Multiple targets identified with genome wide profiling of small RNA and mRNA expression are linked to fracture healing in mice

Long-bone fracture is a common injury and its healing process at the fracture site involves several overlapping phases, including inflammation, migration of mesenchymal progenitors into the fracture site, endochondral ossification, angiogenesis and finally bone remodelling. Increasing evidence shows...

Descripción completa

Detalles Bibliográficos
Autores principales: Bourgery, Matthieu, Ekholm, Erika, Fagerlund, Katja, Hiltunen, Ari, Puolakkainen, Tero, Pursiheimo, Juha-Pekka, Heino, Terhi, Määttä, Jorma, Heinonen, Jussi, Yatkin, Emrah, Laitala, Tiina, Säämänen, Anna-Marja
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Full Length Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8379442/
https://www.ncbi.nlm.nih.gov/pubmed/34458508
http://dx.doi.org/10.1016/j.bonr.2021.101115
_version_ 1783741009383915520
author Bourgery, Matthieu
Ekholm, Erika
Fagerlund, Katja
Hiltunen, Ari
Puolakkainen, Tero
Pursiheimo, Juha-Pekka
Heino, Terhi
Määttä, Jorma
Heinonen, Jussi
Yatkin, Emrah
Laitala, Tiina
Säämänen, Anna-Marja
author_facet Bourgery, Matthieu
Ekholm, Erika
Fagerlund, Katja
Hiltunen, Ari
Puolakkainen, Tero
Pursiheimo, Juha-Pekka
Heino, Terhi
Määttä, Jorma
Heinonen, Jussi
Yatkin, Emrah
Laitala, Tiina
Säämänen, Anna-Marja
author_sort Bourgery, Matthieu
collection PubMed
description Long-bone fracture is a common injury and its healing process at the fracture site involves several overlapping phases, including inflammation, migration of mesenchymal progenitors into the fracture site, endochondral ossification, angiogenesis and finally bone remodelling. Increasing evidence shows that small noncoding RNAs are important regulators of chondrogenesis, osteogenesis and fracture healing. MicroRNAs are small single-stranded, non-coding RNA-molecules intervening in most physiological and biological processes, including fracture healing. Angiogenin-cleaved 5′ tRNA halves, also called as tiRNAs (stress-induced RNAs) have been shown to repress protein translation. In order to gain further understanding on the role of small noncoding RNAs in fracture healing, genome wide expression profiles of tiRNAs, miRNAs and mRNAs were followed up to 14 days after fracture in callus tissue of an in vivo mouse model with closed tibial fracture and, compared to intact bone and articular cartilage at 2 months of age. Total tiRNA expression level in cartilage was only approximately one third of that observed in control D0 bone. In callus tissue, 11 mature 5′end tiRNAs out of 191 tiRNAs were highly expressed, and seven of them were differentially expressed during fracture healing. When comparing the control tissues, 25 miRNAs characteristic to bone and 29 miRNAs characteristic to cartilage tissue homeostasis were identified. Further, a total of 54 out of 806 miRNAs and 5420 out of 18,700 mRNAs were differentially expressed (DE) in callus tissue during fracture healing and, in comparison to control bone. They were associated to gene ontology processes related to mesenchymal tissue development and differentiation. A total of 581 miRNA-mRNA interactions were identified for these 54 DE miRNAs by literature searches in PubMed, thereby linking by Spearman correlation analysis 14 downregulated and 28 upregulated miRNAs to 164 negatively correlating and 168 positively correlating miRNA-mRNA pairs with chondrogenic and osteogenic phases of fracture healing. These data indicated that tiRNAs and miRNAs were differentially expressed in fracture callus tissue, suggesting them important physiological functions during fracture healing. Hence, the data provided by this study may contribute to future clinical applications, such as potential use as biomarkers or as tools in the development of novel therapeutic approaches for fracture healing.
format Online
Article
Text
id pubmed-8379442
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-83794422021-08-26 Multiple targets identified with genome wide profiling of small RNA and mRNA expression are linked to fracture healing in mice Bourgery, Matthieu Ekholm, Erika Fagerlund, Katja Hiltunen, Ari Puolakkainen, Tero Pursiheimo, Juha-Pekka Heino, Terhi Määttä, Jorma Heinonen, Jussi Yatkin, Emrah Laitala, Tiina Säämänen, Anna-Marja Bone Rep Full Length Article Long-bone fracture is a common injury and its healing process at the fracture site involves several overlapping phases, including inflammation, migration of mesenchymal progenitors into the fracture site, endochondral ossification, angiogenesis and finally bone remodelling. Increasing evidence shows that small noncoding RNAs are important regulators of chondrogenesis, osteogenesis and fracture healing. MicroRNAs are small single-stranded, non-coding RNA-molecules intervening in most physiological and biological processes, including fracture healing. Angiogenin-cleaved 5′ tRNA halves, also called as tiRNAs (stress-induced RNAs) have been shown to repress protein translation. In order to gain further understanding on the role of small noncoding RNAs in fracture healing, genome wide expression profiles of tiRNAs, miRNAs and mRNAs were followed up to 14 days after fracture in callus tissue of an in vivo mouse model with closed tibial fracture and, compared to intact bone and articular cartilage at 2 months of age. Total tiRNA expression level in cartilage was only approximately one third of that observed in control D0 bone. In callus tissue, 11 mature 5′end tiRNAs out of 191 tiRNAs were highly expressed, and seven of them were differentially expressed during fracture healing. When comparing the control tissues, 25 miRNAs characteristic to bone and 29 miRNAs characteristic to cartilage tissue homeostasis were identified. Further, a total of 54 out of 806 miRNAs and 5420 out of 18,700 mRNAs were differentially expressed (DE) in callus tissue during fracture healing and, in comparison to control bone. They were associated to gene ontology processes related to mesenchymal tissue development and differentiation. A total of 581 miRNA-mRNA interactions were identified for these 54 DE miRNAs by literature searches in PubMed, thereby linking by Spearman correlation analysis 14 downregulated and 28 upregulated miRNAs to 164 negatively correlating and 168 positively correlating miRNA-mRNA pairs with chondrogenic and osteogenic phases of fracture healing. These data indicated that tiRNAs and miRNAs were differentially expressed in fracture callus tissue, suggesting them important physiological functions during fracture healing. Hence, the data provided by this study may contribute to future clinical applications, such as potential use as biomarkers or as tools in the development of novel therapeutic approaches for fracture healing. Elsevier 2021-08-05 /pmc/articles/PMC8379442/ /pubmed/34458508 http://dx.doi.org/10.1016/j.bonr.2021.101115 Text en © 2021 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Full Length Article
Bourgery, Matthieu
Ekholm, Erika
Fagerlund, Katja
Hiltunen, Ari
Puolakkainen, Tero
Pursiheimo, Juha-Pekka
Heino, Terhi
Määttä, Jorma
Heinonen, Jussi
Yatkin, Emrah
Laitala, Tiina
Säämänen, Anna-Marja
Multiple targets identified with genome wide profiling of small RNA and mRNA expression are linked to fracture healing in mice
title Multiple targets identified with genome wide profiling of small RNA and mRNA expression are linked to fracture healing in mice
title_full Multiple targets identified with genome wide profiling of small RNA and mRNA expression are linked to fracture healing in mice
title_fullStr Multiple targets identified with genome wide profiling of small RNA and mRNA expression are linked to fracture healing in mice
title_full_unstemmed Multiple targets identified with genome wide profiling of small RNA and mRNA expression are linked to fracture healing in mice
title_short Multiple targets identified with genome wide profiling of small RNA and mRNA expression are linked to fracture healing in mice
title_sort multiple targets identified with genome wide profiling of small rna and mrna expression are linked to fracture healing in mice
topic Full Length Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8379442/
https://www.ncbi.nlm.nih.gov/pubmed/34458508
http://dx.doi.org/10.1016/j.bonr.2021.101115
work_keys_str_mv AT bourgerymatthieu multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT ekholmerika multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT fagerlundkatja multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT hiltunenari multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT puolakkainentero multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT pursiheimojuhapekka multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT heinoterhi multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT maattajorma multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT heinonenjussi multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT yatkinemrah multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT laitalatiina multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice
AT saamanenannamarja multipletargetsidentifiedwithgenomewideprofilingofsmallrnaandmrnaexpressionarelinkedtofracturehealinginmice

Ejemplares similares