SIRT1 Activators as Geroprotective Agents in Brain Aging: Mechanisms and Therapeutic Potential.

SIRT1 Activators as Geroprotective Agents in Brain Aging: Mechanisms and Therapeutic Potential.

Publication date: Apr 04, 2026

The brain undergoes profound molecular and structural changes during the aging process, resulting in the development of neurodegeneration, cognitive impairment, and increased vulnerability to chronic diseases. At the cellular level, brain aging is characterized by oxidative damage, genomic instability, and chronic low-grade inflammation known as inflammaging. Central to this process is Sirtuin 1 (SIRT1), a NAD-dependent class III histone deacetylase, known for its regulatory role in chromatin remodeling, oxidative stress responses, mitochondrial biogenesis, and neuroplasticity. Recent research has identified SIRT1 as a molecular target capable of reversing or attenuating several hallmarks of aging, particularly within the central nervous system (CNS). This narrative review critically evaluates the emerging evidence surrounding the geroprotective effects of SIRT1 activators, which exert dual actions, senomorphic and senolytic, via modulation of signaling pathways, thereby reducing neuronal senescence, enhancing autophagy, and mitigating inflammatory responses. The discussion also addresses the region-specific role of SIRT1 across the brain, particularly in the hippocampus and hypothalamus, which are essential for memory, energy homeostasis, and resilience to stress. Additionally, this review explores how SIRT1 depletion during aging contributes to the development of synaptic dysfunction, impaired cognitive function, and susceptibility to neurodegenerative diseases such as Alzheimer’s disease (AD) and Parkinson’s disease (PD). The therapeutic potential of SIRT1 activators is supported by preclinical and early clinical studies, suggesting their value in preventing or delaying brain aging. Thus, SIRT1 could be a promising pharmacological target for age-associated brain disorders, warranting more robust translational studies to validate these findings in humans.

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Concepts Keywords
Alzheimer Aging
Homeostasis Animals
Neurodegeneration Autophagy
Pharmacological Brain
Resilience Brain aging
Cellular Senescence
Enzyme Activators
Enzyme Activators
Geroprotectors
Humans
Neurodegenerative Diseases
Neuroinflammation
Neuroprotective Agents
Neuroprotective Agents
Oxidative Stress
Oxidative stress
Senotherapeutics
Senotherapeutics
Signal Transduction
SIRT1
SIRT1 protein, human
Sirtuin 1
Sirtuin 1

Semantics

Type Source Name
disease MESH cognitive impairment
disease MESH chronic diseases
disease MESH genomic instability
disease MESH inflammation
drug DRUGBANK Nadide
pathway REACTOME Mitochondrial biogenesis
pathway REACTOME Autophagy
disease MESH neurodegenerative diseases
pathway REACTOME Neurodegenerative Diseases
disease MESH Alzheimer’s disease
disease MESH Parkinson’s disease
disease MESH brain disorders
drug DRUGBANK Coenzyme M
disease MESH Arts
disease MESH Neuroinflammation
drug DRUGBANK Carboxyamidotriazole
disease MESH injury
disease MESH dys
pathway REACTOME Cellular Senescence
disease MESH pus
drug DRUGBANK L-Lysine
disease MESH death
disease MESH fac
pathway KEGG Peroxisome
pathway REACTOME Macroautophagy
pathway KEGG Lysosome
pathway REACTOME Apoptosis
pathway KEGG Oxidative phosphorylation
disease MESH dis
drug DRUGBANK Oxygen
disease MESH carcinogenesis
drug DRUGBANK Nitrogen
drug DRUGBANK Isoxaflutole
pathway REACTOME Mismatch Repair
pathway REACTOME Base Excision Repair
disease MESH frailty
pathway REACTOME DNA methylation
disease MESH mitochondrial dysfunction
drug DRUGBANK Nitric Oxide
disease MESH muscle weakness
drug DRUGBANK Dimercaprol
pathway REACTOME Release
disease MESH mul
disease MESH B cell lymphoma
disease MESH shock
drug DRUGBANK Quercetin
drug DRUGBANK Fisetin
disease MESH RB1
pathway REACTOME Death Receptor Signaling
disease MESH premature aging
drug DRUGBANK Ademetionine
drug DRUGBANK Probucol
drug DRUGBANK Dasatinib
drug DRUGBANK L-Tyrosine
drug DRUGBANK Glutamic Acid
disease MESH insulin resistance
pathway KEGG Insulin resistance
drug DRUGBANK (S)-Des-Me-Ampa
drug DRUGBANK L-Cysteine
pathway REACTOME S Phase
drug DRUGBANK L-Phenylalanine
disease MESH dementia
disease MESH char
disease MESH memory loss
disease MESH heart failure
drug DRUGBANK Serine
pathway REACTOME Metabolism
pathway KEGG Circadian rhythm
drug DRUGBANK Spermidine
disease MESH traumatic brain injury
disease MESH brain injury
drug DRUGBANK Thioredoxin
drug DRUGBANK Mecasermin
drug DRUGBANK Sirolimus
drug DRUGBANK Leptin
disease MESH atrophy
disease MESH Rett syndrome
drug DRUGBANK Trestolone
disease MESH tauopathies
pathway REACTOME Glucose metabolism
disease MESH ischemic stroke
disease MESH cerebrovascular stroke
drug DRUGBANK Resveratrol
pathway KEGG mTOR signaling pathway
disease MESH fed
drug DRUGBANK Metformin
disease MESH T2D
disease MESH hyperinsulinemia
drug DRUGBANK Indoleacetic acid
disease MESH subarachnoid hemorrhage
drug DRUGBANK Cholesterol
disease MESH dyslipidemia
drug DRUGBANK Coenzyme A
drug DRUGBANK Ciclosporin
drug DRUGBANK Atorvastatin
disease MESH obesity
drug DRUGBANK Simvastatin
disease MESH hypoxia
disease MESH ischemia
drug DRUGBANK Methionine
pathway REACTOME Adipogenesis
disease MESH body weight
pathway REACTOME Translation
disease MESH ics
drug DRUGBANK Rasagiline
disease MESH neurological disorders
disease MESH tic
drug DRUGBANK Cysteamine
pathway KEGG Alzheimer disease
disease MESH Papa
disease MESH diabetes mellitus
disease MESH Metabolic Syndrome
drug DRUGBANK Amino acids
pathway REACTOME Reproduction
disease MESH included
drug DRUGBANK Glyburide
disease MESH Visceral Obesity
disease MESH multiple sclerosis
drug DRUGBANK Gold
drug DRUGBANK NADH
disease MESH Gan
disease MESH white matter disease
disease MESH Diabetic Retinopathy
disease MESH Cancer
drug DRUGBANK Deoxy-2-Fluoro-B-D-Cellotrioside
drug DRUGBANK Angiotensin II
disease MESH ars
drug DRUGBANK Troleandomycin
disease MESH Postoperative Cognitive Dysfunction
disease MESH Ladd
disease MESH sepsis
drug DRUGBANK Tretamine
pathway REACTOME Signal Transduction

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