4.4 Article

Enhanced LH action in transgenic female mice expressing hCGβ-subunit induces pituitary prolactinomas; the role of high progesterone levels

Journal

ENDOCRINE-RELATED CANCER
Volume 17, Issue 3, Pages 611-621

Publisher

BIOSCIENTIFICA LTD
DOI: 10.1677/ERC-10-0016

Keywords

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Funding

  1. Academy of Finland (Centre of Excellence) [211480]
  2. Sigrid Juselius Foundation
  3. Finnish Cancer Foundation
  4. Turku Graduate School for Biomedical Sciences
  5. Wellcome Trust [063552, 082101]
  6. Academy of Finland (AKA) [211480] Funding Source: Academy of Finland (AKA)

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The etiology of pituitary adenomas remains largely unknown, with the exception of involvement of estrogens in the formation of prolactinomas. We have examined the molecular pathogenesis of prolactin-producing pituitary adenomas in transgenic female mice expressing the human choriongonadotropin (hCG) beta-subunit. The LH/CG bioactivity is elevated in the mice, with consequent highly stimulated ovarian progesterone (P-4) production, in the face of normal estrogen secretion. Curiously, despite normal estrogen levels, large prolactinomas developed in these mice, and we provide here several lines of evidence that the elevated P-4 levels are involved in the growth of these estrogen-dependent tumors. The antiprogestin mifepristone inhibited tumor growth, and combined postgonadectomy estradiol/P-4 treatment was more effective than estrogen alone in inducing tumor growth. Evidence for direct growth-promoting effect of P-4 was obtained from cultures of primary mouse pituitary cells and rat somatomammotroph GH3 cells. The mouse tumors and cultured cells revealed stimulation of the cyclin D1/cyclin-dependent kinase 4/retinoblastoma protein/transcription factor E2F1 pathway in the growth response to P-4. If extrapolated to humans, and given the importance of endogenous P-4 and synthetic progestins in female reproductive functions and their pharmacotherapy, it is relevant to revisit the potential role of these hormones in the origin and growth of prolactinomas. Endocrine-Related Cancer (2010) 17 611-621

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