Shubhangee Mungre scite author profile

Three independent point mutations within residues 97 to 103 of the simian virus 40 small-t antigen (small-t) greatly reduced the ability of purified small-t to inhibit protein phosphatase 2A in vitro. These mutations affected the interaction of small-t antigen with the protein phosphatase 2A A subunit translated in vitro, and a peptide from the region identified by these mutations released the A subunit from immune complexes. When introduced into virus, the mutations eliminated the ability of small-t to enhance viral transformation of growth-arrested rat Flll cells. In contrast, the mutant small-t antigens were unimpaired in the transactivation of the adenovirus E2 promoter, an activity which was reduced by a double mutation in small-t residues 43 and 45.

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C/EBPβ in Rheumatoid Arthritis: Correlation with Inflammation, Not Disease Specificity1

Pope

Lovis

Mungre

et al. 1999

Clinical Immunology

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Inhibition of the Na+/H+-antiporter by theophylline in growth-arrested monkey kidney cells

Mungre

Renz

Rundell

1991

Experimental Cell Research

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