Senotherapeutics for metabolic disease and diabetic complications
Allyson K. Palmer, Rosa Spinelli, Larissa G. Langhi Prata, Selim Chaib, Masayoshi Suda, Tamar Tchkonia, Ulf Smith, James L. Kirkland

TL;DR
This paper explores how targeting cellular senescence could help treat metabolic diseases like diabetes and obesity.
Contribution
The paper highlights the emerging role of senotherapeutics in addressing metabolic diseases and their complications.
Findings
Senescent cells contribute to metabolic dysfunction through the SASP.
Senotherapeutics show promise in preclinical studies for treating metabolic diseases.
Existing antidiabetic drugs may modulate senescence, offering a new therapeutic approach.
Abstract
Metabolic diseases, including obesity, Type 2 diabetes (T2D), and metabolic syndrome, are increasingly prevalent worldwide, driven by sedentary lifestyles, aging populations, and complex genetic and environmental factors. Traditionally understood as disorders of glucose and lipid metabolism, a growing body of evidence now implicates cellular senescence as a central, age-related contributor to metabolic dysfunction. Senescent cells (SCs) accumulate in key metabolic tissues where they disrupt tissue function through the senescence-associated secretory phenotype (SASP), a pro-inflammatory and fibrogenic secretome. SASP factors exacerbate insulin resistance, chronic inflammation, and tissue remodeling, advancing the progression and complications of metabolic diseases. These insights have catalyzed the development of senotherapeutics, a class of interventions that includes senolytics (to…
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Taxonomy
TopicsTelomeres, Telomerase, and Senescence · Skin Protection and Aging · Epigenetics and DNA Methylation
