Single-Cell Integration Analysis of Heterotopic Ossification and Fibrocartilage Developmental Lineage: Endoplasmic Reticulum Stress Effector Xbp1 Transcriptionally Regulates the Notch Signaling Pathway to Mediate Fibrocartilage Differentiation

INTRODUCTION: Regeneration of fibrochondrocytes is essential for the healing of the tendon-bone interface (TBI), which is similar to the formation of neurogenic heterotopic ossification (HO). Through single-cell integrative analysis, this study explored the homogeneity of HO cells and fibrochondrocy...

Descripción completa

Detalles Bibliográficos
Autores principales: Chen, Yisheng, Sun, Yaying, Xu, Yuzhen, Lin, Wei-Wei, Luo, Zhiwen, Han, Zhihua, Liu, Shaohua, Qi, Beijie, Sun, Chenyu, Go, Ken, Kang, x.-R., Chen, Jiwu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8563124/
https://www.ncbi.nlm.nih.gov/pubmed/34737845
http://dx.doi.org/10.1155/2021/7663366
_version_ 1784593368289902592
author Chen, Yisheng
Sun, Yaying
Xu, Yuzhen
Lin, Wei-Wei
Luo, Zhiwen
Han, Zhihua
Liu, Shaohua
Qi, Beijie
Sun, Chenyu
Go, Ken
Kang, x.-R.
Chen, Jiwu
author_facet Chen, Yisheng
Sun, Yaying
Xu, Yuzhen
Lin, Wei-Wei
Luo, Zhiwen
Han, Zhihua
Liu, Shaohua
Qi, Beijie
Sun, Chenyu
Go, Ken
Kang, x.-R.
Chen, Jiwu
author_sort Chen, Yisheng
collection PubMed
description INTRODUCTION: Regeneration of fibrochondrocytes is essential for the healing of the tendon-bone interface (TBI), which is similar to the formation of neurogenic heterotopic ossification (HO). Through single-cell integrative analysis, this study explored the homogeneity of HO cells and fibrochondrocytes. METHODS: This study integrated six datasets, namely, GSE94683, GSE144306, GSE168153, GSE138515, GSE102929, and GSE110993. The differentiation trajectory and key transcription factors (TFs) for HO occurrence were systematically analyzed by integrating single-cell RNA (scRNA) sequencing, bulk RNA sequencing, and assay of transposase accessible chromatin seq. The differential expression and enrichment pathways of TFs in heterotopically ossified tissues were identified. RESULTS: HO that mimicked pathological cells was classified into HO1 and HO2 cell subsets. Results of the pseudo-temporal sequence analysis suggested that HO2 is a differentiated precursor cell of HO1. The analysis of integrated scRNA data revealed that ectopically ossified cells have similar transcriptional characteristics to cells in the fibrocartilaginous zone of tendons. The modified SCENIC method was used to identify specific transcriptional regulators associated with ectopic ossification. Xbp1 was defined as a common key transcriptional regulator of ectopically ossified tissues and the fibrocartilaginous zone of tendons. Subsequently, the CellPhoneDB database was completed for the cellular ligand-receptor analysis. With further pathway screening, this study is the first to propose that Xbp1 may upregulate the Notch signaling pathway through Jag1 transcription. Twenty-four microRNAs were screened and were found to be potentially associated with upregulation of XBP1 expression after acute ischemic stroke. CONCLUSION: A systematic analysis of the differentiation landscape and cellular homogeneity facilitated a molecular understanding of the phenotypic similarities between cells in the fibrocartilaginous region of tendon and HO cells. Furthermore, by identifying Xbp1 as a hub regulator and by conducting a ligand–receptor analysis, we propose a potential Xbp1/Jag1/Notch signaling pathway.
format Online
Article
Text
id pubmed-8563124
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Hindawi
record_format MEDLINE/PubMed
spelling pubmed-85631242021-11-03 Single-Cell Integration Analysis of Heterotopic Ossification and Fibrocartilage Developmental Lineage: Endoplasmic Reticulum Stress Effector Xbp1 Transcriptionally Regulates the Notch Signaling Pathway to Mediate Fibrocartilage Differentiation Chen, Yisheng Sun, Yaying Xu, Yuzhen Lin, Wei-Wei Luo, Zhiwen Han, Zhihua Liu, Shaohua Qi, Beijie Sun, Chenyu Go, Ken Kang, x.-R. Chen, Jiwu Oxid Med Cell Longev Research Article INTRODUCTION: Regeneration of fibrochondrocytes is essential for the healing of the tendon-bone interface (TBI), which is similar to the formation of neurogenic heterotopic ossification (HO). Through single-cell integrative analysis, this study explored the homogeneity of HO cells and fibrochondrocytes. METHODS: This study integrated six datasets, namely, GSE94683, GSE144306, GSE168153, GSE138515, GSE102929, and GSE110993. The differentiation trajectory and key transcription factors (TFs) for HO occurrence were systematically analyzed by integrating single-cell RNA (scRNA) sequencing, bulk RNA sequencing, and assay of transposase accessible chromatin seq. The differential expression and enrichment pathways of TFs in heterotopically ossified tissues were identified. RESULTS: HO that mimicked pathological cells was classified into HO1 and HO2 cell subsets. Results of the pseudo-temporal sequence analysis suggested that HO2 is a differentiated precursor cell of HO1. The analysis of integrated scRNA data revealed that ectopically ossified cells have similar transcriptional characteristics to cells in the fibrocartilaginous zone of tendons. The modified SCENIC method was used to identify specific transcriptional regulators associated with ectopic ossification. Xbp1 was defined as a common key transcriptional regulator of ectopically ossified tissues and the fibrocartilaginous zone of tendons. Subsequently, the CellPhoneDB database was completed for the cellular ligand-receptor analysis. With further pathway screening, this study is the first to propose that Xbp1 may upregulate the Notch signaling pathway through Jag1 transcription. Twenty-four microRNAs were screened and were found to be potentially associated with upregulation of XBP1 expression after acute ischemic stroke. CONCLUSION: A systematic analysis of the differentiation landscape and cellular homogeneity facilitated a molecular understanding of the phenotypic similarities between cells in the fibrocartilaginous region of tendon and HO cells. Furthermore, by identifying Xbp1 as a hub regulator and by conducting a ligand–receptor analysis, we propose a potential Xbp1/Jag1/Notch signaling pathway. Hindawi 2021-10-26 /pmc/articles/PMC8563124/ /pubmed/34737845 http://dx.doi.org/10.1155/2021/7663366 Text en Copyright © 2021 Yisheng Chen et al. https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Chen, Yisheng
Sun, Yaying
Xu, Yuzhen
Lin, Wei-Wei
Luo, Zhiwen
Han, Zhihua
Liu, Shaohua
Qi, Beijie
Sun, Chenyu
Go, Ken
Kang, x.-R.
Chen, Jiwu
Single-Cell Integration Analysis of Heterotopic Ossification and Fibrocartilage Developmental Lineage: Endoplasmic Reticulum Stress Effector Xbp1 Transcriptionally Regulates the Notch Signaling Pathway to Mediate Fibrocartilage Differentiation
title Single-Cell Integration Analysis of Heterotopic Ossification and Fibrocartilage Developmental Lineage: Endoplasmic Reticulum Stress Effector Xbp1 Transcriptionally Regulates the Notch Signaling Pathway to Mediate Fibrocartilage Differentiation
title_full Single-Cell Integration Analysis of Heterotopic Ossification and Fibrocartilage Developmental Lineage: Endoplasmic Reticulum Stress Effector Xbp1 Transcriptionally Regulates the Notch Signaling Pathway to Mediate Fibrocartilage Differentiation
title_fullStr Single-Cell Integration Analysis of Heterotopic Ossification and Fibrocartilage Developmental Lineage: Endoplasmic Reticulum Stress Effector Xbp1 Transcriptionally Regulates the Notch Signaling Pathway to Mediate Fibrocartilage Differentiation
title_full_unstemmed Single-Cell Integration Analysis of Heterotopic Ossification and Fibrocartilage Developmental Lineage: Endoplasmic Reticulum Stress Effector Xbp1 Transcriptionally Regulates the Notch Signaling Pathway to Mediate Fibrocartilage Differentiation
title_short Single-Cell Integration Analysis of Heterotopic Ossification and Fibrocartilage Developmental Lineage: Endoplasmic Reticulum Stress Effector Xbp1 Transcriptionally Regulates the Notch Signaling Pathway to Mediate Fibrocartilage Differentiation
title_sort single-cell integration analysis of heterotopic ossification and fibrocartilage developmental lineage: endoplasmic reticulum stress effector xbp1 transcriptionally regulates the notch signaling pathway to mediate fibrocartilage differentiation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8563124/
https://www.ncbi.nlm.nih.gov/pubmed/34737845
http://dx.doi.org/10.1155/2021/7663366
work_keys_str_mv AT chenyisheng singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT sunyaying singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT xuyuzhen singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT linweiwei singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT luozhiwen singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT hanzhihua singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT liushaohua singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT qibeijie singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT sunchenyu singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT goken singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT kangxr singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation
AT chenjiwu singlecellintegrationanalysisofheterotopicossificationandfibrocartilagedevelopmentallineageendoplasmicreticulumstresseffectorxbp1transcriptionallyregulatesthenotchsignalingpathwaytomediatefibrocartilagedifferentiation

Ejemplares similares