具有改善的凝血酶和胰蛋白酶选择性的基于苯并咪唑的因子Xa抑制剂。

Benzimidazole-based fXa inhibitors with improved thrombin and trypsin selectivity.

作者信息

Shaw Kenneth J, Guilford William J, Griedel Brian D, Sakata Steve, Trinh Lan, Wu Shung, Xu Wei, Zhao Zuchun, Morrissey Michael M

机构信息

Medicinal Chemistry, Berlex Biosciences, 15049 San Pablo Avenue, PO Box 4099, 94804-0099, Richmond, CA, USA

出版信息

Bioorg Med Chem Lett. 2002 May 6;12(9):1311-4. doi: 10.1016/s0960-894x(02)00145-2.

DOI:10.1016/s0960-894x(02)00145-2

PMID:11965378

Abstract

Optimization of the benzimidazole-based fXa inhibitors for selectivity versus thrombin and trypsin was achieved by substitution on the benzimidazole ring and replacement of the naphthylamidine group. Substitution of a nitro group at the 4-position on the benzimidazole improves both potency against fXa and selectivity versus thrombin. Alternatively, replacement of the naphthylamidine with either a biphenylamidine or propenylbenzamidine not only improves fXa potency and selectivity versus thrombin, but selectivity versus trypsin as well.

摘要

通过在苯并咪唑环上进行取代以及替换萘基脒基团，实现了基于苯并咪唑的fXa抑制剂对凝血酶和胰蛋白酶选择性的优化。在苯并咪唑的4位上取代硝基，可提高对fXa的效力以及对凝血酶的选择性。另外，用联苯脒或丙烯基苯甲脒取代萘基脒，不仅能提高对fXa的效力和对凝血酶的选择性，还能提高对胰蛋白酶的选择性。

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具有改善的凝血酶和胰蛋白酶选择性的基于苯并咪唑的因子Xa抑制剂。

Benzimidazole-based fXa inhibitors with improved thrombin and trypsin selectivity.

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