The reaction of rabbits to rous sarcoma virus

## Cultures of cells from embryos of Af, C3H-Hg and (CBAT6T6 x Af)F, mice rapidly developed oncogenicity for syngeneic animals after exposure to RSV (Carr-Zilber strain). The tumours of mice were virogenic and contained the group-specific antigen of avian sarcoma-leukosis complex. However, when the

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

## Abstract A nontransformed line of Chinese hamster ovary (CHO) cells (Pollard and Stanners, 1979) has been transformed by the Schmidt‐Ruppin subgroup D strain of Rous sarcoma virus (SR‐RSV). SR‐RSV transformed CHO cells are shown to differ from spontaneously transformed cells in that the virally

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 For simple retroviruses, such as the Rous sarcoma virus (RSV), post‐transcriptional control elements regulate viral RNA splicing, export, stability, and packaging into virions. These RNA sequences interact with cellular host proteins to regulate and facilitate productive viral infection