Literature DB >> 6335503

Three independent polyproteins coded by the gag gene of type-D retrovirus in a continuous human cell line.

V A Morozov, K V Ilyin.   

Abstract

The processing of gag-gene-coded polyproteins of type D retrovirus (HEp-2 V) in chronically infected continuous human larynx carcinoma cell line HEp-2 (HeLa-like) was investigated by means of the pulse-chase modification of the radioimmunoprecipitation test. Three independent polyproteins coded by the gag gene of HEp-2 V were revealed in the immunoprecipitates: Pr 78gag, a direct precursor of the virus internal structural polypeptides, described in a previous report (1); Pr 180gag + pol, a probable reverse transcriptase precursor; and gPr 78gag, a glycosylated polyprotein of unknown function. Two unstable intermediate polyproteins derived from Pr 78gag cleavage were detected in the presence of serine protease inhibitors. These polypeptides, having molecular weights of 37 K and 33 K, are Pr 37gag and Pr 33gag respectively. A probable scheme of gag-gene-coded polyproteins processing is suggested, and speculations on the gag-gene-coded glycosylated polyproteins of retroviruses as growth factor receptors are also presented.

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Year:  1984        PMID: 6335503

Source DB:  PubMed          Journal:  Int J Tissue React        ISSN: 0250-0868


  1 in total

1.  Study of the gag-coded polyproteins of type D retroviruses. Block of glycosylation inhibits the processing of major structural protein.

Authors:  P O Ilyinskii; V A Morozov; K V Ilyin
Journal:  Arch Virol       Date:  1990       Impact factor: 2.574

  1 in total

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