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Polyoma T (tumor) antigen species in abortively and stably transformed cells

✍ Scribed by Benjamin, Thomas L. ;Schaffhausen, Brian S. ;Silver, Jonathan E.


Book ID
102927807
Publisher
Wiley (John Wiley & Sons)
Year
1979
Tongue
English
Weight
666 KB
Volume
12
Category
Article
ISSN
0091-7419

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✦ Synopsis


Abstract

Stable neoplastic transformation of cells by polyoma virus requires the participation of two viral genes, designated ts‐a and hr‐t. The effects of mutations in these two genes on the patterns of T‐antigen synthesis during productive infection have been previously described: ts‐ a mutants are affected in the β€œlarge” (100K) nuclear T antigen, and hr‐t mutants are affected in the β€œmiddle” (36K, 56K, 63K) and β€œsmall” (22K) T agtigens. The latter are associated predominantly with the plasma membrane (56K) and cytosol fractions, rrespectively.

Here we examine the expression of the various forms of polyoma T antigen in nonproductive infection (abortive transformation) as well as in stably transformed cell lines of different species. The results on abortive transformation are essentially the same as those described above for productive infection. In stably transformed cells, the middle and small T antigens are seen to various extents. The large T antigen, however, is often absent or present below the level of detection. Clones lacking the large T antigen are found most often among mouse transformants, but are also seen among rat transformants. Retention of the 100K species in transformed cells therefore appears to be, at least in part, an inverse function of the level of permissivity of the host toward productive viral infection. These findings indicate that the induction of the transformed phenotype in both abortively and stably transformed cells generally does not require the large T antigen, but rather the products of the hr‐t gene.


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