Characterization of non-producer human cells induced by kirsten sarcoma virus

## Abstract Non‐producer (NP) human cells were isolated from transformed foci induced by the Kirsten mouse sarcoma virus. These morphologically altered NP cells produced neither infectious virus nor complement‐fixing antigens of the murine sarcoma‐leukemia virus complex. However, the sarcoma virus

## Abstract Guinea‐pig embryo cells were transformed in vitro by the Kirsten strain of mouse sarcoma virus (Ki‐MSV). The transformed cells were found to release infectious virus continuously and produced high titers of group‐specific, complement‐fixing antigen characteristic of the murine leukemia—

## Abstract Reports from several laboratories have suggested that the virus transformed state may be maintained either by ectopically produced growth factors of alternatively by ectopically produced serine proteases including plasminogen activator. Here we show that the maintenance of transformatio

## Abstract A human revertant cell line, derived from non‐producer human osteosarcoma cells (NP/KHOS) induced by Kirsten murine sarcoma virus, was treated __in vitro__ with various levels of polycyclic aromatic hydrocarbons (3‐methylcholanthrene, 7,12‐dimethylbenz(__a__)anthracene, and benzo(__a__)

## abbreviated as MLV. ' Three different serum pools collected from the same animals. Designations such as In, 1 b, lc etc. distinguish these pools. ## Rat strain obtained from Dr. Bengt Gustafsson The cells were incubated with undiluted sera. Thereafter, rabbit complement preadsorbed with YAC

## Abstract A pseudotype focus‐forming virus was prepared by fusion of human cells infected with RD‐114 virus and non‐producer hamster cells transformed by murine sarcoma virus. The focus‐forming virus, designated MSV (RD‐114), transformed human fibroblasts, including WI‐38, but no mouse, hamster,