract

Cancer-related, mucin-type carbohydrate epitopes, principally mannose and sialo-syl residues, are expressed on the envelope protein gp 160 of the human immunodeficiency virus (HIV). Anticarbohydrate antibodies directed toward these and other carbohydrate epitopes are known to neutralize HIV-1 infection by cell-free virus. Carbohydrates, however, being T cell-independent antigens, typically elicit diminished immune responses. To overcome this potential draw back, we have examined the ability of peptides that mimic such epitopes to elicit immune responses that cross-react with carbohydrate structures. We report that mouse polyclonal antisera generated against peptides that mimic mucin-related carbohydrate epitopes have anti-HIV-1 activity. Generation of antibodies was not lr-gene restricted, as at least two different strains of mice. Balb/c (H-2d) and C57Bl/6 (H-2b), responded equally to the peptides. The antipeptide sera displayed neutralizing activity against HIV-I/MN and HIV-I/3B viral strains. This neutralization was as good as human anti-HIV sera. These results indicate that peptide mimics of carbohydrates provide a novel strategy for the further development of reagents that elicit immune responses to carbohydrate epitopes associated with many infectious organisms and tumor cells.

摘要

与癌症相关的黏蛋白型碳水化合物表位,主要是甘露糖和唾液酸残基,在人类免疫缺陷病毒(HIV)的包膜蛋白gp160上表达。已知针对这些及其他碳水化合物表位的抗碳水化合物抗体可通过无细胞病毒中和HIV-1感染。然而,碳水化合物作为不依赖T细胞的抗原,通常引发的免疫反应较弱。为克服这一潜在缺陷,我们研究了模拟此类表位的肽引发与碳水化合物结构发生交叉反应的免疫反应的能力。我们报告称,针对模拟黏蛋白相关碳水化合物表位的肽产生的小鼠多克隆抗血清具有抗HIV-1活性。抗体的产生不受Ir基因限制,因为至少两种不同品系的小鼠,即Balb/c(H-2d)和C57Bl/6(H-2b),对这些肽的反应相同。抗肽血清对HIV-I/MN和HIV-I/3B病毒株具有中和活性。这种中和效果与人类抗HIV血清相当。这些结果表明,碳水化合物的肽模拟物为进一步开发引发针对与许多感染性生物体和肿瘤细胞相关的碳水化合物表位的免疫反应的试剂提供了一种新策略。

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