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Usage Information

PPAR-γ receptor ligands: novel therapy for pituitary adenomas
Anthony P. Heaney, … , Manory Fernando, Shlomo Melmed
Anthony P. Heaney, … , Manory Fernando, Shlomo Melmed
Published May 1, 2003
Citation Information: J Clin Invest. 2003;111(9):1381-1388. https://doi.org/10.1172/JCI16575.
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PPAR-γ receptor ligands: novel therapy for pituitary adenomas

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Abstract

Pituitary tumors cause considerable morbidity due to local invasion, hypopituitarism, or hormone hypersecretion. In many cases, no suitable drug therapies are available, and surgical excision is currently the only effective treatment. We show here abundant expression of nuclear hormone receptor PPAR-γ in all of 39 human pituitary tumors. PPAR-γ activating thiazolidinediones (TZDs) rosiglitazone and troglitazone induced G0-G1 cell-cycle arrest and apoptosis in human, rat somatolactotroph, and murine gonadotroph pituitary tumor cells, and suppressed in vitro hormone secretion. In vivo development and growth of murine somatolactotroph and gonadotroph tumors, generated by subcutaneous injection of prolactin-secreting (PRL-secreting) and growth hormone–secreting (GH-secreting) GH3 cells, luteinizing hormone–secreting (LH-secreting) LβT2 cells, and α-T3 cells, was markedly suppressed in rosiglitazone-treated mice, and serum GH, PRL, and LH levels were attenuated in all treated animals (P < 0.009). These results demonstrate that PPAR-γ is an important molecular target in pituitary adenoma cells and PPAR-γ ligands inhibit tumor cell growth and GH, PRL, and LH secretion in vitro and in vivo. TZDs are proposed as novel oral medications for managing pituitary tumors.

Authors

Anthony P. Heaney, Manory Fernando, Shlomo Melmed

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Usage data is cumulative from June 2024 through June 2025.

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