Aortic banding in rats induced cardiac hypertrophy with selectively enhanced protein expression of PKC-delta (up to 289±12%) and PKC-alpha (up to 212±20%) compared to sham operation.
Pressure-overload cardiac hypertrophy in rats is associated with differential upregulation of specific PKC isozymes (PKC-alpha and PKC-delta) at both the protein and mRNA levels.
OBJECTIVE: Protein kinase C (PKC) plays a key role in myocardial hypertrophy. To evaluate whether its isoforms are expressed differentially during gradual development of pressure-overload-induced cardiac hypertrophy, banding of the ascending aorta was used as an experimental model of left ventricular hypertrophy. METHODS: One, 7 and 30 days after sham operation or aortic banding in male Wistar rats, the PKC activity and the expression of the cardiac PKC isozymes (PKC-alpha, -delta, - epsilon and -zeta), both at the protein and the mRNA level, were determined in the left and right ventricle. RESULTS: Left ventricular hypertrophy developed rapidly as early as 1 day after aortic banding followed by further progression at day 7 and day 30. This was paralleled by an increased total PKC enzyme activity in the cytosol fraction and a selectively enhanced protein expression of PKC-delta (day 7, 267+/-18%; day 30, 289+/-12%) and PKC-alpha (day 7, 212+/-20%; day 30, 193+/-14%). The protein amount of PKC- epsilon was not changed in either group. This differential protein expression was associated with a significant increase of the absolute mRNA levels for PKC-delta and PKC-alpha up to 202+/-20% (day 30) and 177+/-17% (day 30), whereas significant alterations in the PKC- epsilon mRNA levels were not detected. A selective upregulation of PKC-alpha and PKC-delta, both on the protein and on the mRNA level, was also noted in the right ventricle during the development of right ventricular hypertrophy, suggesting an adaptive response following elevated left ventricular enddiastolic pressure after long-term aortic banding for 30 days. CONCLUSIONS: This study characterizes in the right and left ventricle a differential regulation of the dominant PKC isozymes in pressure-overload cardiac hypertrophy both at the protein and the mRNA level.
Martin Braun (Tue,) conducted a other in pressure-overload-induced cardiac hypertrophy. Aortic banding vs. Sham operation was evaluated on PKC activity and expression of cardiac PKC isozymes (PKC-alpha, -delta, -epsilon and -zeta). Aortic banding in rats induced cardiac hypertrophy with selectively enhanced protein expression of PKC-delta (up to 289±12%) and PKC-alpha (up to 212±20%) compared to sham operation.