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Targeted demethylation at the CDKN1C/p57 locus induces human β cell replication.

Citation
Ou, K., et al. “Targeted Demethylation At The Cdkn1C/P57 Locus Induces Human Β Cell Replication.”. The Journal Of Clinical Investigation, pp. 209-214.
Center University of Pennsylvania
Author Kristy Ou, Ming Yu, Nicholas G Moss, Yue J Wang, Amber W Wang, Son C Nguyen, Connie Jiang, Eseye Feleke, Vasumathi Kameswaran, Eric F Joyce, Ali Naji, Benjamin Glaser, Dana Avrahami, Klaus H Kaestner
Keywords beta cells, diabetes, Endocrinology, Epigenetics
Abstract

The loss of insulin-secreting β cells is characteristic among type I and type II diabetes. Stimulating proliferation to expand sources of β cells for transplantation remains a challenge because adult β cells do not proliferate readily. The cell cycle inhibitor p57 has been shown to control cell division in human β cells. Expression of p57 is regulated by the DNA methylation status of the imprinting control region 2 (ICR2), which is commonly hypomethylated in Beckwith-Wiedemann syndrome patients who exhibit massive β cell proliferation. We hypothesized that targeted demethylation of the ICR2 using a transcription activator-like effector protein fused to the catalytic domain of TET1 (ICR2-TET1) would repress p57 expression and promote cell proliferation. We report here that overexpression of ICR2-TET1 in human fibroblasts reduces p57 expression levels and increases proliferation. Furthermore, human islets overexpressing ICR2-TET1 exhibit repression of p57 with concomitant upregulation of Ki-67 while maintaining glucose-sensing functionality. When transplanted into diabetic, immunodeficient mice, the epigenetically edited islets show increased β cell replication compared with control islets. These findings demonstrate that epigenetic editing is a promising tool for inducing β cell proliferation, which may one day alleviate the scarcity of transplantable β cells for the treatment of diabetes.

Year of Publication
2019
Journal
The Journal of clinical investigation
Volume
129
Issue
1
Number of Pages
209-214
Date Published
12/2019
ISSN Number
1558-8238
DOI
10.1172/JCI99170
Alternate Journal
J. Clin. Invest.
PMID
30352048
PMCID
PMC6307972
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