Intrasarcoplasmic Amyloidosis Impairs Proteolytic Function of Proteasomes in Cardiomyocytes by Compromising Substrate Uptake

doi:10.1161/01.RES.0000189262.92896.0b

Circulation Research. 2005
Published online before print October 6, 2005, doi: 10.1161/01.RES.0000189262.92896.0b

A more recent version of this article appeared on November 11, 2005

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Submitted on June 27, 2005
Revised on September 20, 2005
Accepted on September 27, 2005

Intrasarcoplasmic Amyloidosis Impairs Proteolytic Function of Proteasomes in Cardiomyocytes by Compromising Substrate Uptake

Quanhai Chen ; Jin-Bao Liu ; Kathleen M. Horak ; Hanqiao Zheng ; Asangi R.K. Kumarapeli ; Jie Li ; Faqian Li ; A. Martin Gerdes ; Eric F. Wawrousek ; and Xuejun Wang ^*

From the Cardiovascular Research Institute (Q.C., J.-B.L., K.M.H., H.Z., A.R.K.K., J.L., F.L., A.M.G., X.W.), South Dakota Health Research Foundation, University of South Dakota School of Medicine and Sioux Valley Hospitals and Health System, Sioux Falls; National Eye Institute (E.F.W.), National Institutes of Health, Bethesda, Md; Department of Pathophysiology (J.-B. L), Guangzhou Medical College, Guangzhou, Guangdong, China; and Department of Laboratory Medicine (F. L.) and Division of Basic Biomedical Sciences (Q.C., J.-B.L., K.M.H., H.Z., A.R.K.K., J.L., X.W.), University of South Dakota School of Medicine, Sioux Falls.

^* To whom correspondence should be addressed. E-mail: xwang{at}usd.edu.

The presence of increased ubiquitinated proteins and amyloidoligomers in failing human hearts strikingly resembles the characteristicpathology in the brain of many neurodegenerative diseases. Theubiquitin-proteasome system (UPS) is responsible for degradationof most cellular proteins and plays essential roles in virtuallyall cellular processes. UPS impairment by aberrant protein aggregationwas previously shown in cell culture but remains to be demonstratedin intact animals. Mechanisms underlying the impairment arepoorly understood. We report here that UPS proteolytic functionis severely impaired in the heart of a mouse model of intrasarcoplasmicamyloidosis caused by cardiac-restricted expression of a humandesmin-related myopathy-linked missense mutation of ${alpha}$ B-crystallin(CryAB^R120G). The UPS impairment was detected before cardiachypertrophy, and failure became discernible, suggesting thatdefective protein turnover likely contributes to cardiac remodelingand failure in this model. Further analyses reveal that theimpairment is likely attributable to insufficient delivery ofsubstrate proteins into the 20S proteasomes, and depletion ofkey components of the 19S subcomplex may be responsible. Thederangement is likely caused by aberrant protein aggregationrather than loss of function of the CryAB gene because UPS malfunctionwas not evident in CryAB-null hearts and inhibition of aberrantprotein aggregation by Congo red or a heat shock protein significantlyattenuated CryAB^R120G-induced UPS malfunction in cultured cardiomyocytes.Because of the central role of the UPS in cell regulation andthe high intrasarcoplasmic amyloidosis prevalence in failinghuman hearts, our data suggest a novel pathogenic process incardiac disorders with abnormal protein aggregation.

Key words: proteasome • ubiquitin • protein aggregation • ${alpha}$ B-crystallin • desmin-related cardiomyopathy • amyloidosis • transgenic mice

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				X. Wang and J. Robbins Heart Failure and Protein Quality Control Circ. Res., December 8, 2006; 99(12): 1315 - 1328. [Abstract] [Full Text] [PDF]

				A. V. Gomes, C. Zong, R. D. Edmondson, X. Li, E. Stefani, J. Zhang, R. C. Jones, S. Thyparambil, G.-W. Wang, X. Qiao, et al. Mapping the Murine Cardiac 26S Proteasome Complexes Circ. Res., August 18, 2006; 99(4): 362 - 371. [Abstract] [Full Text] [PDF]

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