Developmental reprogramming of IGF signaling and susceptibility to endometrial hyperplasia in the rat. Academic Article

abstract

• In rodents, a brief neonatal exposure of the developing reproductive tract to the xenoestrogen, diethylstilbestrol (DES) reprograms developing tissues to increase susceptibility to tumorigenesis in adult animals, including uterine adenocarcinoma. Progression from a normal endometrium to carcinoma occurs via the intermediate stage of endometrial hyperplasia. We previously reported that endometrial hyperplasia in postmenopausal women is linked to abnormal insulin-like growth factor-I (IGF-I) signaling. To identify early events involved in the development of hyperplasia in the endometrium, we examined expression and activation of IGF-I pathway components in endometrium of rats exposed to DES. By 5 months of age, 36/60 (60%) of rats exposed to DES on days 3-5 after birth developed endometrial hyperplasia compared to 0% of vehicle-treated controls. Consistent with activation of a mitogenic signaling pathway, Ki67-positive cells increased in DES-exposed endometrium despite compromised ovarian function and hypoestrogenic milieu characteristic of DES-exposed animals. The endometrium of DES-exposed rats overexpressed IGF-II and insulin receptor substrate-1 (IRS-1) and exhibited elevated Akt expression and activation (as judged by phosphorylation) and mTOR signaling (phosphorylation of S6) compared to vehicle-treated endometrium. In contrast to vehicle-treated endometrium, in which negative feedback to IRS-1 was observed (phosphorylation of S636/639), negative feedback to IRS-1 was absent in DES-exposed endometrium. These data support a central role for IGF-I signaling in the development of both human and rodent endometrial hyperplasia. Furthermore, both global activation of IGF-IR signaling and abrogation of negative feedback to IRS-1 appear to be reprogrammed by DES in endometrial hyperplasia, implicating for the first time loss of negative feedback to IRS-1 in development of a preneoplastic lesion.

authors

• Davies, Peter

published proceedings

• Lab Invest

author list (cited authors)

• McCampbell, A. S., Walker, C. L., Broaddus, R. R., Cook, J. D., & Davies, P.

citation count

• 29

complete list of authors

• McCampbell, Adrienne S||Walker, Cheryl L||Broaddus, Russell R||Cook, Jennifer D||Davies, Peter JA

publication date

• January 2008

publisher

• Elsevier  Publisher

published in

• Laboratory Investigation  Journal

keywords

• Adaptor Proteins, Signal Transducing
• Animals
• Animals, Newborn
• Carcinogens
• Diethylstilbestrol
• Endometrial Hyperplasia
• Female
• Genetic Predisposition To Disease
• Insulin Receptor Substrate Proteins
• Insulin-Like Growth Factor I
• Insulin-Like Growth Factor II
• Ki-67 Antigen
• Phosphorylation
• Proto-Oncogene Proteins C-akt
• RNA, Neoplasm
• Rats
• Rats, Mutant Strains
• Ribosomal Protein S6 Kinases
• Signal Transduction
• Time Factors

Digital Object Identifier (DOI)

• 10.1038/labinvest.2008.29

start page

• 615

end page

• 626

volume

• 88

issue

• 6

URL

• http://dx.doi.org/10.1038/labinvest.2008.29