Decrease in sarcoglycans and dystrophin in failing heart following acute myocardial infarction

doi:10.1016/S0008-6363(03)00385-7

Cardiovascular Research 2003 59(2):419-427; doi:10.1016/S0008-6363(03)00385-7
© 2003 by European Society of Cardiology

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Decrease in sarcoglycans and dystrophin in failing heart following acute myocardial infarction

Hiroyuki Yoshida^a, Masaya Takahashi^a, Miki Koshimizu^a, Kouichi Tanonaka^a, Ryo Oikawa^a, Teruhiko Toyo-oka^b and Satoshi Takeo^a^,*

^aDepartment of Pharmacology, Tokyo University of Pharmacy and Life Science, 1432-1 Horinouchi, Hachioji, Tokyo 192-0392, Japan
^bDepartment of Organ Pathophysiology and Internal Medicine, Tokyo University Hospital, Tokyo 113-8655, Japan

^* Corresponding author. Tel.: +81-426-76-4583; fax: +81-426-76-5560. takeos{at}ps.toyaku.ac.jp

Objective: Genetic defects in several sarcoglycans (SGs) anddystrophin (Dys) play a critical role in cardiomyopathy. Thepresent study was designed to determine whether changes in SGsand Dys might occur in animals with chronic heart failure (CHF)induced by acute myocardial infarction (AMI), which have nogenetic defects. Methods: AMI was induced by the left coronaryartery ligation (CAL) in rats. The hemodynamic parameters ofthe 2- and 8-week CAL (2w- and 8w-CAL) rats were measured andthe myocardial SGs, Dys, calpain, and calpastatin levels weredetermined by the Western blot method. Myocardial calpain-likeprotease activity was evaluated as caseinolysis activity. Results:Increases in left ventricular end-diastolic pressure (LVEDP)and right ventricular systolic pressure, and a decrease in ±dP/dtwere observed at the 2nd week, whereas cardiac output index(COI) was preserved. In contrast, the 8w-CAL rats showed a furtherincrement in LVEDP with low COI. ${alpha}$ -SG of the viable left ventricle(LV), and septum (Sep) of the 8w-CAL rat decreased (60–70%of the control). The ${alpha}$ - and β-SGs of the right ventricle(RV) of the 2w- and 8w-CAL rats were reduced, while ${gamma}$ - and ${delta}$ -SGsin the three regions did not change significantly. Dys in theviable LV and RV of the 8w-CAL rat decreased (75% of the control).The amount of m-calpain in the three regions of the 2w- and8w-CAL rats increased (140–200% of the control), whereasthe endogenous calpain inhibitor, calpastatin, did not changesignificantly. The in vitro degradation studies using purifiedm-calpain or cytosolic fractions of the 8w-CAL rat heart suggesteda reduction in SGs and Dys by calpain. Conclusion: The resultssuggest that a decrease in SGs and Dys may play an importantrole in the pathophysiology of CHF following AMI.

KEYWORDS Calpain; Dystrophin; Heart failure; Hemodynamics; Sarcoglycan

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