Obesity increases genomic instability at DNA repeat-mediated endogenous mutation hotspots.
Pallavi KompellaGuliang WangRussell E DurrettYanhao LaiCeleste MarinYuan LiuSamy L HabibJohn DiGiovanniKaren M VasquezPublished in: Nature communications (2024)
Obesity is associated with increased cancer risk, yet the underlying mechanisms remain elusive. Obesity-associated cancers involve disruptions in metabolic and cellular pathways, which can lead to genomic instability. Repetitive DNA sequences capable of adopting alternative DNA structures (e.g., H-DNA) stimulate mutations and are enriched at mutation hotspots in human cancer genomes. However, it is not known if obesity impacts DNA repeat-mediated endogenous mutation hotspots. We address this gap by measuring mutation frequencies in obese and normal-weight transgenic reporter mice carrying either a control human B-DNA- or an H-DNA-forming sequence (from a translocation hotspot in c-MYC in Burkitt lymphoma). Here, we discover that H-DNA-induced DNA damage and mutations are elevated in a tissue-specific manner, and DNA repair efficiency is reduced in obese mice compared to those on the control diet. These findings elucidate the impact of obesity on cancer-associated endogenous mutation hotspots, providing mechanistic insight into the link between obesity and cancer.
Keyphrases
- weight loss
- circulating tumor
- high fat diet induced
- insulin resistance
- metabolic syndrome
- cell free
- single molecule
- type diabetes
- dna damage
- dna repair
- weight gain
- bariatric surgery
- endothelial cells
- nucleic acid
- adipose tissue
- body mass index
- oxidative stress
- skeletal muscle
- squamous cell carcinoma
- papillary thyroid
- gene expression
- diffuse large b cell lymphoma
- physical activity
- obese patients
- mass spectrometry
- crispr cas
- squamous cell
- high glucose
- genetic diversity