OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formation

OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formation

Abstract Background Oligodendrocytes, responsible for axon ensheathment, are critical for central nervous system (CNS) development, function, and diseases. OLIG2 is an important transcription factor (TF) that acts during oligodendrocyte development and performs distinct functions at different stages...

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Main Authors: Haichao Wei, Xiaomin Dong, Yanan You, Bo Hai, Raquel Cuevas-Diaz Duran, Xizi Wu, Natasha Kharas, Jia Qian Wu
Format: Article
Language:English
Published: BMC 2021-06-01
Series:BMC Biology
Subjects:
Oligodendrocyte development
OLIG2
LncRNAs
Histone modification
Transcriptional regulation
Regulation after transcription
Online Access:https://doi.org/10.1186/s12915-021-01057-6
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spelling doaj-714642cc7ba24c9489f7eb314b7d4d232021-06-27T11:29:04ZengBMCBMC Biology1741-70072021-06-0119112110.1186/s12915-021-01057-6OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formationHaichao Wei0Xiaomin Dong1Yanan You2Bo Hai3Raquel Cuevas-Diaz Duran4Xizi Wu5Natasha Kharas6Jia Qian Wu7The Vivian L. Smith Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at HoustonThe Vivian L. Smith Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at HoustonThe Vivian L. Smith Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at HoustonThe Vivian L. Smith Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at HoustonThe Vivian L. Smith Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at HoustonThe Vivian L. Smith Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at HoustonDepartment of Neurobiology and Anatomy, The University of Texas Medical School at HoustonThe Vivian L. Smith Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at HoustonAbstract Background Oligodendrocytes, responsible for axon ensheathment, are critical for central nervous system (CNS) development, function, and diseases. OLIG2 is an important transcription factor (TF) that acts during oligodendrocyte development and performs distinct functions at different stages. Previous studies have shown that lncRNAs (long non-coding RNAs; > 200 bp) have important functions during oligodendrocyte development, but their roles have not been systematically characterized and their regulation is not yet clear. Results We performed an integrated study of genome-wide OLIG2 binding and the epigenetic modification status of both coding and non-coding genes during three stages of oligodendrocyte differentiation in vivo: neural stem cells (NSCs), oligodendrocyte progenitor cells (OPCs), and newly formed oligodendrocytes (NFOs). We found that 613 lncRNAs have OLIG2 binding sites and are expressed in at least one cell type, which can potentially be activated or repressed by OLIG2. Forty-eight of them have increased expression in oligodendrocyte lineage cells. Predicting lncRNA functions by using a “guilt-by-association” approach revealed that the functions of these 48 lncRNAs were enriched in “oligodendrocyte development and differentiation.” Additionally, bivalent genes are known to play essential roles during embryonic stem cell differentiation. We identified bivalent genes in NSCs, OPCs, and NFOs and found that some bivalent genes bound by OLIG2 are dynamically regulated during oligodendrocyte development. Importantly, we unveiled a previously unknown mechanism that, in addition to transcriptional regulation via DNA binding, OLIG2 could self-regulate through the 3′ UTR of its own mRNA. Conclusions Our studies have revealed the missing links in the mechanisms regulating oligodendrocyte development at the transcriptional level and after transcription. The results of our research have improved the understanding of fundamental cell fate decisions during oligodendrocyte lineage formation, which can enable insights into demyelination diseases and regenerative medicine.https://doi.org/10.1186/s12915-021-01057-6Oligodendrocyte developmentOLIG2LncRNAsHistone modificationTranscriptional regulationRegulation after transcription
collection DOAJ
language English
format Article
sources DOAJ
author Haichao Wei
Xiaomin Dong
Yanan You
Bo Hai
Raquel Cuevas-Diaz Duran
Xizi Wu
Natasha Kharas
Jia Qian Wu
spellingShingle Haichao Wei
Xiaomin Dong
Yanan You
Bo Hai
Raquel Cuevas-Diaz Duran
Xizi Wu
Natasha Kharas
Jia Qian Wu
OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formation
BMC Biology
Oligodendrocyte development
OLIG2
LncRNAs
Histone modification
Transcriptional regulation
Regulation after transcription
author_facet Haichao Wei
Xiaomin Dong
Yanan You
Bo Hai
Raquel Cuevas-Diaz Duran
Xizi Wu
Natasha Kharas
Jia Qian Wu
author_sort Haichao Wei
title OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formation
title_short OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formation
title_full OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formation
title_fullStr OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formation
title_full_unstemmed OLIG2 regulates lncRNAs and its own expression during oligodendrocyte lineage formation
title_sort olig2 regulates lncrnas and its own expression during oligodendrocyte lineage formation
publisher BMC
series BMC Biology
issn 1741-7007
publishDate 2021-06-01
description Abstract Background Oligodendrocytes, responsible for axon ensheathment, are critical for central nervous system (CNS) development, function, and diseases. OLIG2 is an important transcription factor (TF) that acts during oligodendrocyte development and performs distinct functions at different stages. Previous studies have shown that lncRNAs (long non-coding RNAs; > 200 bp) have important functions during oligodendrocyte development, but their roles have not been systematically characterized and their regulation is not yet clear. Results We performed an integrated study of genome-wide OLIG2 binding and the epigenetic modification status of both coding and non-coding genes during three stages of oligodendrocyte differentiation in vivo: neural stem cells (NSCs), oligodendrocyte progenitor cells (OPCs), and newly formed oligodendrocytes (NFOs). We found that 613 lncRNAs have OLIG2 binding sites and are expressed in at least one cell type, which can potentially be activated or repressed by OLIG2. Forty-eight of them have increased expression in oligodendrocyte lineage cells. Predicting lncRNA functions by using a “guilt-by-association” approach revealed that the functions of these 48 lncRNAs were enriched in “oligodendrocyte development and differentiation.” Additionally, bivalent genes are known to play essential roles during embryonic stem cell differentiation. We identified bivalent genes in NSCs, OPCs, and NFOs and found that some bivalent genes bound by OLIG2 are dynamically regulated during oligodendrocyte development. Importantly, we unveiled a previously unknown mechanism that, in addition to transcriptional regulation via DNA binding, OLIG2 could self-regulate through the 3′ UTR of its own mRNA. Conclusions Our studies have revealed the missing links in the mechanisms regulating oligodendrocyte development at the transcriptional level and after transcription. The results of our research have improved the understanding of fundamental cell fate decisions during oligodendrocyte lineage formation, which can enable insights into demyelination diseases and regenerative medicine.
topic Oligodendrocyte development
OLIG2
LncRNAs
Histone modification
Transcriptional regulation
Regulation after transcription
url https://doi.org/10.1186/s12915-021-01057-6
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AT xiaomindong olig2regulateslncrnasanditsownexpressionduringoligodendrocytelineageformation
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