The structure and function of the rous sarcoma virus RNA stability element

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 Chondroblasts and retinal melanoblasts have been transformed with a temperature‐sensitive Rous Sacroma Virus. At permissive temperature the transformed cells do not display their unique phenotypic properties. When such transformed cells are shifted to non‐permissive temperature they do

## The majority of human, animal andplant viral pathogens possess genomes composed of RNA. The strategies evolved for expression and replication of viral RNA genomes can differ signijicantly from those utilized for expression and replication of host-cell genetic material. Consequently, knowledge of

## Abstract Clonal lines of murine and avion sarcoma virus‐transformed mammalian cells, in which the viruses do not productively replicate, were studied for the occurrence of spontaneous or chemical‐induced morphologic reversion. From over 10,000 single‐cellderived clones of MSV‐transformed nonprod

## Abstract The horizontal development of lymphoid cell‐mediated specific antitumor immunity was studied in R/F rats, inoculated with the Schmidt‐Ruppin strain of Rous sarcoma virus (SR‐RSV) during the neonatal period. Lymph‐node cells (LNC) were harvested from individual animals on consecutive occ