Innate immune signaling drives late cardiac toxicity following DNA-damaging cancer therapies.
Achraf ShamseddineSuchit H PatelValery ChavezZachary R MooreMutayyaba AdnanMelody DiBonaJun LiChau T DangLakshmi V RamanathanKevin C OeffingerJennifer E LiuRichard M SteingartAlessandra PiersigilliNicholas D SocciAngel T ChanAnthony F YuSamuel F BakhoumAdam M SchmittPublished in: The Journal of experimental medicine (2022)
Late cardiac toxicity is a potentially lethal complication of cancer therapy, yet the pathogenic mechanism remains largely unknown, and few treatment options exist. Here we report DNA-damaging agents such as radiation and anthracycline chemotherapies inducing delayed cardiac inflammation following therapy due to activation of cGAS- and STING-dependent type I interferon signaling. Genetic ablation of cGAS-STING signaling in mice inhibits DNA damage-induced cardiac inflammation, rescues late cardiac functional decline, and prevents death from cardiac events. Treatment with a STING antagonist suppresses cardiac interferon signaling following DNA-damaging therapies and effectively mitigates cardiac toxicity. These results identify a therapeutically targetable, pathogenic mechanism for one of the most vexing treatment-related toxicities in cancer survivors.
Keyphrases
- left ventricular
- oxidative stress
- dna damage
- cancer therapy
- circulating tumor
- type diabetes
- heart failure
- stem cells
- gene expression
- mouse model
- drug delivery
- radiation therapy
- genome wide
- adipose tissue
- bone marrow
- radiation induced
- nucleic acid
- insulin resistance
- smoking cessation
- high fat diet induced
- papillary thyroid
- cell therapy
- replacement therapy
- radiofrequency ablation
- stress induced