人类免疫缺陷病毒1型Gag前体的C末端一半对于高效的病毒颗粒组装来说已足够。
The C-terminal half of the human immunodeficiency virus type 1 Gag precursor is sufficient for efficient particle assembly.
作者信息
Borsetti A, Ohagen A, Göttlinger H G
机构信息
Department of Cancer Immunology and AIDS, Dana-Farber Cancer Institute, and Department of Pathology, Harvard Medical School, Boston, Massachusetts 02215, USA.
出版信息
J Virol. 1998 Nov;72(11):9313-7. doi: 10.1128/JVI.72.11.9313-9317.1998.
Abstract
Human immunodeficiency virus type 1 particle assembly is directed by the Gag polyprotein Pr55(gag), the precursor for the matrix (MA), capsid (CA), and nucleocapsid proteins of the mature virion. We now show that CA sequences N terminal to the major homology region (MHR), which form a distinct domain, are dispensable for particle formation. However, slightly larger deletions which extend into the MHR severely impair particle production. Remarkably, a deletion which removed essentially all MA and CA sequences between the N-terminal myristyl anchor and the MHR reduced the yield of extracellular particles only moderately. Particle formation even exceeded wild-type levels when additional MA sequences, either from the N or the C terminus of the domain, were retained. We conclude that no distinct region between the myristyl anchor and the MHR is required for efficient particle assembly or release.
摘要
1型人类免疫缺陷病毒颗粒组装由Gag多聚蛋白Pr55(gag)指导,Pr55(gag)是成熟病毒体的基质(MA)、衣壳(CA)和核衣壳蛋白的前体。我们现在表明,位于主要同源区域(MHR) N端的CA序列(形成一个独特结构域)对于颗粒形成是可有可无的。然而,延伸到MHR的稍大缺失会严重损害颗粒产生。值得注意的是,一个缺失基本上去除了N端肉豆蔻酰化锚定和MHR之间的所有MA和CA序列,仅适度降低了细胞外颗粒的产量。当保留来自该结构域N端或C端的额外MA序列时,颗粒形成甚至超过了野生型水平。我们得出结论,肉豆蔻酰化锚定和MHR之间没有独特区域对于高效颗粒组装或释放是必需的。
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