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1. The mouse metabolic phenotyping center (MMPC) live consortium: an NIH resource for in vivo characterization of mouse models of diabetes and obesity.

2. Endothelial β1-integrins are necessary for microvascular function and glucose uptake.

4. Epoxygenase Cyp2c44 Regulates Hepatic Lipid Metabolism and Insulin Signaling by Controlling FATP2 Localization and Activation of the DAG/PKCδ Axis.

5. Exercise training adaptations in liver glycogen and glycerolipids require hepatic AMP-activated protein kinase in mice.

6. Insulin, Muscle Glucose Uptake, and Hexokinase: Revisiting the Road Not Taken.

7. Capillary Endothelial Insulin Transport: The Rate-limiting Step for Insulin-stimulated Glucose Uptake.

8. EET Analog Treatment Improves Insulin Signaling in a Genetic Mouse Model of Insulin Resistance.

9. Exercise and Adipose Tissue Immunity: Outrunning Inflammation.

10. Reciprocity Between Skeletal Muscle AMPK Deletion and Insulin Action in Diet-Induced Obese Mice.

11. Influence of the integrin alpha-1 subunit and its relationship with high-fat diet upon extracellular matrix synthesis in skeletal muscle and tendon.

12. American Heart Association Vascular Disease Strategically Focused Research Network.

14. Transendothelial Insulin Transport is Impaired in Skeletal Muscle Capillaries of Obese Male Mice.

15. Perfusion controls muscle glucose uptake by altering the rate of glucose dispersion in vivo.

16. CD44 contributes to hyaluronan-mediated insulin resistance in skeletal muscle of high-fat-fed C57BL/6 mice.

17. Fibrotic Encapsulation Is the Dominant Source of Continuous Glucose Monitor Delays.

19. Energy metabolism couples hepatocyte integrin-linked kinase to liver glucoregulation and postabsorptive responses of mice in an age-dependent manner.

20. Rapid changes in the microvascular circulation of skeletal muscle impair insulin delivery during sepsis.

21. SIRT2 knockout exacerbates insulin resistance in high fat-fed mice.

22. CETP Inhibition Improves HDL Function but Leads to Fatty Liver and Insulin Resistance in CETP-Expressing Transgenic Mice on a High-Fat Diet.

23. Acute Nitric Oxide Synthase Inhibition Accelerates Transendothelial Insulin Efflux In Vivo.

24. Automated quantification of microvascular perfusion.

25. Reduced Nonexercise Activity Attenuates Negative Energy Balance in Mice Engaged in Voluntary Exercise.

27. Integrin-Linked Kinase Is Necessary for the Development of Diet-Induced Hepatic Insulin Resistance.

28. Liver AMP-Activated Protein Kinase Is Unnecessary for Gluconeogenesis but Protects Energy State during Nutrient Deprivation.

30. Integrin-Linked Kinase in Muscle Is Necessary for the Development of Insulin Resistance in Diet-Induced Obese Mice.

32. SIRT3 Is Crucial for Maintaining Skeletal Muscle Insulin Action and Protects Against Severe Insulin Resistance in High-Fat-Fed Mice.

33. CETP Expression Protects Female Mice from Obesity-Induced Decline in Exercise Capacity.

34. Mass spectrometry-based microassay of ²H and 13C plasma glucose labeling to quantify liver metabolic fluxes in vivo.

35. Enhanced Mitochondrial Superoxide Scavenging Does Not Improve Muscle Insulin Action in the High Fat-Fed Mouse.

36. Heterozygous SOD2 Deletion Impairs Glucose-Stimulated Insulin Secretion, but Not Insulin Action, in High-Fat-Fed Mice.

37. Diminishing impairments in glucose uptake, mitochondrial content, and ADP-stimulated oxygen flux by mesenchymal stem cell therapy in the infarcted heart.

38. Glucose-6-Phosphate-Mediated Activation of Liver Glycogen Synthase Plays a Key Role in Hepatic Glycogen Synthesis.

40. Mesenchymal stem cell transplantation for the infarcted heart: therapeutic potential for insulin resistance beyond the heart.

41. Relaxin Treatment Reverses Insulin Resistance in Mice Fed a High-Fat Diet.

42. Hyaluronan Accumulates With High-Fat Feeding and Contributes to Insulin Resistance.

43. Muscle-Specific Vascular Endothelial Growth Factor Deletion Induces Muscle Capillary Rarefaction Creating Muscle Insulin Resistance.

44. AS160 deficiency causes whole-body insulin resistance via composite effects in multiple tissues.

45. Transgenic mice overexpressing renin exhibit glucose intolerance and diet-genotype interactions.

47. Regulation of Endogenous Glucose Production in Glucose Transporter 4 Over-Expressing Mice.

48. Toll-like Receptor 4 Deficiency Promotes the Alternative Activation of Adipose Tissue Macrophages.

49. Mesenchymal stem cell transplantation for the infarcted heart: a role in minimizing abnormalities in cardiac-specific energy metabolism.

50. Overproduction of Angiotensinogen from Adipose Tissue Induces Adipose Inflammation, Glucose Intolerance, and Insulin Resistance.

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