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The inhibitory complex of human alpha 1-proteinase inhibitor and human leukocyte elastase is a neutrophil chemoattractant

机译:人类α1-蛋白酶抑制剂和人类白细胞弹性蛋白酶的抑制复合物是中性粒细胞趋化因子

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摘要

An inhibitor-proteinase complex consisting of human alpha 1-PI and human leukocyte elastase is chemotactic for human neutrophils. The chemotactic activity is optimal at 1 nM and is associated only with the alpha 1-PI portion of the complex. Neither HLE in the complex, free HLE, nor native alpha 1-PI possesses chemotactic activity for human neutrophils. alpha 1-PI in complex is hydrolyzed at the Met-358-Ser-359 bond. The chemotactic activity is associated with the Mr 4,200 fragment of alpha 1-PI that has Ser-359 as its NH2 terminus. The region of the HLE-alpha 1-PI complex that stimulates chemotaxis appears to be the same as that of the Mr 4,200 fragment generated by hydrolysis of the Pro-357-Met-358 bond during proteolytic inactivation of alpha 1-PI. The data suggest the presence of a neutrophil surface receptor bound by alpha 1-PI after the formation of a complex with HLE or after proteolytic degradation. This receptor may play a role in clearance of these modified alpha 1-PI molecules.
机译:由人α1-PI和人白细胞弹性蛋白酶组成的抑制剂-蛋白酶复合物对人中性粒细胞具有趋化作用。趋化活性在1 nM时最佳,并且仅与复合物的α1-PI部分相关。复杂的游离HLE中的HLE和天然α1-PI都不具有对人类嗜中性粒细胞的趋化活性。复合物中的α1-PI在Met-358-Ser-359键处水解。趋化活性与具有Ser-359作为其NH2末端的α1-PI的Mr 4,200片段相关。 HLE-α1-PI复合物刺激趋化性的区域似乎与在α1-PI的蛋白水解失活过程中通过Pro-357-Met-358键的水解产生的Mr 4,200片段的区域相同。数据表明在与HLE形成复合物后或在蛋白水解降解后,存在被α1-PI结合的嗜中性粒细胞表面受体。该受体可能在这些修饰的α1-PI分子的清除中起作用。

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  • 年度 1988
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