Targeted inactivation of hepatocyte growth factor receptor c-met in β-cells leads to defective insulin secretion and GLUT-2 downregulation without alteration of β-cell mass

Keyphrases

• Glucose Transporter 2 (GLUT2) 100%
• Insulin Secretion 100%
• Cell Mass 100%
• Islet 100%
• C-Met 100%
• Hepatocyte Growth Factor Receptor 100%
• Cell Function 75%
• Hepatocyte Growth Factor 75%
• Cell Proliferation 50%
• Plasma Insulin 50%
• Cell Growth 50%
• Glucose-stimulated Insulin Secretion 50%
• High Glucose 25%
• Glucose Tolerance 25%
• Transgenic Mice 25%
• Cell Survival 25%
• Overexpression 25%
• Insulin 25%
• Insulin Resistance 25%
• Blood Glucose 25%
• Glucokinase 25%
• Littermate 25%
• Physiological Role 25%
• Exogenous Insulin 25%
• Glucose-insulin System 25%
• Impaired Glucose Tolerance 25%
• Conditional Ablation 25%
• Islet Cells 25%
• Normal Weight 25%
• Glucose Challenge 25%
• Blood Plasma 25%
• Cell Composition 25%
• Doublet 25%
• MET Signaling 25%
• Islet Morphology 25%

Biochemistry, Genetics and Molecular Biology

• Downregulation 100%
• Growth Factor Receptor 100%
• Insulin Release 100%
• Hepatocyte Growth Factor 100%
• GLUT2 100%
• Cell Function 75%
• Cell Proliferation 50%
• Cell Growth 50%
• Insulin Blood Level 50%
• Body Weight 25%
• Transgenic Mouse 25%
• Cell Survival 25%
• Insulin Resistance 25%
• Glucokinase 25%
• Glucose Blood Level 25%
• Impaired Glucose Tolerance 25%
• Cell Composition 25%

Immunology and Microbiology

• Hepatocyte Growth Factor 100%
• Downregulation 100%
• Insulin Release 100%
• Glucose Transporter 100%
• Cell Function 75%
• Cell Proliferation 50%
• Cell Growth 50%
• Insulin Blood Level 50%
• Insulin 50%
• Cell Survival 25%
• Insulin Resistance 25%
• Glucose Blood Level 25%
• Transgenic Mouse 25%
• Body Weight 25%
• Cell Composition 25%
• In Vitro 25%