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APOBEC3 inhibits mouse mammary tumour virus replication in vivo.

机译:APOBEC3在体内抑制小鼠乳腺肿瘤病毒复制。

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摘要

Genomes of all mammals encode apobec3 genes, which are thought to have a function in intrinsic cellular immunity to several viruses including human immunodeficiency virus type 1 (HIV-1). APOBEC3 (A3) proteins are packaged into virions and inhibit retroviral replication in newly infected cells, at least in part by deaminating cytidines on the negative strand DNA intermediates. However, the role of A3 in innate resistance to mouse retroviruses is not understood. Here we show that A3 functions during retroviral infection in vivo and provides partial protection to mice against infection with mouse mammary tumour virus (MMTV). Both mouse A3 and human A3G proteins interacted with the MMTV nucleocapsid in an RNA-dependent fashion and were packaged into virions. In addition, mouse A3-containing and human A3G-containing virions showed a marked decrease in titre. Last, A3(-/-) mice were more susceptible to MMTV infection, because virus spread was more rapid and extensive than in their wild-type littermates.
机译:所有哺乳动物的基因组都编码apobec3基因,该基因被认为在对几种病毒(包括1型人类免疫缺陷病毒(HIV-1))的固有细胞免疫中具有功能。将APOBEC3(A3)蛋白包装到病毒粒子中,并至少部分地通过使负链DNA中间体上的胞苷脱氨基来抑制新感染细胞中的逆转录病毒复制。但是,尚不了解A3在对小鼠逆转录病毒的固有抗性中的作用。在这里,我们显示A3在体内逆转录病毒感染过程中发挥功能,并为小鼠提供部分保护,使其免受小鼠乳腺肿瘤病毒(MMTV)的感染。小鼠A3和人类A3G蛋白均以RNA依赖性方式与MMTV核衣壳相互作用,并被包装到病毒体中。此外,含小鼠A3和人A3G的病毒体的滴度显着降低。最后,A3(-/-)小鼠更容易受到MMTV感染,因为病毒的传播比其野生型同窝幼仔更为迅速和广泛。

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