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Simian Immunodeficiency Virus Variants That Differ in Pathogenicity Differ in Fitness under Rapid Cell Turnover Conditions

机译:在快速细胞周转条件下致病性不同的猿猴免疫缺陷病毒变种也不同

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摘要

Simian immunodeficiency virus (SIV) has been shown to progress through a number of changes that lead to the emergence of pathogenic viral variants in macaques initially infected with a mildly cytopathic variant, SIVMneCL8. One of these late-stage isolates, SIVMne170, replicates to high levels in vivo and causes a rapid disease course when reintroduced into naïve macaques, resulting in a viral set point up to 3,000-fold higher than the set point of the parental virus, SIVMneCL8. However, in cell culture both viruses replicate with similar kinetics. One major difference between in vivo and in vitro cultures is the life span of the infected cells. Here, we manipulated the life span of infected cells in vitro, and we show that the fitness of SIVMne170 in cultures with a limited cell life span dramatically increased compared to its fitness in cultures with a nonlimited life span of cells. The increase in fitness was at least partially due to the fact that the rapid turnover system eliminates the negative influence of the cytopathic effects associated with replication of SIVMne170. Because the relative fitness of SIVMneCL8 and SIVMne170 observed in the rapid turnover system more accurately reflects their fitness in vivo, the system represents an improved approach to comparing relative fitness of viruses.
机译:猿猴免疫缺陷病毒(SIV)已显示出通过许多变化而进展,这些变化导致最初感染有轻度细胞病变变体SIVMneCL8的猕猴中出现病原性病毒变体。这些晚期分离株之一,SIVMne170,在体内复制到高水平,当重新引入幼稚的猕猴时会引起快速的病程,导致病毒设定点比亲代病毒SIVMneCL8的设定点高3,000倍。但是,在细胞培养中,两种病毒都以相似的动力学复制。体内和体外培养之间的主要区别之一是被感染细胞的寿命。在这里,我们在体外操纵了受感染细胞的寿命,并且显示出与细胞寿命无限的培养物相比,SIVMne170在细胞寿命有限的培养物中的适应性显着提高。适应性的提高至少部分是由于快速更新系统消除了与SIVMne170复制相关的细胞病变效应的负面影响。由于在快速更新系统中观察到的SIVMneCL8和SIVMne170的相对适应性更准确地反映了它们在体内的适应性,因此该系统代表了一种比较病毒相对适应性的改进方法。

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