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Natural Isolates of Simian Virus 40 from Immunocompromised Monkeys Display Extensive Genetic Heterogeneity: New Implications for Polyomavirus Disease

机译:免疫受损猴子的猿猴病毒40天然分离物显示广泛的遗传异质性:多瘤病毒病的新影响。

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摘要

Simian virus 40 (SV40) DNAs in brain tissue and peripheral blood mononuclear cells (PBMCs) of eight simian immunodeficiency virus-infected rhesus monkeys with SV40 brain disease were analyzed. We report the detection, cloning, and identification of five new SV40 strains following a quadruple testing-verification strategy. SV40 genomes with archetypal regulatory regions (containing a duplication within the G/C-rich regulatory region segment and a single 72-bp enhancer element) were recovered from seven animal brains, two tissues of which also contained viral genomes with nonarchetypal regulatory regions (containing a duplication within the G/C-rich regulatory region segment as well as a variable duplication within the enhancer region). In contrast, PBMC DNAs from five of six animals had viral genomes with both regulatory region types. It appeared, based on T-antigen variable-region sequences, that nonarchetypal virus variants arose de novo within each animal. The eighth animal exclusively yielded a new type of SV40 strain (SV40-K661), containing a protoarchetypal regulatory region (lacking a duplication within the G/C-rich segment of the regulatory region and containing one 72-bp element in the enhancer region), from both brain tissue and PBMCs. The presence of SV40 in PBMCs suggests that hematogenous spread of viral infection may occur. An archetypal version of a virus similar to SV40 reference strain 776 (a kidney isolate) was recovered from one brain, substantiating the idea that SV40 is neurotropic as well as kidney-tropic. Indirect evidence suggests that maternal-infant transmission of SV40 may have occurred in one animal. These findings provide new insights for human polyomavirus disease.
机译:分析了八只猿猴免疫缺陷病毒感染的恒河猴的大脑组织和外周血单核细胞(PBMC)中的猿猴病毒40(SV40)DNA,并对其进行了分析。我们报告了通过四重测试-验证策略对五种新的SV40菌株的检测,克隆和鉴定。从7个动物大脑中回收了具有原型调控区(在富含G / C的调控区片段中有重复,并且有一个72 bp的增强子)的SV40基因组,其中两个组织还包含具有非原型调控区的病毒基因组(包含在富含G / C的调节区域内进行重复,以及在增强子区域内进行可变重复)。相反,六只动物中有五只的PBMC DNA具有两种调节区域类型的病毒基因组。基于T抗原可变区序列,似乎在每只动物中从头出现了非原型病毒变体。第八只动物专门产生了一种新的SV40株(SV40-K661),其中包含一个原型原型调控区(在调控区的富含G / C的片段内缺乏重复,而在增强子区则包含一个72 bp的元件) ,来自脑组织和PBMC。 PBMC中SV40的存在表明可能发生病毒感染的血源性传播。从一个大脑中回收了类似于SV40参考菌株776(肾脏分离株)的病毒的原型版本,从而证实了SV40具有神经嗜性和嗜肾性。间接证据表明,SV40的母婴传播可能在一只动物中发生。这些发现为人类多瘤病毒病提供了新的见解。

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