Tight Control of Exogenous SERCA Expression Is Required to Obtain Acceleration of Calcium Transients With Minimal Cytotoxic Effects in Cardiac Myocytes

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Circulation Research. 2001;88:415-421

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	Apoptosis
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(Circulation Research. 2001;88:415.)
© 2001 American Heart Association, Inc.

Cellular Biology

Tight Control of Exogenous SERCA Expression Is Required to Obtain Acceleration of Calcium Transients With Minimal Cytotoxic Effects in Cardiac Myocytes

J. Michael O’Donnell, Carlota M. Sumbilla, Hailun Ma, Iain K. G. Farrance, Marco Cavagna, Michael G. Klein, Giuseppe Inesi

From the Department of Biochemistry and Molecular Biology, University of Maryland School of Medicine, Baltimore, Md.

Correspondence to Giuseppe Inesi, University of Maryland, 108 N Greene St, Baltimore, MD 21201-1503. E-mail ginesi{at}umaryland.edu

Abstract—Collateral effects of exogenous sarcoendoplasmicreticulum Ca²⁺ ATPase (SERCA) expression were characterizedin neonatal rat and chicken embryo cardiac myocytes, and theconditions required to produce acceleration of Ca²⁺ transientswith minimal toxicity were established. Cultured myocytes wereinfected with adenovirus vector carrying the cDNA of wild-typeSERCA1, an inactive SERCA1 mutant, or enhanced green fluorescenceprotein under control of the cytomegalovirus promoter. Controlswere exposed to empty virus vector. Each group was tested withand without phenylephrine (PHE) treatment. Under conditionsof limited calf-serum exposure, the infected rat myocytes manifesteda more rapid increase in size, protein content, and rate ofprotein synthesis relative to noninfected controls. These changeswere not accompanied by reversal to fetal transcriptional pattern(as observed in hypertrophy triggered by PHE) and may be attributableto facilitated exchange with serum factors. SERCA virus titers>5 to 6 plaque-forming units per cell produced overcrowdingof ATPase molecules on intracellular membranes, followed byapoptotic death of a significant number of rat but not chickenmyocytes. Enhanced green fluorescence protein virus and emptyvirus also produced cytotoxic effects but at higher titers thanSERCA. Expression of exogenous SERCA and enhancement of Ca²⁺ transientkinetics could be obtained with minimal cell damage in rat myocytesif the SERCA virus titer were maintained within 1 to 4 plaque-formingunits per cell. Expression of endogenous SERCA was unchanged,but expression of exogenous SERCA was higher in myocytes renderedhypertrophic by treatment with PHE than in nontreated controls.

Key Words: SERCA • gene therapy • heart • adenovirus • calcium transients

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