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5. Upregulation of mitochondrial ATPase inhibitory factor 1 (ATPIF1) mediates increased glycolysis in mouse hearts

6. Danicamtiv Increases Myosin Recruitment and Alters Cross-Bridge Cycling in Cardiac Muscle

9. Danicamtiv increases myosin recruitment and alters the chemomechanical cross bridge cycle in cardiac muscle

10. dATP elevation induces myocardial metabolic remodeling to support improved cardiac function

12. Correcting dilated cardiomyopathy with fibroblast-targeted p38 deficiency

13. dATP Elevation Induces Myocardial Metabolic Remodeling to Support Improved Cardiac Function

16. Structural OFF/ON transitions of myosin in relaxed porcine myocardium predict calcium-activated force.

24. ATP binding without hydrolysis switches sulfonylurea receptor 1 (SUR1) to outward-facing conformations that activate KATP channels.

30. Serum Amyloid A Facilitates the Binding of High-Density Lipoprotein From Mice Injected With Lipopolysaccharide to Vascular Proteoglycans

35. Upregulation of mitochondrial ATPase inhibitory factor 1 (ATPIF1) mediates increased glycolysis in mouse hearts.

36. Calcium has a direct effect on thick filament activation in porcine myocardium.

37. Blunted Cardiac Mitophagy in Response to Metabolic Stress Contributes to HFpEF.

39. Danicamtiv increases myosin recruitment and alters the chemomechanical cross bridge cycle in cardiac muscle.

40. Correcting dilated cardiomyopathy with fibroblast-targeted p38 deficiency.

41. ATP binding without hydrolysis switches sulfonylurea receptor 1 (SUR1) to outward-facing conformations that activate K ATP channels.

42. The neuronal K + Cl - co-transporter 2 (Slc12a5) modulates insulin secretion.

43. Deficiency of lymphotoxin-α does not exacerbate high-fat diet-induced obesity but does enhance inflammation in mice.

44. Receptors for tumor necrosis factor-alpha play a protective role against obesity and alter adipose tissue macrophage status.

45. Dietary alpha-lipoic acid supplementation inhibits atherosclerotic lesion development in apolipoprotein E-deficient and apolipoprotein E/low-density lipoprotein receptor-deficient mice.

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