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1. A role for the cerebellum in the control of verbal interference: Comparison of bilingual and monolingual adults.

2. Evidence against a cognitive advantage in the older bilingual population.

3. Mortality Risk in Alcoholic Patients in Northern Italy: Comorbidity and Treatment Retention Effects in a 30-Year Follow-Up Study.

4. Mortality Risk in Alcoholic Patients in Northern Italy: Comorbidity and Treatment Retention Effects in a 30-Year Follow-Up Study.

5. GLP-1(32-36)amide Pentapeptide Increases Basal Energy Expenditure and Inhibits Weight Gain in Obese Mice.

6. GLP-1-derived nonapeptide GLP-1(28–36)amide inhibits weight gain and attenuates diabetes and hepatic steatosis in diet-induced obese mice

7. GLP-1-derived nonapeptide GLP-1(28–36)amide targets to mitochondria and suppresses glucose production and oxidative stress in isolated mouse hepatocytes

8. Insulin-like actions of glucagon-like peptide-1: a dual receptor hypothesis

9. Role of Disulfide Bonds in Acrp30/Adiponectin Structure and Signaling Specificity.

10. Enhanced muscle fat oxidation and glucose transport by ACRP30 globular domain: Acetyl-CoA carboxylase inhibition and AMP-activated protein kinase activation.

11. Developmental trajectories of metacognitive processing and executive function from childhood to older age.

12. AMP-activated protein kinase and its regulation by adiponectin and interleukin-6.

13. Mice Lacking Adiponectin Show Decreased Hepatic Insulin Sensitivity and Reduced Responsiveness to Peroxisome Proliferator-activated Receptor γ Agonists.

14. Developmental trajectories of control of verbal and non-verbal interference in speech comprehension in monolingual and multilingual children.

15. FGF21 does not require interscapular brown adipose tissue and improves liver metabolic profile in animal models of obesity and insulin-resistance.

16. GLP-1(32–36)amide, a novel pentapeptide cleavage product of GLP-1, modulates whole body glucose metabolism in dogs.

17. Thiazolidinediones can rapidly activate AMP-activated protein kinase in mammalian tissues.

18. AICAR administration causes an apparent enhancement of muscle and liver insulin action in insulin-resistant high-fat-fed rats.

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