Dissociation of Sarcoglycans and the Dystrophin Carboxyl Terminus From the Sarcolemma in Enteroviral Cardiomyopathy

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Circulation Research. 2000;87:489-495

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(Circulation Research. 2000;87:489.)
© 2000 American Heart Association, Inc.

Cellular Biology

Dissociation of Sarcoglycans and the Dystrophin Carboxyl Terminus From the Sarcolemma in Enteroviral Cardiomyopathy

Gil-Hwan Lee¹, Cornel Badorff¹, Kirk U. Knowlton

From the Department of Medicine, University of California, San Diego (La Jolla). Dr Lee’s present address is the Department of Internal Medicine, Catholic University of Korea, Seoul, Korea. Dr Badorff’s present address is the Department of Cardiology, Goethe-University, Frankfurt/Main, Germany.

Correspondence to Kirk U. Knowlton, MD, Department of Medicine, 0613K, University of California, San Diego, 9500 Gilman Dr, La Jolla, CA 92093-0613. E-mail kknowlton{at}ucsd.edu

Abstract—Enteroviral infection can cause an acquired formof dilated cardiomyopathy. We recently reported that dystrophinis cleaved, functionally impaired, and morphologically disruptedin vitro as well as in vivo during infection with coxsackievirusB3. Genetic dystrophin truncations lead to a marked decreasein dystrophin-associated glycoproteins, whereas expression ofonly the naturally occurring dystrophin carboxyl terminus, Dp-71,restores the sarcolemmal association of the dystrophin-associatedglycoproteins. We sought to determine whether acute cleavageof dystrophin leads to a dissociation of the carboxyl-terminaldystrophin fragment and of the sarcoglycans from the sarcolemmaduring coxsackievirus B3 infection. We found that in culturedcardiac myocytes and murine hearts infected with coxsackievirusB3, the sarcolemmal localization of the dystrophin carboxylterminus is lost. The dystrophin-associated glycoproteins ${alpha}$ -,ß-, ${gamma}$ -, and ${delta}$ -sarcoglycan and ß-dystroglycan weremarkedly decreased in the membrane fraction of infected cellsin culture, and the typical sarcolemmal localization for eachof these proteins was lost in coxsackievirus-B3–infected cardiomyocytesin vivo. Furthermore, sucrose gradient ultracentrifugation demonstratedthat ${delta}$ -sarcoglycan was physically dissociated from dystrophinwithin the membrane fraction. In vivo, the sarcolemmal integritywas functionally impaired with Evans blue dye uptake even thoughthere was no generalized disruption of the sarcolemma of infectedmyocytes evidenced by intact wheat germ agglutinin staining.In analogy to hereditary sarcoglycanopathies, this disintegrationof the sarcoglycan complex may, in addition to the dystrophincleavage, play an important role in the pathogenesis of enterovirus-induced cardiomyopathy.These results imply a potential role for disruption of the sarcoglycansin an acquired form of heart failure.

Key Words: heart failure • cardiomyopathy • sarcoglycans • myocarditis • coxsackievirus

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