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鼻病毒1A非衣壳蛋白中模糊加工和选择性降解的证据。

Evidence of ambiguous processing and selective degradation in the noncapsid proteins of rhinovirus 1A.

作者信息

McLean C, Matthews T J, Rueckert R R

出版信息

J Virol. 1976 Sep;19(3):903-14. doi: 10.1128/JVI.19.3.903-914.1976.

Abstract

Pulse-chase kinetics and extensive pactamycin mapping studies show that the translation of rhinovirus 1A proceeds in the order: initiate-P1-S-P2-terminate, where P1 is the precursor to the capsid proteins, S is a stable primary gene product, and P2 is the precursor to a family of noncapsid products. Initial examination of the molar stoichiometry of the families of rhinoviral proteins in infected cells suggested that both the P1 and P2 regions were translated more frequently than the S region. However, we show that this apparent asymmetry in translation is an artifact arising from two phenomena: (i) ambiguous cleavage sites which result in two alternative products from the S region, having apparent molecular weights of 47,000 and 38,000, and (ii) several fates for the P2 precursors, including degradation of 35 to 45% of the P2 family to small unidentifiable products. Another artifact, a time-dependent shift in the pactamycin mapping position of polypeptide r-39, was traced to a selective inhibition of the rate of cleavage of its precursor (peak 76). The processing rate of the capsid precursor (peak 92) was not retarded by pactamycin.

摘要

脉冲追踪动力学和广泛的放线菌酮图谱研究表明,鼻病毒1A的翻译按以下顺序进行:起始-P1-S-P2-终止,其中P1是衣壳蛋白的前体,S是一种稳定的初级基因产物,P2是一类非衣壳产物的前体。对感染细胞中鼻病毒蛋白家族的摩尔化学计量的初步检查表明,P1和P2区域的翻译频率均高于S区域。然而,我们表明这种明显的翻译不对称是由两种现象引起的假象:(i)模糊的切割位点导致S区域产生两种替代产物,表观分子量分别为47,000和38,000,以及(ii)P2前体的几种命运,包括35%至45%的P2家族降解为无法识别的小产物。另一个假象,即多肽r-39的放线菌酮图谱位置随时间的变化,被追溯到其前体(峰76)切割速率的选择性抑制。衣壳前体(峰92)的加工速率不受放线菌酮的阻碍。

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本文引用的文献

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RNA metabolism in the HeLa cell nucleus.海拉细胞核中的RNA代谢
J Mol Biol. 1966 May;17(1):117-30. doi: 10.1016/s0022-2836(66)80098-0.
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J Virol. 1974 Aug;14(2):261-9. doi: 10.1128/JVI.14.2.261-269.1974.
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Kinetics of synthesis and cleavage of encephalomyocarditis virus-specific proteins.
Virology. 1972 Nov;50(2):535-49. doi: 10.1016/0042-6822(72)90405-9.

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