© 2004 by European Society of Cardiology
Copyright © 2004, European Society of Cardiology
Defective glycosylation of calsequestrin in heart failure
aProgram in Molecular and Cellular Cardiology, Cardiology Research Division, Department of Medicine, Wayne State University, Elliman Building, Room 1107, 421 E. Canfield Avenue, Detroit, MI 48201, USA
bMichigan Proteome Consortium, Department of Biochemistry, 3B Biochemistry, Wilson Road, East Lansing, MI 48824, USA
cDepartment of Physiology, University of Wisconsin-Madison, 1300 University Ave., Madison, WI 53706, USA
dBarbara Ann Karmanos Cancer Institute, Wayne State University, 716 Harper Professional Office Building, Detroit, MI 48201, USA
* Corresponding author. Tel.: +1-313-5778734; fax: +1-313-5778615. Email address: s.cala{at}wayne.edu
Objective: Levels of Ca2+ regulatory proteins have been extensively analyzed in cardiomyopathies as possible indices of change in sarcoplasmic reticulum (SR) structure and function. Measures of calsequestrin (CSQ), however, a critical protein component of the Ca2+ release complex in junctional sarcoplasmic reticulum, have provided little or no evidence of underlying dysfunction. We previously reported that calsequestrin isolated from heart tissue exists in a variety of glycoforms and phosphoforms reflecting mannose trimming of N-linked glycans and phosphorylation and dephosphorylation on protein kinase CK2-sensitive sites. Methods: Here, we tested whether the distribution of molecular forms changes in heart failure (HF) reflecting possible remodeling of diseased tissue. Canine hearts were paced (220 beats/min) for 6–8 weeks to induce heart failure. Calsequestrin was purified from heart failure and sham-operated (control) treated canine ventricles and analyzed by electrospray mass spectrometry. Results: The results showed striking changes in the mass distribution of calsequestrin molecules present in tissue from heart failure (five animals) compared with control (five animals). In heart failure, calsequestrin contained glycan structures that were uncharacteristic of normal junctional sarcoplasmic reticulum, consistent with altered metabolism or altered trafficking through secretory compartments. Glycoforms containing Man8,9, expected for a phenotype less muscle-like, were more than doubled in heart failure hearts, and molecules were also phosphorylated to a higher level. Conclusions: These data reveal in tachycardia-induced heart failure a new and potentially important change in the mannose content of calsequestrin glycans, perhaps indicative of defective junctional SR trafficking and Ca2+ release complex assembly.
KEYWORDS Calsequestrin; Mass spectrometry; Heart failure; Phosphorylation; CK2; SR
Time for primary review 17 days
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