5 years ago

Novel naftopidil derivatives containing methyl phenylacetate and their blocking effects on α1D/1A-adrenoreceptor subtypes

Novel naftopidil derivatives containing methyl phenylacetate and their blocking effects on α1D/1A-adrenoreceptor subtypes
α 1-Adrenoceptor (α 1-AR) antagonists are considered to be the most effective monotherapy agents for lower urinary tract symptoms associated with benign prostatic hyperplasia (LUTS/BPH). In this study, we synthesized compounds 217, which are novel piperazine derivatives that contain methyl phenylacetate. We then evaluated the vasodilatory activities of these compounds. Among them, we found that compounds 2, 7, 12, which contain 2-OCH3, 2-CH3 or 2, 5-CH3, respectively, exhibited potent α 1-blocking activity similar to protype drug naftopidil (1). The antagonistic effects of 2, 7, and 12 on the (−)-noradrenaline-induced contractile response of isolated rat prostatic vas deferens (α 1A), spleen (α 1B) and thoracic aorta (α 1D) were further characterized to assess the sub receptor selectivity. Compared with naftopidil (1) and terazosin, compound 12 showed the most desirable α 1D/1A subtype selectivity, especially improved α 1A subtype selectivity, and the ratios pA 2 (α 1D)/pA 2 (α 1B) and pA 2 (α 1A)/pA 2 (α 1B) were 17.0- and 19.5-fold, respectively, indicating less cardiovascular side effects when used to treat LUTS/BPH. Finally, we investigated the chiral pharmacology of 12. We found, however, that the activity of enantiomers (R)-12 and (S)-12 are not significantly different from that of rac-12.

Publisher URL: www.sciencedirect.com/science

DOI: S0960894X18300799

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