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1型人类免疫缺陷病毒分离株病毒粒子包膜糖蛋白gp120的差异性丢失:对感染性和中和作用的影响。

Differential loss of envelope glycoprotein gp120 from virions of human immunodeficiency virus type 1 isolates: effects on infectivity and neutralization.

作者信息

McKeating J A, McKnight A, Moore J P

机构信息

Chester Beatty Laboratories, Institute of Cancer Research, London, United Kingdom.

出版信息

J Virol. 1991 Feb;65(2):852-60. doi: 10.1128/JVI.65.2.852-860.1991.

Abstract

Several parameters which may affect the infectivity of human immunodeficiency virus type 1 in tissue culture were analyzed. In particular, we used gel exclusion chromatography to investigate how the loss of the surface glycoprotein gp120 from virions of the HTLV-IIIB (IIIB), HTLV-IIIRF (RF), and SF-2 isolates modulates infectivity. In IIIB and RF cultures, a high proportion of the total gp120 was virion bound initially but was gradually lost from the virions over time. In contrast, most of the gp120 (and p24) in SF-2-infected cultures was soluble and the few particles present had a fivefold-lower level of virus-bound gp120. However, this reduced level of virion-bound gp120 was more resistant to shedding. Loss of a major proportion of gp120 from IIIB and RF virions resulted in reduced infectivities, and in addition, the resulting accumulation of soluble gp120 in the cultures could competitively inhibit viral infection, especially with SF-2. Increased shedding of virion gp120 also affected the neutralization of IIIB and RF particles. However, the high sensitivity to human serum neutralization characteristic of SF-2 was unaffected by soluble gp120 in cultures, suggesting that the epitopes responsible are not present on soluble gp120.

摘要

分析了几个可能影响1型人类免疫缺陷病毒在组织培养中感染性的参数。特别地,我们使用凝胶排阻色谱法研究了HTLV-IIIB(IIIB)、HTLV-IIIRF(RF)和SF-2毒株的病毒粒子表面糖蛋白gp120的丢失如何调节感染性。在IIIB和RF培养物中,最初总gp120的很大一部分与病毒粒子结合,但随着时间的推移逐渐从病毒粒子中丢失。相比之下,SF-2感染培养物中的大多数gp120(和p24)是可溶的,存在的少数颗粒上与病毒结合的gp120水平低五倍。然而,这种与病毒粒子结合的gp120水平的降低对脱落更具抗性。IIIB和RF病毒粒子中大部分gp120的丢失导致感染性降低,此外,培养物中可溶性gp120的积累会竞争性抑制病毒感染,尤其是对SF-2。病毒粒子gp120脱落增加也影响了IIIB和RF颗粒的中和作用。然而,SF-2对人血清中和的高敏感性不受培养物中可溶性gp120的影响,这表明相关表位不存在于可溶性gp120上。

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