Obesity triggers tumoral senescence and renders poorly immunogenic malignancies amenable to senolysis.
Frédérik FournierRoberto Diaz-MarinFrédérique PilonMathieu NeaultRachel JuneauGabrielle GirouardAriel M WilsonBruno LarrivéeFrédérick A MalletteSergio Crespo-GarciaPrzemyslaw SapiehaPublished in: Proceedings of the National Academy of Sciences of the United States of America (2022)
Obesity is a major risk factor for cancer. Conventional thought suggests that elevated adiposity predisposes to heightened inflammatory stress and potentiates tumor growth, yet underlying mechanisms remain ill-defined. Here, we show that tumors from patients with a body mass index >35 carry a high burden of senescent cells. In mouse syngeneic tumor models, we correlated a pronounced accretion of senescent cancer cells with poorly immunogenic tumors when mice were subjected to diet-induced obesity (DIO). Highly immunogenic tumors showed lesser senescence burden suggesting immune-mediated elimination of senescent cancer cells, likely targeted as a consequence of their senescence-associated secretory phenotype. Treatment with the senolytic BH3 mimetic small molecule inhibitor ABT-263 selectively stalled tumor growth in mice with DIO to rates comparable to regular diet-fed mice. Thus, consideration of body adiposity in the selection of cancer therapy may be a critical determinant for disease outcome in poorly immunogenic malignancies.
Keyphrases
- high fat diet induced
- insulin resistance
- weight gain
- cancer therapy
- weight loss
- body mass index
- small molecule
- metabolic syndrome
- dna damage
- adipose tissue
- type diabetes
- endothelial cells
- skeletal muscle
- stress induced
- physical activity
- induced apoptosis
- drug delivery
- oxidative stress
- papillary thyroid
- signaling pathway
- replacement therapy
- childhood cancer