Description |
Lifelong over-expression of GLUT1 transporter in the heart has been shown to preserve contractile function after aortic constriction. However it is unclear whether this protective effect is due to GLUT1 overexpression itself or due to reprogramming of heart metabolism as a result of long-term increased glucose utilization. We, therefore generated mice with cardiomyocyte-restricted inducible overexpression of GLUTI(GIHA) to test if short-term GLUT1 overexpression at the onset of pressure overload hypertrophy (POH) is sufficient to prevent the progression to heart failure in a model of POH. Six-week old mice were subjected to transverse aortic constriction (TAC) to induce POH. GLUT1 transgene expression was initiated 2 days prior to TAC surgery and resulted in a 4-fold increase in cardiac GLUT1 protein levels relative to controls. Four weeks after TAC, cardiac contractile function was equivalently impaired in control and G1HA mice, as shown by increased left ventricular developed pressure and decreased in maximal dp/dt ratio. In contrast, mitochondrial function following TAC was preserved and fibrosis was significantly decreased in G1HA mice relative to control. In summary, our data suggest that a short-term increase in GLUT 1-mediated glucose uptake preserves mitochondrial function and attenuates pathological remodeling, but does not prevent cardiac dysfunction following POH. |