QL treatment promoted glucose oxidation and free fatty acid (FFA) uptake in a HIF-1α-independent manner. (a) QL promoted CS protein activity (/group). (b and c) QL elevated PDH and CS protein expressions, while the HIF-1α inhibitor did not significantly attenuate this effect (/group). (d) QL decreased serum FFA levels (/group). (e and f) QL significantly promoted FFA uptake by increasing the expressions of CD36 and PGC-1α, which were downregulated in the MI group, and the HIF-1α inhibitor could not reversed this effect (/group). Data are expressed as . and compared with the sham group; ^# and ^## compared with the MI group.