Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defects

Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defects

Abstract Background Neural tube defects (NTDs) are severe, common birth defects that result from failure of normal neural tube closure during early embryogenesis. Accumulating strong evidence indicates that genetic factors contribute to NTDs etiology, among them, HOX genes play a key role in neural...

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Main Authors: Juan Yu, Lei Wang, Pei Pei, Xue Li, Jianxin Wu, Zhiyong Qiu, Juan Zhang, Ruifang Ao, Shan Wang, Ting Zhang, Jun Xie
Format: Article
Language:English
Published: BMC 2019-12-01
Series:Epigenetics & Chromatin
Subjects:
Neural tube defects
Retinoic acid
Hox genes
H3K27me3
UTX
SUZ12
Online Access:https://doi.org/10.1186/s13072-019-0318-1
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spelling doaj-daece1d35d4d41dcbdc2d46eed7bbec02020-12-20T12:17:40ZengBMCEpigenetics & Chromatin1756-89352019-12-0112111910.1186/s13072-019-0318-1Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defectsJuan Yu0Lei Wang1Pei Pei2Xue Li3Jianxin Wu4Zhiyong Qiu5Juan Zhang6Ruifang Ao7Shan Wang8Ting Zhang9Jun Xie10Department of Biochemistry and Molecular Biology, Shanxi Medical UniversityBeijing Municipal Key Laboratory of Child Development and Nutriomics, Capital Institute of PediatricsBeijing Municipal Key Laboratory of Child Development and Nutriomics, Capital Institute of PediatricsSchool of Clinical Medical, Weifang Medical UniversityDepartment of Biochemistry, Capital Institute of PediatricsBeijing Municipal Key Laboratory of Child Development and Nutriomics, Capital Institute of PediatricsDepartment of Biochemistry and Molecular Biology, Shanxi Medical UniversityDepartment of Biochemistry and Molecular Biology, Shanxi Medical UniversityBeijing Municipal Key Laboratory of Child Development and Nutriomics, Capital Institute of PediatricsBeijing Municipal Key Laboratory of Child Development and Nutriomics, Capital Institute of PediatricsDepartment of Biochemistry and Molecular Biology, Shanxi Medical UniversityAbstract Background Neural tube defects (NTDs) are severe, common birth defects that result from failure of normal neural tube closure during early embryogenesis. Accumulating strong evidence indicates that genetic factors contribute to NTDs etiology, among them, HOX genes play a key role in neural tube closure. Although abnormal HOX gene expression can lead to NTDs, the underlying pathological mechanisms have not fully been understood. Method We detected that H3K27me3 and expression of the Hox genes in a retinoic acid (RA) induced mouse NTDs model on E8.5, E9.5 and E10.5 using RNA-sequencing and chromatin immunoprecipitation sequencing assays. Furthermore, we quantified 10 Hox genes using NanoString nCounter in brain tissue of fetuses with 39 NTDs patients including anencephaly, spina bifida, hydrocephaly and encephalocele. Results Here, our results showed differential expression in 26 genes with a > 20-fold change in the level of expression, including 10 upregulated Hox genes. RT-qPCR revealed that these 10 Hox genes were all upregulated in RA-induced mouse NTDs as well as RA-treated embryonic stem cells (ESCs). Using ChIP-seq assays, we demonstrate that a decrease in H3K27me3 level upregulates the expression of Hox cluster A–D in RA-induced mouse NTDs model on E10.5. Interestingly, RA treatment led to attenuation of H3K27me3 due to cooperate between UTX and Suz12, affecting Hox gene regulation. Further analysis, in human anencephaly cases, upregulation of 10 HOX genes was observed, along with aberrant levels of H3K27me3. Notably, HOXB4, HOXC4 and HOXD1 expression was negatively correlated with H3K27me3 levels. Conclusion Our results indicate that abnormal HOX gene expression induced by aberrant H3K27me3 levels may be a risk factor for NTDs and highlight the need for further analysis of genome-wide epigenetic modification in NTDs.https://doi.org/10.1186/s13072-019-0318-1Neural tube defectsRetinoic acidHox genesH3K27me3UTXSUZ12
collection DOAJ
language English
format Article
sources DOAJ
author Juan Yu
Lei Wang
Pei Pei
Xue Li
Jianxin Wu
Zhiyong Qiu
Juan Zhang
Ruifang Ao
Shan Wang
Ting Zhang
Jun Xie
spellingShingle Juan Yu
Lei Wang
Pei Pei
Xue Li
Jianxin Wu
Zhiyong Qiu
Juan Zhang
Ruifang Ao
Shan Wang
Ting Zhang
Jun Xie
Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defects
Epigenetics & Chromatin
Neural tube defects
Retinoic acid
Hox genes
H3K27me3
UTX
SUZ12
author_facet Juan Yu
Lei Wang
Pei Pei
Xue Li
Jianxin Wu
Zhiyong Qiu
Juan Zhang
Ruifang Ao
Shan Wang
Ting Zhang
Jun Xie
author_sort Juan Yu
title Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defects
title_short Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defects
title_full Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defects
title_fullStr Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defects
title_full_unstemmed Reduced H3K27me3 leads to abnormal Hox gene expression in neural tube defects
title_sort reduced h3k27me3 leads to abnormal hox gene expression in neural tube defects
publisher BMC
series Epigenetics & Chromatin
issn 1756-8935
publishDate 2019-12-01
description Abstract Background Neural tube defects (NTDs) are severe, common birth defects that result from failure of normal neural tube closure during early embryogenesis. Accumulating strong evidence indicates that genetic factors contribute to NTDs etiology, among them, HOX genes play a key role in neural tube closure. Although abnormal HOX gene expression can lead to NTDs, the underlying pathological mechanisms have not fully been understood. Method We detected that H3K27me3 and expression of the Hox genes in a retinoic acid (RA) induced mouse NTDs model on E8.5, E9.5 and E10.5 using RNA-sequencing and chromatin immunoprecipitation sequencing assays. Furthermore, we quantified 10 Hox genes using NanoString nCounter in brain tissue of fetuses with 39 NTDs patients including anencephaly, spina bifida, hydrocephaly and encephalocele. Results Here, our results showed differential expression in 26 genes with a > 20-fold change in the level of expression, including 10 upregulated Hox genes. RT-qPCR revealed that these 10 Hox genes were all upregulated in RA-induced mouse NTDs as well as RA-treated embryonic stem cells (ESCs). Using ChIP-seq assays, we demonstrate that a decrease in H3K27me3 level upregulates the expression of Hox cluster A–D in RA-induced mouse NTDs model on E10.5. Interestingly, RA treatment led to attenuation of H3K27me3 due to cooperate between UTX and Suz12, affecting Hox gene regulation. Further analysis, in human anencephaly cases, upregulation of 10 HOX genes was observed, along with aberrant levels of H3K27me3. Notably, HOXB4, HOXC4 and HOXD1 expression was negatively correlated with H3K27me3 levels. Conclusion Our results indicate that abnormal HOX gene expression induced by aberrant H3K27me3 levels may be a risk factor for NTDs and highlight the need for further analysis of genome-wide epigenetic modification in NTDs.
topic Neural tube defects
Retinoic acid
Hox genes
H3K27me3
UTX
SUZ12
url https://doi.org/10.1186/s13072-019-0318-1
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