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首页> 外文期刊>BMC Biochemistry >Fusion of the C-terminal triskaidecapeptide of hirudin variant 3 to alpha1-proteinase inhibitor M358R increases the serpin-mediated rate of thrombin inhibition
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Fusion of the C-terminal triskaidecapeptide of hirudin variant 3 to alpha1-proteinase inhibitor M358R increases the serpin-mediated rate of thrombin inhibition

机译:水rud素变体3的C端三skaidecapeptide与alpha1蛋白酶抑制剂M358R的融合增加丝氨酸蛋白酶抑制剂介导的凝血酶抑制率

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摘要

Background Alpha-1 proteinase inhibitor (API) is a plasma serpin superfamily member that inhibits neutrophil elastase; variant API M358R inhibits thrombin and activated protein C (APC). Fusing residues 1-75 of another serpin, heparin cofactor II (HCII), to API M358R (in HAPI M358R) was previously shown to accelerate thrombin inhibition over API M358R by conferring thrombin exosite 1 binding properties. We hypothesized that replacing HCII 1-75 region with the 13 C-terminal residues (triskaidecapeptide) of hirudin variant 3 (HV354-66) would further enhance the inhibitory potency of API M358R fusion proteins. We therefore expressed HV3API M358R (HV354-66 fused to API M358R) and HV3API RCL5 (HV354-66 fused to API F352A/L353V/E354V/A355I/I356A/I460L/M358R) API M358R) as N-terminally hexahistidine-tagged polypeptides in E. coli.
机译:背景Alpha-1蛋白酶抑制剂(API)是血浆Serpin超家族成员,可抑制嗜中性粒细胞弹性蛋白酶。 API M358R变体抑制凝血酶和活化蛋白C(APC)。先前显示,通过赋予凝血酶异位点1结合特性,将另一种丝氨酸蛋白酶抑制剂,肝素辅因子II(HCII)的残基1-75融合到API M358R(在HAPI M358R中)可加速对API M358R的凝血酶抑制作用。我们假设,用水rud素变体3(HV354-66)的13个C末端残基(三skaidecapeptide)替换HCII 1-75区将进一步增强API M358R融合蛋白的抑制能力。因此,我们将HV3API M358R(与API M358R融合的HV354-66)和HV3API RCL5(与API F352A / L353V / E354V / A355I / I356A / I460L / M358R融合的HV354-66)表达为N-末端被六组氨酸标记的多肽大肠杆菌。

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