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氨基酸、肽和蛋白质氢过氧化物对组织蛋白酶及相关蛋白酶的抑制作用。

Inhibition of cathepsins and related proteases by amino acid, peptide, and protein hydroperoxides.

作者信息

Headlam Henrietta A, Gracanin Michelle, Rodgers Kenneth J, Davies Michael J

机构信息

The Heart Research Institute, 145 Missenden Road, Camperdown, Sydney, NSW 2050, Australia.

出版信息

Free Radic Biol Med. 2006 May 1;40(9):1539-48. doi: 10.1016/j.freeradbiomed.2005.12.036. Epub 2006 Mar 10.

DOI:10.1016/j.freeradbiomed.2005.12.036
PMID:16632114
Abstract

Reaction of radicals in the presence of O2, and singlet oxygen, with some amino acids, peptides, and proteins yields hydroperoxides. These species are key intermediates in chain reactions and protein damage. Previously we have shown that peptide and protein hydroperoxides react rapidly with thiols, and that this can result in inactivation of thiol-dependent enzymes. The major route for the cellular removal of damaged proteins is via catabolism mediated by proteosomal and lysosomal pathways; cysteine proteases (cathepsins) play a key role in the latter system. We hypothesized that inactivation of cysteine proteases by hydroperoxide-containing oxidised proteins may contribute to the accumulation of modified proteins within cells. We show here that thiol-dependent cathepsins, either isolated or in cell lysates, are rapidly and efficiently inactivated by amino acid, peptide, and protein hydroperoxides in a time- and concentration-dependent manner; this occurs with similar efficacy to equimolar H2O2. Inactivation involves reaction of the hydroperoxide with Cys residues as evidenced by thiol loss and formation of sulfenic acid intermediates. Structurally related, non-thiol-dependent cathepsins are less readily inactivated by these hydroperoxides. This inhibition, by oxidized proteins, of the system designed to remove modified proteins, may contribute to the accumulation of damaged proteins in cells subject to oxidative stress.

摘要

自由基在氧气和单线态氧存在的情况下与某些氨基酸、肽和蛋白质发生反应会生成氢过氧化物。这些物质是链式反应和蛋白质损伤的关键中间体。此前我们已经表明,肽和蛋白质氢过氧化物能与硫醇迅速反应,这可能导致硫醇依赖性酶失活。细胞清除受损蛋白质的主要途径是通过蛋白酶体和溶酶体途径介导的分解代谢;半胱氨酸蛋白酶(组织蛋白酶)在后一系统中起关键作用。我们推测含氢过氧化物的氧化蛋白质使半胱氨酸蛋白酶失活可能导致细胞内修饰蛋白质的积累。我们在此表明,无论是分离的还是细胞裂解物中的硫醇依赖性组织蛋白酶,都会被氨基酸、肽和蛋白质氢过氧化物以时间和浓度依赖性方式迅速且有效地失活;其发生效率与等摩尔的过氧化氢相似。失活涉及氢过氧化物与半胱氨酸残基的反应,硫醇损失和亚磺酸中间体的形成证明了这一点。结构相关的非硫醇依赖性组织蛋白酶较不易被这些氢过氧化物失活。氧化蛋白质对旨在清除修饰蛋白质的系统的这种抑制作用,可能导致遭受氧化应激的细胞中受损蛋白质的积累。

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