Klaude Maria, Hammarqvist Folke, Wemerman Jan
Karolinska University Hospital, Huddinge, Anasthesiology, KFC, Novum S-141 86 Huddinge, Sweden.
Clin Nutr. 2005 Apr;24(2):259-65. doi: 10.1016/j.clnu.2004.11.002.
BACKGROUND & AIMS: Muscle wasting during critical illness is generally believed to be an increase in muscle protein degradation mediated by the proteasome proteolytic pathway. Polyubiquinated proteins are recognised and degraded by the 26S multicatalytic proteasome complex. Animal models for various catabolic conditions have shown increased expression of mRNA:s for several enzymes and subunits in the ubiquitin-proteasome pathway as well as an increase in proteasome activity. The aim of this study was to measure the proteolytic activity of the proteasome in human skeletal muscle. We investigated the proteasome activity in leg muscle biopsies from 7 critically ill patients and from a reference group of 7 age and sex matched patients by a method that could also be suitable for repetitive measurements of intensive care unit patients in future studies.
Proteasomes were isolated by ultracentrifugation and the fractions containing cytosolic soluble and membrane-bound proteasomes were, respectively, incubated with a fluorogenic peptide substrate to assess the chymotrypsin-like peptidase activity.
In the critically ill the proteasome activity in the membrane-bound fraction of proteasomes was 30% higher compared to the reference group (P<0.02), whereas no difference was seen regarding the soluble fraction.
The results indicate that there is an altered distribution of proteasome activity at the subcellular level in skeletal muscle of critically ill intensive care unit patients.
危重病期间的肌肉消耗通常被认为是由蛋白酶体蛋白水解途径介导的肌肉蛋白降解增加所致。多聚泛素化蛋白被26S多催化蛋白酶体复合物识别并降解。各种分解代谢状态的动物模型显示,泛素-蛋白酶体途径中几种酶和亚基的mRNA表达增加,同时蛋白酶体活性也增加。本研究的目的是测量人骨骼肌中蛋白酶体的蛋白水解活性。我们通过一种在未来研究中也适用于对重症监护病房患者进行重复测量的方法,调查了7例危重病患者以及7例年龄和性别匹配的参照组患者腿部肌肉活检标本中的蛋白酶体活性。
通过超速离心分离蛋白酶体,分别将含有胞质可溶性和膜结合蛋白酶体的组分与一种荧光肽底物孵育,以评估类胰凝乳蛋白酶样肽酶活性。
与参照组相比,危重病患者蛋白酶体膜结合组分中的蛋白酶体活性高30%(P<0.02),而可溶性组分未见差异。
结果表明,重症监护病房危重病患者骨骼肌中亚细胞水平的蛋白酶体活性分布发生了改变。