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Mechanisms of gender-specific TCDD-induced toxicity in guinea pig adipose tissue.

作者信息

Enan E, El-Sabeawy F, Overstreet J, Matsumura F, Lasley B

机构信息

Department of Environmental Toxicology and Institute of Toxicology and Environmental Health, University of California, Davis 95616, USA.

出版信息

Reprod Toxicol. 1998 May-Jun;12(3):357-69. doi: 10.1016/s0890-6238(98)00017-3.

DOI:10.1016/s0890-6238(98)00017-3
PMID:9628558
Abstract

After treatment with TCDD, the activities of cytosolic AhR-associated c-Src kinase, microsomal protein kinase C (nPKC epsilon), microsomal c-Src kinase, nuclear p44/42 MAPK, c-Jun N terminus kinase, and the amount of microsomal pan-Ras protein were different in males and females. TCDD did not decrease body or adipose tissue weights in transgenic src-deficient male mice as compared to their wild-type littermates, and the activity of AhR-associated c-Src kinase was not increased by TCDD in src-deficient male mice. Similar results were obtained when TCDD was given to male guinea pigs treated with the Src-kinase inhibitor, geldanamycin. Treatment with estradiol protected male guinea pigs from TCDD-induced wasting. TCDD induced similar changes in protein tyrosine kinase activity in adipose tissues of castrated male and intact female guinea pigs. The gender-specific mechanisms of TCDD-induced toxicity appear to involve c-Src kinase, nPKC epsilon, and pan-Ras, as well as overlap in the cytosolic signal transduction pathways of TCDD and sex steroids.

摘要

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