Lewandowski E Douglas, O'donnell J Michael, Scholz Thomas D, Sorokina Natalia, Buttrick Peter M
Program in Integrative Cardiac Metabolism, 835 S. Wolcott Ave., MC901, University of Illinois, College of Medicine, Chicago, IL 60612, USA.
Am J Physiol Cell Physiol. 2007 May;292(5):C1880-6. doi: 10.1152/ajpcell.00576.2006. Epub 2007 Jan 17.
Glucose metabolism in the heart requires oxidation of cytosolic NADH from glycolysis. This study examines shuttling reducing equivalents from the cytosol to the mitochondria via the activity and expression of the oxoglutarate-malate carrier (OMC) in rat hearts subjected to 2 wk (Hyp2, n = 6) and 10 wk (Hyp10, n = 8) of pressure overload hypertrophy vs. that of sham-operated rats (Sham2, n = 6; and Sham10, n = 7). Moderate aortic banding produced increased atrial natriuretic factor (ANF) mRNA expression at 2 and 10 wk, but only at 10 wk did hearts develop compensatory hypertrophy (33% increase, P < 0.05). Isolated hearts were perfused with the short-chain fatty acid [2,4-(13)C(2)]butyrate (2 mM) and glucose (5 mM) to enable dynamic-mode (13)C NMR of intermediate exchange across OMC. OMC flux increased before the development of hypertrophy: Hyp2 = 9.6 +/- 2.1 vs. Sham2 = 3.7 +/- 1.2 muM.min(-1).g dry wt(-1), providing an increased contribution of cytosolic NADH to energy synthesis in the mitochondria. With compensatory hypertrophy, OMC flux returned to normal: Hyp10 = 3.9 +/- 1.7 vs. Sham10 = 3.8 +/- 1.2 muM.g(-1).min(-1). Despite changes in activity, no differences in OMC expression occurred between Hyp and Sham groups. Elevated OMC flux represented augmented cytosolic NADH shuttling, coupled to increased nonoxidative glycolysis, in response to hypertrophic stimulus. However, development of compensatory hypertrophy moderated the pressure-induced elevation in OMC flux, which returned to control levels. The findings indicate that the challenge of pressure overload increases cytosolic redox state and its contribution to mitochondrial oxidation but that hypertrophy, before decompensation, alleviates this stress response.
心脏中的葡萄糖代谢需要糖酵解产生的胞质NADH进行氧化。本研究通过检测大鼠心脏中α-酮戊二酸-苹果酸载体(OMC)的活性和表达,研究了压力超负荷肥大2周(Hyp2,n = 6)和10周(Hyp10,n = 8)时,还原当量从胞质向线粒体的穿梭情况,并与假手术大鼠(Sham2,n = 6;Sham10,n = 7)进行比较。适度的主动脉缩窄在2周和10周时使心房利钠因子(ANF)mRNA表达增加,但仅在10周时心脏出现代偿性肥大(增加33%,P < 0.05)。用短链脂肪酸[2,4-(13)C(2)]丁酸(2 mM)和葡萄糖(5 mM)灌注离体心脏,以实现通过OMC进行中间交换的动态模式(13)C NMR。在肥大发生前,OMC通量增加:Hyp2 = 9.6 +/- 2.1 μM·min(-1)·g干重(-1),而Sham2 = 3.7 +/- 1.2 μM·min(-1)·g干重(-1),这使得胞质NADH对线粒体能量合成的贡献增加。随着代偿性肥大出现,OMC通量恢复正常:Hyp10 = 3.9 +/- 1.7 μM·g(-1)·min(-1),而Sham10 = 3.8 +/- 1.2 μM·g(-1)·min(-1)。尽管活性发生了变化,但Hyp组和Sham组之间OMC的表达没有差异。OMC通量升高代表着响应肥大刺激,胞质NADH穿梭增加,并与非氧化糖酵解增加相关。然而,代偿性肥大的发展减轻了压力诱导的OMC通量升高,使其恢复到对照水平。研究结果表明,压力超负荷的挑战增加了胞质氧化还原状态及其对线粒体氧化的贡献,但在失代偿前,肥大减轻了这种应激反应。
