A hPSC-based platform to discover gene-environment interactions that impact human β-cell and dopamine neuron survival.
Ting ZhouTae Wan KimChi Nok ChongLei TanSadaf AminZohreh Sadat BadieyanSuranjit MukherjeeZaniar GhazizadehHui ZengMin GuoMiguel CrespoTuo ZhangReyn KenyonChristopher L RobinsonEffie ApostolouHui WangJenny Zhaoying XiangTodd EvansLorenz StuderShuibing ChenPublished in: Nature communications (2018)
Common disorders, including diabetes and Parkinson's disease, are caused by a combination of environmental factors and genetic susceptibility. However, defining the mechanisms underlying gene-environment interactions has been challenging due to the lack of a suitable experimental platform. Using pancreatic β-like cells derived from human pluripotent stem cells (hPSCs), we discovered that a commonly used pesticide, propargite, induces pancreatic β-cell death, a pathological hallmark of diabetes. Screening a panel of diverse hPSC-derived cell types we extended this observation to a similar susceptibility in midbrain dopamine neurons, a cell type affected in Parkinson's disease. We assessed gene-environment interactions using isogenic hPSC lines for genetic variants associated with diabetes and Parkinson's disease. We found GSTT1-/- pancreatic β-like cells and dopamine neurons were both hypersensitive to propargite-induced cell death. Our study identifies an environmental chemical that contributes to human β-cell and dopamine neuron loss and validates a novel hPSC-based platform for determining gene-environment interactions.
Keyphrases
- pluripotent stem cells
- genome wide
- cell death
- endothelial cells
- copy number
- type diabetes
- cardiovascular disease
- single cell
- uric acid
- induced pluripotent stem cells
- high throughput
- genome wide identification
- cell therapy
- spinal cord
- glycemic control
- high glucose
- dna methylation
- gene expression
- stem cells
- adipose tissue
- skeletal muscle
- cell proliferation
- mesenchymal stem cells