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5. Non-alcoholic fatty liver disease, and the underlying altered fatty acid metabolism, reveals brain hypoperfusion and contributes to the cognitive decline in APP/PS1 mice

6. Non-Alcoholic Fatty Liver Disease, and the Underlying Altered Fatty Acid Metabolism, Reveals Brain Hypoperfusion and Contributes to the Cognitive Decline in APP/PS1 Mice

7. High Systolic Blood Pressure Induces Cerebral Microvascular Endothelial Dysfunction, Neurovascular Unit Damage, and Cognitive Decline in Mice

11. Expression profile of hepatic genes related to lipid homeostasis in LSR heterozygous mice contributes to their increased response to high-fat diet

12. Role of the lipoprotein receptor LSR (lipolysis stimulated lipoprotein receptor) in brain cholesterol homeostasis and cognitive abilities in aging

17. Increased Susceptibility of Dyslipidemic LSR+/− Mice to Amyloid Stress is Associated with Changes in Cortical Cholesterol Levels

18. Brain region-specific immunolocalization of the lipolysis-stimulated lipoprotein receptor ( LSR) and altered cholesterol distribution in aged LSR+/− mice.

19. Human apolipoprotein E allele and docosahexaenoic acid intake modulate peripheral cholesterol homeostasis in mice

20. Impact of pulse pressure on cerebrovascular events leading to age-related cognitive decline.

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