Enhancement by asbestos of oncogenesis by moloney murine sarcoma virus in CBA mice

## Abstract Injection of Moloney mouse sarcoma virus (M‐MSV) in adult mice of several inbred strains revealed that all strains except AKR are highly susceptible to M‐MSV tumor development. F1 hybrids between AKR and CBA, DBA/2 or NIH mice are as resistant (93%) as the parental AKR strain, which ind

## Abstract We have shown in the preceding paper that AKR mice are highly resistant to M‐MSV tumor development, and that resistance is transmitted as a dominant character In the present studies the tumor‐response pattern of F1 hybrids between resistant AKR and susceptible strains (C57Bl/6, BALB/c a

## Abstract Pre‐treatment of BALB/c mice with an intraperitoneal injection of heat‐inactivated serum obtained from BALB/c mice with progressively growing Moloney‐virus‐induced sarcomas (“progressor” mice) shortens the latent period and increases the growth rate and maximum size of primary sarcomas

Murine sarcoma virus (Moloney) ( M S V ) transformed C3H2K cells originating ,ji.otn the kidney tissues of a newborn C3HIHe mouse. Titration of tlze virus showed a one-hit dose response in the presence of an excess of Friend leukemia virus (FL V ) and a two-hit dose response in the absence of FLV, i

## Abstract Female R rats mated with an R male and inoculated __in utero__, after fetectomy, with murine sarcoma virus (Moloney), developed tumors. These tumors originated in the uterus and were of fetal origin. Intravenous or intraperitoneal injection of the virus induced similar tumors. Infectiou

## Abstract Sublethally irradiated BALB/c mice innoculated with Moloney sarcoma virus (MSV‐M) develop progressively growing tumors and die within 30 days of virus innoculation. These animals can be protected from tumor progression (and death) by innoculation of small numbers of MSV‐immune T lymphoc