Targeted Disruption of the Mouse Sod I Gene Makes the Hearts Vulnerable to Ischemic Reperfusion Injury

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Circulation Research. 2000;86:264-269

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	Genetically altered mice
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(Circulation Research. 2000;86:264.)
© 2000 American Heart Association, Inc.

Integrative Physiology

Targeted Disruption of the Mouse Sod I Gene Makes the Hearts Vulnerable to Ischemic Reperfusion Injury

Tetsuya Yoshida, Nilanjana Maulik, Richard M. Engelman, Ye-Shih Ho, Dipak K. Das

From the Cardiovascular Research Center (T.Y., N.M., R.M.E., D.K.D.), Department of Surgery, University of Connecticut School of Medicine, Farmington, Conn, and Institute of Chemical Toxicology (Y.-S.H.), Wayne State University, Detroit, Mich.

Correspondence to Dipak K. Das, University of Connecticut, School of Medicine, Cardiovascular Research Center, Department of Surgery, Farmington, CT 06030-1110. E-mail ddas{at}neuron.uchc.edu

Abstract—The role of Cu/Zn–superoxide dismutase(SOD) in myocardial ischemic reperfusion injury was studiedby using a mouse model with targeted disruption of the mouseSod I gene. Inactivation of the functional mouse Sod I genein hearts by gene targeting (Sod I^+/-) resulted in a 50% reductionof Cu/Zn-SOD mRNA and significant reduction of Cu/Zn-SOD enzymeactivity compared with that of wild-type Sod I^+/+ mice. Cu/Zn-SODmRNA could not be detected in Sod I^-/- heart. The isolated buffer-perfusedhearts from the knockout mice devoid of any functional copyof the Sod I (Sod I^-/-) and matched nontransgenic control micewere subjected to 30 minutes of global ischemia followed by2 hours of reperfusion. For both groups of mice, the postischemicfunctional recovery for the hearts was lower than the baseline,but the recovery for the Sod I^-/- was less compared with thewild-type mice. Thus, the postischemic recovery of the developedforce and the maximum first derivative of the developed forcewere consistently lower for the Sod I^-/- mouse hearts comparedwith wild-type control hearts. The coronary flow was lower comparedwith the baseline levels for both groups of hearts, but therewas no significant difference between the groups. The myocardialinfarction determined from the ratio of infarct size/area ofrisk was higher for the Sod I^-/- mice compared with the control mice.The amount of creatine kinase release from the wild-type mouse heartswas less compared with the Sod I^-/- mouse hearts. In concert,a reduced amount of oxidative stress was found in the heartsof wild-type mice compared with Sod I^-/- mouse hearts. Theseresults documented that Sod I^-/- mouse hearts were more susceptibleto ischemic reperfusion injury compared with corresponding wild-typemouse hearts, suggesting that the Sod I gene constitutes animportant defense element for the hearts.

Key Words: transgenic • knockout • ischemia/reperfusion • free radicals • oxidative stress

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