In Vivo and In Vitro Analysis of Hyperoxia-Induced Gene Expression in Mouse Lung and Mouse Transformed Clara Cells

## Abstract The Ki‐__ras__ proto‐oncogene is activated by specific point mutations and is the transforming gene often identified in rodent and human lung tumors. An in vitro model to aid in the study of the consequences of Ki‐__ras__ activation and expression in mouse lung is needed. Accordingly, w

## Abstract Many transformed mouse lung cells, including LM2 cells, contain activating mutations in the Ki‐__ras__ gene and show reduced responsiveness to growth inhibition by glucocorticoids. LM2GR cells, which are LM2 cells stably transfected with a rat glucocorticoid receptor __(GR)__ gene, were

## Abstract New cell‐surface antigens were detected on nineteen of twenty‐four malignant lines of 3‐methylcholanthrene (MCA)‐ or MCA‐epoxide‐transformed cells derived from cloned C3H mouse prostate cells. Exhaustive cross‐tests between lines derived from single control clones showed that in all but

## Abstract The immuno‐reactivity of C57BL mouse spleen cells previously sensitized in vitro against syngeneic fibroblasts or syngeneic 3LL Lewis tumor cells was investigated. The sensitized spleen cells were assayed in vitro to test their cytotoxicity against the 3LL tumor cells. In addition, sple