首页> 美国卫生研究院文献>Journal of Virology >Equal levels of gp120 retention and neutralization resistance of phenotypically distinct primary human immunodeficiency virus type 1 variants upon soluble CD4 treatment.
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Equal levels of gp120 retention and neutralization resistance of phenotypically distinct primary human immunodeficiency virus type 1 variants upon soluble CD4 treatment.

机译:在可溶性CD4处理后表型上不同的人类免疫缺陷病毒1型变异体的gp120保留水平和中和抗性相等。

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摘要

Human immunodeficiency virus type 1 (HIV-1) variants passaged in T-cell lines, often called laboratory isolates, are potently neutralized by soluble CD4 (sCD4), whereas primary HIV-1 variants are highly resistant to sCD4 neutralization. Previously, it was demonstrated that the domain from V1 to V3 of the HIV-1 gp120 molecule contains one of the major determinants of sCD4 neutralization sensitivity, and the same region has also been implicated as influencing syncytium-inducing (SI) capacity and T-cell-line tropism. To determine possible differences in sCD4 neutralization sensitivity between phenotypically distinct primary HIV-1 variants, a panel of non-syncytium-inducing (NSI) and SI HIV-1 variants was studied. Primary NSI and SI HIV-1 variants appeared to be equally resistant to sCD4 neutralization. Consistent with this observation, sCD4 did not induce gp120 shedding from either primary NSI or SI HIV-1 variants at 37 degrees C. Thus, it is not the potential of certain primary HIV-1 variants to infect T-cell lines but rather their adaptation to T-cell lines that is reflected in specific properties of the viral envelope which influence sCD4 neutralization sensitivity.
机译:在T细胞系中传代的人类免疫缺陷病毒1型(HIV-1)变异体(通常称为实验室分离株)被可溶性CD4(sCD4)有效中和,而主要的HIV-1变异体对sCD4中和具有高度抗性。先前已证明,HIV-1 gp120分子从V1到V3的结构域包含sCD4中和敏感性的主要决定因素之一,并且还暗示了同一区域会影响合胞体诱导(SI)能力和T-细胞系向性。为了确定在表型上不同的主要HIV-1变体之间sCD4中和敏感性的可能差异,研究了一组非合胞体诱导(NSI)和SI HIV-1变体。主要的NSI和SI HIV-1变体似乎对sCD4中和具有相同的抗性。与该观察结果一致,sCD4并未在37摄氏度时诱导从原发性NSI或SI HIV-1变异体中释放出gp120。因此,某些原发性HIV-1变异体并非具有感染T细胞系的潜力,而是它们的适应性反映在病毒包膜的特定特性中的T细胞系影响sCD4中和敏感性。

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