Author
Listed:
- Ting Zhou
(Weill Cornell Medical College)
- Tae Wan Kim
(Sloan-Kettering Institute for Cancer Research
Sloan-Kettering Institute for Cancer Research)
- Chi Nok Chong
(Weill Cornell Medical College)
- Lei Tan
(Weill Cornell Medical College
Shanghai Jiao Tong University, School of Medicine)
- Sadaf Amin
(Weill Cornell Medical College)
- Zohreh Sadat Badieyan
(Weill Cornell Medical College)
- Suranjit Mukherjee
(Weill Cornell Medical College)
- Zaniar Ghazizadeh
(Weill Cornell Medical College)
- Hui Zeng
(Weill Cornell Medical College)
- Min Guo
(Weill Cornell Medical College)
- Miguel Crespo
(Weill Cornell Medical College)
- Tuo Zhang
(Weill Cornell Medical College)
- Reyn Kenyon
(Weill Cornell Medical College)
- Christopher L. Robinson
(Weill Cornell Medical College)
- Effie Apostolou
(Weill Cornell Medical College)
- Hui Wang
(Shanghai Jiao Tong University, School of Medicine)
- Jenny Zhaoying Xiang
(Weill Cornell Medical College)
- Todd Evans
(Weill Cornell Medical College)
- Lorenz Studer
(Sloan-Kettering Institute for Cancer Research
Sloan-Kettering Institute for Cancer Research)
- Shuibing Chen
(Weill Cornell Medical College
Weill Cornell Medical College)
Abstract
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.
Suggested Citation
Ting Zhou & Tae Wan Kim & Chi Nok Chong & Lei Tan & Sadaf Amin & Zohreh Sadat Badieyan & Suranjit Mukherjee & Zaniar Ghazizadeh & Hui Zeng & Min Guo & Miguel Crespo & Tuo Zhang & Reyn Kenyon & Christo, 2018.
"A hPSC-based platform to discover gene-environment interactions that impact human β-cell and dopamine neuron survival,"
Nature Communications, Nature, vol. 9(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:9:y:2018:i:1:d:10.1038_s41467-018-07201-1
DOI: 10.1038/s41467-018-07201-1
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