Table 2.
The Phenotypes of Mouse Models with Genetically Modified GLUTs
| Isoform | Overexpression or knockout | Tissue specific | General phenotype | Cardiac phenotype | Reference |
|---|---|---|---|---|---|
| GLUT1 | Overexpression | Skeletal muscle | Increase basal glucose uptake | n.d. | (73) |
| GLUT1 | Overexpression | Cardiac | Increase glucose uptake, glycolysis, and glycogen storage | Protect from pressure overload and ischemia induced heart failure; promote cardiac dysfunction in high fat diet induced obesity model | (125,135,259) |
| GLUT1 | Inducible overexpression | Cardiac | n.d. | Preserve mitochondria function; exacerbates hypertrophic phenotype | (173) |
| GLUT4 | Overexpression | Systematic* | Increased glucose uptake, glycolysis and glycogen in skeletal and cardiac muscle reduced fasting plasma glucose levels; improved glucose tolerance in high fat diet and db/db diabetic model | n.d. | (14,66,77,86) |
| GLUT4 | Overexpression | Skeletal and cardiac muscle | Improve insulin action; reduce basal blood glucose levels in streptozotocin-induced diabetic mice | n.d. | (121) |
| GLUT1 | Knock out | Systematic | Homozygous: lethal Heterozygous: growth retardation; severe brain dysfunction | n.d. | (80,248) |
| GLUT4 | Knock out | Systematic* | Homozygous: growth-retarded, shorter life span with normal blood glucose level Heterozygous: reduce muscle glucose uptake; develop hyperglycemia and hyperinsulinemia | Homozygous: severe cardiac hypertrophy and dysfunction | (101,220) |
| GLUT4 | Knockout | Cardiac | Normal systematic glucose metabolism with normal life span | Normal cardiac function with moderate hypertrophy at baseline. Impair glycolysis and exacerbate ischemia reperfusion injury | (1,232) |
Note. n.d. not determined. Systematic *refers to overexpression or knock out of GLUT4 at the sites where endogenous GLUT4 is expressed.