作者
Oliver Drews, Osamu Tsukamoto, David Liem, John Streicher, Yibin Wang, Peipei Ping
发表日期
2010/10/29
期刊
Circulation research
卷号
107
期号
9
页码范围
1094-1101
出版商
Lippincott Williams & Wilkins
简介
Rationale:
Proteasomal degradation is altered in many disease phenotypes including cardiac hypertrophy, a prevalent condition leading to heart failure. Our recent investigations identified heterogeneous subpopulations of proteasome complexes in the heart and implicated multiple mechanisms for their regulation.
Objective:
The study aimed at identification of molecular mechanisms changing proteasome function in the hypertrophic heart.
Method and Results:
Proteasome function, expression, and assembly were analyzed during the development of cardiac hypertrophy induced by β-adrenergic stimulation. The analysis revealed, for the first time, divergent regulation of proteasome function in cardiac hypertrophy. Proteasome complexes have 3 different proteolytic activities, which are ATP-dependent for 26S complexes (19S assembled with 20S) and ATP-independent for 20S core particles. The 26S activities were …
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