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胆汁淤积性肝病患儿血清中的中性内肽酶活性未升高:氨肽酶 - m在肽的顺序水解中的独特作用

Neutral endopeptidase activity is not elevated in serum in children with cholestatic liver disease: a unique role of aminopeptidase-m in sequential hydrolysis of peptides.

作者信息

Janas Roman M, Socha Jerzy, Janas Jadwiga, Warnawin Krzysztof

机构信息

Department of Radioimmunology, The Children's Memorial Health Institute, Warsaw, Poland.

出版信息

Dig Dis Sci. 2002 Aug;47(8):1766-74. doi: 10.1023/a:1016440511089.

Abstract

The aim of this study was to determine whether neutral endopeptidase activity is elevated in serum in children with cholestatic liver disease (Alagille syndrome), and whether the enzyme cooperates with the serum aminopeptidase-M in degradation of peptides. Our data suggest that neutral endopeptidase activity remains at a very low level,.undetectable with the assays we have applied, both in the serum from healthy children and those with cholestasis. In contrast, the serum aminopeptidase-M activity is highly increased in cholestasis. We have demonstrated that aminopeptidase-M alone is capable of sequential and complete hydrolysis of enkephalins and low-molecular-weight, nonspecific peptides. The rate of release of free amino acids from both exogenous or endogenous substrate peptides was statistically significantly higher in serum in children with cholestasis compared with healthy children (P < 0.05). Substance P (Ki = 2.5 micromol/liter) and bradykinin (Ki = 27 micromol/liter) were shown to be potent inhibitors of the serum aminopeptidase-M. We postulate that aminopeptidase-M, except when regulating the activity of bioactive peptides, may serve as a scavenger of short, nonspecific peptides in the circulation. Our data seem to provide new insights for further studies on the role of serum peptidases both in physiology and pathophysiology.

摘要

本研究的目的是确定胆汁淤积性肝病(阿拉吉耶综合征)患儿血清中的中性内肽酶活性是否升高,以及该酶是否与血清氨肽酶-M协同作用参与肽的降解。我们的数据表明,无论是在健康儿童还是胆汁淤积患儿的血清中,中性内肽酶活性都维持在极低水平,用我们所采用的检测方法无法检测到。相比之下,胆汁淤积时血清氨肽酶-M活性显著升高。我们已经证明,单独的氨肽酶-M能够对脑啡肽和低分子量非特异性肽进行连续和完全的水解。与健康儿童相比,胆汁淤积患儿血清中外源性或内源性底物肽释放游离氨基酸的速率在统计学上显著更高(P < 0.05)。P物质(Ki = 2.5微摩尔/升)和缓激肽(Ki = 27微摩尔/升)被证明是血清氨肽酶-M的有效抑制剂。我们推测,氨肽酶-M除了调节生物活性肽的活性外,还可能作为循环中短链非特异性肽的清除剂。我们的数据似乎为进一步研究血清肽酶在生理和病理生理中的作用提供了新的见解。

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