Novel interactions of large P3 moiety and small P4 moiety in the binding of the peptide mimetic factor VIIa inhibitor |
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| Authors: | Kadono Shojiro Sakamoto Akihisa Kikuchi Yasufumi Oh-Eda Masayoshi Yabuta Naohiro Yoshihashi Kazutaka Kitazawa Takehisa Suzuki Tsukasa Koga Takaki Hattori Kunihiro Shiraishi Takuya Haramura Masayuki Kodama Hirofumi Ono Yoshiyuki Esaki Toru Sato Haruhiko Watanabe Yoshiaki Itoh Susumu Ohta Masateru Kozono Toshiro |
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| Affiliation: | Fuji Gotemba Research Labs, Chugai Pharmaceutical Co., Ltd., 1-135 Komakado, Gotemba, Shizuoka 412-8513, Japan. kadonosuj@chugai-pharm.co.jp |
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| Abstract: | ![]()
Selective factor VIIa-tissue factor complex (FVIIa/TF) inhibition is seen as a promising target for developing new anticoagulant drugs. A novel peptide mimetic factor VIIa inhibitor, ethylsulfonamide-d-biphenylalanine-Gln-p-aminobenzamidine, shows 100-fold selectivity against thrombin in spite of its large P3 moiety, unlike previously reported FVIIa/TF selective inhibitors. X-ray crystal structure analysis reveals that the large P3 moiety, d-biphenylalanine, and the small P4 moiety, ethylsulfonamide, make novel interactions with the 170-loop and Lys192 of FVIIa/TF, respectively, accompanying ligand-induced conformational changes of the 170-loop, Gln217, and Lys192. Structural comparisons of FVIIa with thrombin and amino acid sequence comparisons among coagulation serine proteases suggest that these interactions play an important role in achieving selective inhibition for FVIIa/TF. |
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| Keywords: | Factor VIIa Blood coagulation Serine protease X-ray crystallography Drug design |
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