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MicroRNA-26a targets ten eleven translocation enzymes and is regulated during pancreatic cell differentiation.


ABSTRACT: Ten eleven translocation (TET) enzymes (TET1/TET2/TET3) and thymine DNA glycosylase (TDG) play crucial roles in early embryonic and germ cell development by mediating DNA demethylation. However, the molecular mechanisms that regulate TETs/TDG expression and their role in cellular differentiation, including that of the pancreas, are not known. Here, we report that (i) TET1/2/3 and TDG can be direct targets of the microRNA miR-26a, (ii) murine TETs, especially TET2 and TDG, are down-regulated in islets during postnatal differentiation, whereas miR-26a is up-regulated, (iii) changes in 5-hydroxymethylcytosine accompany changes in TET mRNA levels, (iv) these changes in mRNA and 5-hydroxymethylcytosine are also seen in an in vitro differentiation system initiated with FACS-sorted adult ductal progenitor-like cells, and (v) overexpression of miR-26a in mice increases postnatal islet cell number in vivo and endocrine/acinar colonies in vitro. These results establish a previously unknown link between miRNAs and TET expression levels, and suggest a potential role for miR-26a and TET family proteins in pancreatic cell differentiation.

SUBMITTER: Fu X 

PROVIDER: S-EPMC3816405 | biostudies-other | 2013 Oct

REPOSITORIES: biostudies-other

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MicroRNA-26a targets ten eleven translocation enzymes and is regulated during pancreatic cell differentiation.

Fu Xianghui X   Jin Liang L   Wang Xichun X   Luo Angela A   Hu Junkai J   Zheng Xianwu X   Tsark Walter M WM   Riggs Arthur D AD   Ku Hsun Teresa HT   Huang Wendong W  

Proceedings of the National Academy of Sciences of the United States of America 20131010 44


Ten eleven translocation (TET) enzymes (TET1/TET2/TET3) and thymine DNA glycosylase (TDG) play crucial roles in early embryonic and germ cell development by mediating DNA demethylation. However, the molecular mechanisms that regulate TETs/TDG expression and their role in cellular differentiation, including that of the pancreas, are not known. Here, we report that (i) TET1/2/3 and TDG can be direct targets of the microRNA miR-26a, (ii) murine TETs, especially TET2 and TDG, are down-regulated in i  ...[more]

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