Map kinase activation correlates with K-ras mutation and loss of heterozygosity on chromosome 6 in alveolar bronchiolar carcinomas from B6C3F1 mice exposed to vanadium pentoxide for 2 years

doi:10.1093/carcin/23.10.1737

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Carcinogenesis, Vol. 23, No. 10, 1737-1743, October 2002
© 2002 Oxford University Press

CARCINOGENESIS

Map kinase activation correlates with K-ras mutation and loss of heterozygosity on chromosome 6 in alveolar bronchiolar carcinomas from B6C3F1 mice exposed to vanadium pentoxide for 2 years

Theodora R. Devereux¹^,4, Wanda Holliday¹, Colleen Anna¹, Nancy Ress², Joseph Roycroft² and Robert C. Sills³

¹ Laboratory of Molecular Carcinogenesis,
² Toxicology Operations Branch and
³ Laboratory of Experimental Pathology, National Institute of Environmental Health Sciences, PO Box 12233, National Institutes of Health, Research Triangle Park, NC 27709, USA

Previous work showed a correlation between K-ras mutation andloss of heterozygosity (LOH) on chromosome 6 in the region ofK-ras in lung carcinomas from B6C3F1 mice. We hypothesized thatmitogen-activated protein kinase (MAPK) would be activated onlyin those lung neoplasms with both K-ras mutation and LOH. AsMAPK activity can be correlated directly with signal detectionusing antibodies to phosphorylated MAPK, we were able to analyzelung carcinomas from B6C3F1 mice for the presence or absenceof MAPK activity by western analysis. Vanadium pentoxide-inducedmouse lung carcinomas, which had been shown to have a high frequencyof K-ras mutations and LOH on chromosome 6 and for which frozentumor tissue was available, were used for this study. TotalMAPK expression levels were similar between normal lung andlung carcinomas. Phospho-MAPK was elevated in five of six lungcarcinoma samples examined in which K-ras mutations and chromosome6 LOH were identified and in four of five carcinomas with K-rasmutations that lacked LOH. Phospho-MAPK was undetectable orweakly expressed in seven carcinomas examined without K-rasmutations and in normal lung. By immunohistochemistry threeK-ras positive/LOH negative samples exhibited multifocal areasof nuclear and cytoplasmic staining for phospho-MAPK. Largeamounts of non-staining fibroblasts, lymphocytes and macrophageswere also observed in these tumors. Two of these lung carcinomaswere microdissected and chromosome 6 LOH was detected in regionsof phospho-MAPK positive cells. These results suggest that MAPKis activated during vanadium pentoxide-induced B6C3F1 mouselung tumorigenesis following K-ras mutation and loss of thewild-type K-ras allele.

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