Influence of Exercise and Genistein to Mitigate the Deleterious Effects of High-Fat High-Sugar Diet on Alzheimer's Disease-Related Markers in Male Mice.
Juhi ShahTyler OroszAvneet SinghSavan Parameshwar LaxmaRachel E GrossNicholas SmithSpencer VroegopSydney SudlerJames T PorterMaria ColonLauren JunJeganathan R BabuMinsub ShimThomas L BroderickLayla Al-NakkashPublished in: International journal of molecular sciences (2024)
The prevalence of obesity and related consequences, including insulin resistance and Alzheimer's-like neuropathology, has increased dramatically. Contributing to this prevalence is the shift in lifestyle preference away from wholesome foods and exercise to the Western-style diet and sedentarism. Despite advances in drug development, a healthy diet and regular exercise remain the most effective approaches to mitigating the unwanted sequelae of diet-induced obesity on brain health. In this study, we used the high-fat high-sugar (HFHS) mouse model of neurodegeneration to examine the effects of exercise training (HFHS+Ex), genistein treatment (HFHS+Gen), and combination treatment (HFHS+Ex+Gen) on proteins relating to neurodegeneration in the brain of male mice. After a period of 12 weeks, as expected, HFHS feeding increased body weight, adipose tissue weight, and systemic plasma inflammation (TNF-α) compared to lean mice fed a standard diet. HFHS feeding also increased protein expression of brain markers of insulin resistance (pGSK-3β, p-IR), apoptosis (caspase 3), early neurofibrillary tangles (CP13), and amyloid-beta precursor (CT20). Compared to HFHS mice, Ex decreased body weight, plasma TNF-α, and expression of pGSK-3β, caspase 3, CP13, amyloid-β precursor (22c11), and ADAM10. Treatment with Gen was equally protective on these markers and decreased the expression of p-IR. Combination treatment with Ex and Gen afforded the greatest overall benefits, and this group exhibited the greatest reduction in body and adipose tissue weight and all brain markers, except for 22c11 and ADAM10, which were decreased compared to mice fed an HFHS diet. In addition, levels of 4G8, which detects protein levels of amyloid-β, were decreased with combination treatment. Our results indicate that exercise training, genistein supplementation, or combination treatment provide varying degrees of neuroprotection from HFHS feeding-induced Alzheimer's pathology. Future perspectives could include evaluating moderate exercise regimens in combination with dietary supplementation with genistein in humans to determine whether the same benefits translate clinically.
Keyphrases
- insulin resistance
- adipose tissue
- physical activity
- weight loss
- body weight
- high fat diet induced
- mouse model
- metabolic syndrome
- rheumatoid arthritis
- oxidative stress
- high intensity
- body mass index
- white matter
- public health
- computed tomography
- risk assessment
- healthcare
- small molecule
- high fat diet
- weight gain
- multiple sclerosis
- cardiovascular disease
- magnetic resonance imaging
- cell proliferation
- replacement therapy
- postmenopausal women
- drug induced
- climate change
- endoplasmic reticulum stress
- image quality
- diabetic rats
- amino acid