首页> 美国卫生研究院文献>Biochemical Journal >Ferritin binds to light chain of human H-kininogen and inhibits kallikrein-mediated bradykinin release.
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Ferritin binds to light chain of human H-kininogen and inhibits kallikrein-mediated bradykinin release.

机译:铁蛋白与人H激肽原的轻链结合并抑制激肽释放酶介导的缓激肽释放。

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摘要

Ferritin is an iron-storage protein that exists in both intracellular and extracellular compartments. We have previously identified H-kininogen (high-molecular-weight kininogen) as a ferritin-binding protein [Torti and Torti (1998) J. Biol. Chem. 273, 13630-13635]. H-Kininogen is a precursor of the potent pro-inflammatory peptide bradykinin, which is released from H-kininogen following cleavage of H-kininogen by the serine protease kallikrein. In this report, we demonstrate that binding of ferritin to H-kininogen occurs via the modified light chain of H-kininogen, and that ferritin binds preferentially to activated H-kininogen. We further demonstrate that binding of ferritin to H-kininogen retards the proteolytic cleavage of H-kininogen by kallikrein and its subsequent release of bradykinin from H-kininogen. Ferritin does not interfere with the ability of kallikrein to digest a synthetic substrate, suggesting that ferritin specifically impedes the ability of kallikrein to digest H-kininogen, perhaps by steric hindrance. Based on these results, we propose a model of sequential H-kininogen cleavage and ferritin binding. These results are consistent with the hypothesis that the binding of ferritin to H-kininogen may serve to modulate bradykinin release.
机译:铁蛋白是一种铁存储蛋白,存在于细胞内和细胞外区室。我们先前已经确定H-激肽原(高分子量激肽原)为铁蛋白结合蛋白[Torti和Torti(1998)J。化学273,13630-13635]。 H-激肽原是强促炎肽缓激肽的前体,其在丝氨酸蛋白酶激肽释放酶切割H-激肽原后从H-激肽原中释放出来。在此报告中,我们证明了铁蛋白与H-激肽原的结合是通过H-激肽原的修饰轻链发生的,并且铁蛋白优先与活化的H-激肽原结合。我们进一步证明,铁蛋白与H-激肽原的结合可抑制激肽释放酶对H-激肽原的蛋白水解切割,并从H-激肽原中释放缓激肽。铁蛋白不干扰激肽释放酶消化合成底物的能力,这表明铁蛋白可能通过空间位阻而特异性地阻止激肽释放酶消化H激肽原的能力。基于这些结果,我们提出了顺序的H-激肽原裂解和铁蛋白结合的模型。这些结果与铁蛋白与H-激肽原的结合可能起到调节缓激肽释放的假设相一致。

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