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Sequential regulatory loops as key gatekeepers for neuronal reprogramming in human cells.


ABSTRACT: Direct conversion of somatic cells into neurons holds great promise for regenerative medicine. However, neuronal conversion is relatively inefficient in human cells compared to mouse cells. It has been unclear what might be the key barriers to reprogramming in human cells. We recently elucidated an RNA program mediated by the polypyrimidine tract binding protein PTB to convert mouse embryonic fibroblasts (MEFs) into functional neurons. In human adult fibroblasts (HAFs), however, we unexpectedly found that invoking the documented PTB-REST-miR-124 loop generates only immature neurons. We now report that the functionality requires sequential inactivation of PTB and the PTB paralog nPTB in HAFs. Inactivation of nPTB triggers another self-enforcing loop essential for neuronal maturation, which comprises nPTB, the transcription factor BRN2, and miR-9. These findings suggest that two separate gatekeepers control neuronal conversion and maturation and consecutively overcoming these gatekeepers enables deterministic reprogramming of HAFs into functional neurons.

SUBMITTER: Xue Y 

PROVIDER: S-EPMC4882254 | biostudies-literature | 2016 Jun

REPOSITORIES: biostudies-literature

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Sequential regulatory loops as key gatekeepers for neuronal reprogramming in human cells.

Xue Yuanchao Y   Qian Hao H   Hu Jing J   Zhou Bing B   Zhou Yu Y   Hu Xihao X   Karakhanyan Aziz A   Pang Zhiping Z   Fu Xiang-Dong XD  

Nature neuroscience 20160425 6


Direct conversion of somatic cells into neurons holds great promise for regenerative medicine. However, neuronal conversion is relatively inefficient in human cells compared to mouse cells. It has been unclear what might be the key barriers to reprogramming in human cells. We recently elucidated an RNA program mediated by the polypyrimidine tract binding protein PTB to convert mouse embryonic fibroblasts (MEFs) into functional neurons. In human adult fibroblasts (HAFs), however, we unexpectedly  ...[more]

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