Human In Vitro Models for Assessing the Genomic Basis of Chemotherapy-Induced Cardiovascular Toxicity.
Emily A PinheiroTarek MagdyMaged M CostantinePublished in: Journal of cardiovascular translational research (2020)
Chemotherapy-induced cardiovascular toxicity (CICT) is a well-established risk for cancer survivors and causes diseases such as heart failure, arrhythmia, vascular dysfunction, and atherosclerosis. As our knowledge of the precise cardiovascular risks of each chemotherapy agent has improved, it has become clear that genomics is one of the most influential predictors of which patients will experience cardiovascular toxicity. Most recently, GWAS-led, top-down approaches have identified novel genetic variants and their related genes that are statistically related to CICT. Importantly, the advent of human-induced pluripotent stem cell (hiPSC) models provides a system to experimentally test the effect of these genomic findings in vitro, query the underlying mechanisms, and develop novel strategies to mitigate the cardiovascular toxicity liabilities due to these mechanisms. Here we review the cardiovascular toxicities of chemotherapy drugs, discuss how these can be modeled in vitro, and suggest how these models can be used to validate genetic variants that predispose patients to these effects.
Keyphrases
- chemotherapy induced
- end stage renal disease
- heart failure
- stem cells
- oxidative stress
- chronic kidney disease
- ejection fraction
- endothelial cells
- prognostic factors
- peritoneal dialysis
- young adults
- bone marrow
- cardiovascular disease
- atrial fibrillation
- left ventricular
- risk assessment
- locally advanced
- high glucose
- radiation therapy
- dna methylation
- patient reported outcomes
- genome wide
- single cell
- cell therapy
- cardiac resynchronization therapy