Effect of drug-resistance reversors on expressions of oncogenes or tumor suppressor oncogenes of human tumor cell lines

## Abstract The expression of nine oncogenes (c‐myc, N‐myc, N‐ras, H‐ras, k‐ras, abl, fos, src, and raf) and two tumor suppressor genes (p53 and RB) were studied by northern blot hybridization in six human hepatocellular carcinoma or hepatoblastoma cell lines (PLC/PRF/5, HepSB, Hep G2, 2.2.15, HLE,

## Abstract Human osteosarcoma and fibrosarcoma cell lines were investigated for alterations in oncogenes, tumor suppressor genes, and growth factors, all of which have been implicated in tumor formation. Characterization of oncogenes that are involved in osteosarcoma formation, including the __c‐f

To detect mutationally activated ras oncogenes, we analyzed electrophoretic mobilities of ras p21 proteins utilizing the fact that many ras oncogenes produce abnormal p21 proteins that migrate at SDS/polyacrylamide gel electrophoresis as a fast-moving or slow-moving species in comparison to a normal

## Abstract Human papillomavirus (HPV)‐induced carcinogenesis is critically dependent on the activities of the viral __E6__ and __E7__ oncogenes. Here, we demonstrate that expression of the putative tumor suppressor gene __B‐cell translocation gene‐2__ (__BTG2__) is reinduced in HPV16‐ and HPV18‐po