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The novel inhibitors of serine proteases

机译:丝氨酸蛋白酶的新型抑制剂

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摘要

Thirty optically active nonprotein α-amino acids and peptides based thereon have been screened for their ability to interact with bovine trypsin and proteinase K from Tritirachium album Limber, which belong to the group of serine proteases. Both structure-based drug design approach and determination of enzyme activity have been used to identify low molecular weight inhibitors of trypsin and proteinase K. Compounds have been selected that according to the docking analysis were able to interact with trypsin and proteinase K. Following the docking analysis measurement of enzymes activity (2R,3S)-β-hydroxyleucme and (2S,3R)-β-hydroxyleucine inhibited both enzymes activity, whereas (S)-α-methyl-β-phenylalanine, (R)-α-methyl-β-phenylala-nine, (S)-allylglycine, (R)-allylglycine, (S)-α-allylalanine, (R)-α-allylalanine and allo-O-ethylthreonine inhibited only proteinase K; and N-formyl-(S)-methionyl-(2S,3R)-hydro-xyleucine, N-formyl-(S)-methionyl-(2R,3S)-hydroxyleucine, N-formyl-(S)-methionyl-(S)-allylglycine and N-formyl-(S)-methionyl-(R)-allylglycine inhibited trypsin. It has been shown that inhibition of trypsin by (2R,3S)-β-hydroxyleucine and N-formyl-(S)-methionyl-(2R,3S)-hydroxyleucine is of a competitive mode.
机译:已经筛选了三十种旋光性非蛋白质α-氨基酸和基于其的肽与Tritirachium Album Limber(属于丝氨酸蛋白酶)的牛胰蛋白酶和蛋白酶K相互作用的能力。基于结构的药物设计方法和酶活性的测定均已用于鉴定胰蛋白酶和蛋白酶K的低分子量抑制剂。根据对接分析,选择了能够与胰蛋白酶和蛋白酶K相互作用的化合物。酶活性的分析测定(2R,3S)-β-羟基亮氨酸和(2S,3R)-β-羟基亮氨酸均抑制了这两种酶的活性,而(S)-α-甲基-β-苯丙氨酸,(R)-α-甲基- β-苯丙氨酸,(S)-烯丙基甘氨酸,(R)-烯丙基甘氨酸,(S)-α-烯丙氨酸,(R)-α-烯丙氨酸和同素-O-乙基苏氨酸仅抑制蛋白酶K;和N-甲酰基-(S)-甲硫酰基-(2S,3R)-氢-亮氨酸,N-甲酰基-(S)-甲硫酰基-(2R,3S)-羟基亮氨酸,N-甲酰基-(S)-甲硫酰基-( S)-烯丙基甘氨酸和N-甲酰基-(S)-甲硫酰基-(R)-烯丙基甘氨酸抑制胰蛋白酶。已经显示,(2R,3S)-β-羟基亮氨酸和N-甲酰基-(S)-甲硫酰基-(2R,3S)-羟基亮氨酸对胰蛋白酶的抑制是竞争性模式。

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