Malignant and transforming activity of rous sarcoma virus. I. Malignant effect of rous sarcoma virus

Virus variants from Af mouse tumours induced by syngeneic cultured cells infected with Carr-Zilber strain of Rous sarcoma virus were studied. These variants were highly oncogenic for adult mice and golden hamsters thus differing from the original Carr-Zilber strain. The coat antigens of these viruse

The induction of Rous sarcoma virus f RS V ] production was analyzed in mi-ved cultures of mouse or hamster Rous sarcoma cells and chick embryo cells treated with ultraviolet inactivated hemagglutinating virus of Japan ( U V-H V J ) . The pre-treatment of UV-HVJ with a certain concentration of anti-

## Abstract Avian sarcoma virus (ASV)‐transformed mammalian cells, known to be either virus‐producing, virogenic or non‐virogenic, were tested for viral gene products: for p27 by radioimmunoassay and for group‐specific (gs) antigens by the complement fixation test. Clones of B77 virus‐producing RBI

## Abstract Plasma, serum and the main proteins involved in the final steps of blood coagulation, fibrinogen, thrombin and plasma transglutaminase, have been tested for their ability to inhibit cell transformation and/or to induce reversion of the transformed to the normal phenotype in RSV‐infected

## Abstract Biotin or a serum lipid extract stimulated proliferation of G1 arrested Rous sarcoma virus‐transformed BHK cells in modified Eagle's MEM (BM). The cells could be maintained continuously in BM plus biotin (BMB), but not in BM plus serum lipid extract (BM · L). Avidin inhibited growth sti