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Next step in the development of mesoprogestins: the preclinical profile of EC313

Front Endocrinol (Lausanne). 2023-09; 
K B?aszczak-?wi?tkiewicz, A Krupa, E Mnich, W Elger, M Oettel, H Nair, M Wierzbicki, P Sieroszewski, Z Shaked
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Proteins, Expression, Isolation and Analysis … Plasmids pFastBac1-ERa and pFastBac1-ERb, coding for the full length human estrogen receptors α and β, respectively, were obtained from GenScript. Tritiated Estradiol served as the … Get A Quote

摘要

introduction: The pharmacological target for progesterone, different progestins, and Selective Progesterone Receptor Modulators (SPRMs) is the nuclear progesterone receptor (PR). EC313 is a new member of a subgroup of SPRMs, mesoprogestins, which combine especially PR- agonistic and PR-antagonistic activities in one molecule. methods: The suitable -model for the differentiation of SPRMs from the subgroup of mesoprogestins is the estrogen-primed juvenile rabbit endometrium assay (McPhail Assay). Remarkably, in contrast to other well-known SPRMs with no agonistic effects in this test, EC313 shows clear partial PR-agonistic effects that are higher than that of the well-known mesoprogestin Asoprisnil which already ... More

關(guān)鍵詞

endometriosis, mesoprogestins, progesterone receptor agonists and antagonists, selective progesterone receptor modulators, uterine fibroids/leiomyomas
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