Synthesis and SAR study of novel pseudo-steroids as potent and selective progesterone receptor antagonists |
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| Authors: | Nareshkumar Jain George Allan Olivia Linton Pamela Tannenbaum Xin Chen Jun Xu Peifang Zhu Joseph Gunnet Keith Demarest Scott Lundeen William Murray Zhihua Sui |
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| Affiliation: | Johnson and Johnson Pharmaceutical Research and Development, Medicinal Chemistry, LLC, 665 Stockton Drive, Exton, PA 19341, USA |
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| Abstract: | Synthesis of novel 7-pseudo-steroids 1c has been achieved from trenbolone 3 via an efficient 14 step sequence with overall yields of 10–15%. Various substitutions were incorporated at both the aromatic side chain as well as the D ring. The orientation of aromatic side chain at C10 plays a crucial role for progesterone receptor (PR) activity. Compound 2a (T47D = 1 nM) with –NMe2 para to the aromatic group along with spirofurane groups in the D ring was the optimal substitution. All compounds were also evaluated for glucocorticoid receptor (GR) antagonist activities in vivo in a rat and found efficacious in uterine complement C3 assay via the oral route of administrations. |
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