Journal
NATURE COMMUNICATIONS
Volume 13, Issue 1, Pages -Publisher
NATURE PORTFOLIO
DOI: 10.1038/s41467-022-32972-z
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Funding
- Washington University Diabetes Research Center [NIH DK20579]
- NIH K08 Career Development Award [NIH DK126847]
- NIH R01 [DK103740]
- Chan Zuckerberg Initiative seed network grant [CZF2019-002430]
- International Research Fund for Subsidy of Kyushu University School of Medicine Alumni
- Japan Society for the Promotion of Science (JSPS) Postdoctoral Fellowships for Research Abroad
- Osamu Hayaishi Memorial Scholarship
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This study demonstrates that diabetic kidney disease leads to reduced accessibility of glucocorticoid receptor binding sites and injury-associated expression signature in the proximal tubule. The researchers propose that chromatin accessibility is regulated by genetic background and closely intertwined with metabolic memory.
The proximal tubule is a key regulator of kidney function and glucose metabolism. Diabetic kidney disease leads to proximal tubule injury and changes in chromatin accessibility that modify the activity of transcription factors involved in glucose metabolism and inflammation. Here we use single nucleus RNA and ATAC sequencing to show that diabetic kidney disease leads to reduced accessibility of glucocorticoid receptor binding sites and an injury-associated expression signature in the proximal tubule. We hypothesize that chromatin accessibility is regulated by genetic background and closely-intertwined with metabolic memory, which pre-programs the proximal tubule to respond differently to external stimuli. Glucocorticoid excess has long been known to increase risk for type 2 diabetes, which raises the possibility that glucocorticoid receptor inhibition may mitigate the adverse metabolic effects of diabetic kidney disease.
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