FoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulation

FoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulation

Abstract Background FoxH1 is a forkhead transcription factor with conserved key functions in vertebrate mesoderm induction and left-right patterning downstream of the TGF-beta/Nodal signaling pathway. Binding of the forkhead domain (FHD) of FoxH1 to a highly conserved proximal sequence motif was sho...

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Main Authors: Patrick Fischer, Hao Chen, Frederic Pacho, Dietmar Rieder, Robin A. Kimmel, Dirk Meyer
Format: Article
Language:English
Published: BMC 2019-07-01
Series:BMC Biology
Subjects:
Gastrulation
Nodal signaling
FoxH1
miR-430
MZT
Chromatin folding
Online Access:http://link.springer.com/article/10.1186/s12915-019-0683-z
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spelling doaj-599d7b6a182c4f71844f0a1f133b17332020-11-25T03:24:24ZengBMCBMC Biology1741-70072019-07-0117111710.1186/s12915-019-0683-zFoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulationPatrick Fischer0Hao Chen1Frederic Pacho2Dietmar Rieder3Robin A. Kimmel4Dirk Meyer5Institute of Molecular Biology/CMBI, University of InnsbruckInstitute of Molecular Biology/CMBI, University of InnsbruckInstitute of Molecular Biology/CMBI, University of InnsbruckDivision of Bioinformatics, Biocenter, Innsbruck Medical UniversityInstitute of Molecular Biology/CMBI, University of InnsbruckInstitute of Molecular Biology/CMBI, University of InnsbruckAbstract Background FoxH1 is a forkhead transcription factor with conserved key functions in vertebrate mesoderm induction and left-right patterning downstream of the TGF-beta/Nodal signaling pathway. Binding of the forkhead domain (FHD) of FoxH1 to a highly conserved proximal sequence motif was shown to regulate target gene expression. Results We identify the conserved microRNA-430 family (miR-430) as a novel target of FoxH1. miR-430 levels are increased in foxH1 mutants, resulting in a reduced expression of transcripts that are targeted by miR-430 for degradation. To determine the underlying mechanism of miR-430 repression, we performed chromatin immunoprecipitation studies and overexpression experiments with mutant as well as constitutive active and repressive forms of FoxH1. Our studies reveal a molecular interaction of FoxH1 with miR-430 loci independent of the FHD. Furthermore, we show that previously described mutant forms of FoxH1 that disrupt DNA binding or that lack the C-terminal Smad Interaction Domain (SID) dominantly interfere with miR-430 repression, but not with the regulation of previously described FoxH1 targets. Conclusions We were able to identify the distinct roles of protein domains of FoxH1 in the regulation process of miR-430. We provide evidence that the indirect repression of miR-430 loci depends on the connection to a distal repressive chromosome environment via a non-canonical mode. The widespread distribution of such non-canonical binding sites of FoxH1, found not only in our study, argues against a function restricted to regulating miR-430 and for a more global role of FoxH1 in chromatin folding.http://link.springer.com/article/10.1186/s12915-019-0683-zGastrulationNodal signalingFoxH1miR-430MZTChromatin folding
collection DOAJ
language English
format Article
sources DOAJ
author Patrick Fischer
Hao Chen
Frederic Pacho
Dietmar Rieder
Robin A. Kimmel
Dirk Meyer
spellingShingle Patrick Fischer
Hao Chen
Frederic Pacho
Dietmar Rieder
Robin A. Kimmel
Dirk Meyer
FoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulation
BMC Biology
Gastrulation
Nodal signaling
FoxH1
miR-430
MZT
Chromatin folding
author_facet Patrick Fischer
Hao Chen
Frederic Pacho
Dietmar Rieder
Robin A. Kimmel
Dirk Meyer
author_sort Patrick Fischer
title FoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulation
title_short FoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulation
title_full FoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulation
title_fullStr FoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulation
title_full_unstemmed FoxH1 represses miR-430 during early embryonic development of zebrafish via non-canonical regulation
title_sort foxh1 represses mir-430 during early embryonic development of zebrafish via non-canonical regulation
publisher BMC
series BMC Biology
issn 1741-7007
publishDate 2019-07-01
description Abstract Background FoxH1 is a forkhead transcription factor with conserved key functions in vertebrate mesoderm induction and left-right patterning downstream of the TGF-beta/Nodal signaling pathway. Binding of the forkhead domain (FHD) of FoxH1 to a highly conserved proximal sequence motif was shown to regulate target gene expression. Results We identify the conserved microRNA-430 family (miR-430) as a novel target of FoxH1. miR-430 levels are increased in foxH1 mutants, resulting in a reduced expression of transcripts that are targeted by miR-430 for degradation. To determine the underlying mechanism of miR-430 repression, we performed chromatin immunoprecipitation studies and overexpression experiments with mutant as well as constitutive active and repressive forms of FoxH1. Our studies reveal a molecular interaction of FoxH1 with miR-430 loci independent of the FHD. Furthermore, we show that previously described mutant forms of FoxH1 that disrupt DNA binding or that lack the C-terminal Smad Interaction Domain (SID) dominantly interfere with miR-430 repression, but not with the regulation of previously described FoxH1 targets. Conclusions We were able to identify the distinct roles of protein domains of FoxH1 in the regulation process of miR-430. We provide evidence that the indirect repression of miR-430 loci depends on the connection to a distal repressive chromosome environment via a non-canonical mode. The widespread distribution of such non-canonical binding sites of FoxH1, found not only in our study, argues against a function restricted to regulating miR-430 and for a more global role of FoxH1 in chromatin folding.
topic Gastrulation
Nodal signaling
FoxH1
miR-430
MZT
Chromatin folding
url http://link.springer.com/article/10.1186/s12915-019-0683-z
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