Overlapping and Distinct Expression of Progesterone Receptors A and B in Mouse Uterus and Mammary Gland during the Estrous Cycle

• Published in: Endocrinology (Philadelphia) Vol. 147; no. 12; pp. 5503 - 5512
• Main Authors: Mote, Patricia A, Arnett-Mansfield, Rebecca L, Gava, Natalie, deFazio, Anna, Mulac-Jericevic, Biserka, Conneely, Orla M, Clarke, Christine L
• Format: Journal Article
• Language: English
• Published: Bethesda, MD Endocrine Society 01.12.2006
• Subjects: Animals; Biological and medical sciences; Epithelium - metabolism; Estrous Cycle - metabolism; Female; Fundamental and applied biological sciences. Psychology; Gene Expression Regulation; Humans; Mammary Glands, Animal - metabolism; Mice; Mice, Inbred BALB C; Mice, Knockout; Myometrium - metabolism; Organ Specificity; Ovariectomy - adverse effects; Ovary - metabolism; Ovary - physiology; Receptors, Estrogen - metabolism; Receptors, Progesterone - metabolism; Tissue Distribution; Tumor Cells, Cultured; Uterus - metabolism; Vertebrates: endocrinology; Vertebrata; Mammalia; Mouse; Uterus; Animal; Female genital system; Rodentia; Estrous cycle; Mammary gland; Progesterone receptor
• ISSN: 0013-7227; 1945-7170
• DOI: 10.1210/en.2006-0040

In rodents, progesterone receptors (PRs) A and B have different and often nonoverlapping roles, and this study asked whether different activities of the PR proteins in mouse are related to differences in their expression in reproductive tissues. The individual expression of PRA and PRB was determined immunohistochemically in mammary gland and uterus during the estrous cycle or in response to endocrine manipulation. In the mammary gland, PRA and PRB were colocated in PR+ epithelial cells, with little change during the estrous cycle. In the uterus, PRA was not detected in luminal epithelium at any stage of the cycle, and PR+ luminal cells expressed only PRB. In the stroma and myometrium, PRA and PRB levels fluctuated with cyclical systemic hormone exposure. Observation of functional end points suggested that augmented stromal and/or myometrial PRA in proestrus inhibited estrogen receptor expression and epithelial proliferation. Colocation of PRA and PRB was hormonally regulated, and ovariectomy did not reproduce the expression of PRA and PRB in the uterus during the estrous cycle. Whereas PRB was the only PR in the luminal epithelium in cycling mice, ovariectomy restored PRA expression, resulting in PRA-PRB colocation. In stroma and myometrium, PRA and PRB colocated in PR+ cells, but ovariectomy reduced PRA levels more than PRB, resulting in PRB-only-expressing cells. This study has shown that nonoverlapping PRA and PRB expression in the uterus, in particular the lack of PRA, and expression of PRB only in the luminal epithelium throughout the estrous cycle, is likely to contribute to the distinct roles of PRA and PRB in the adult mouse.