Transforming growth factor-β receptor 1: An intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure

INTRODUCTION: Fetal-originated osteoarthritis is relative to poor cartilage quality and may exhibit transgenerational genetic effects. Previous findings revealed prenatal dexamethasone exposure (PDE) induced poor cartilage quality in offspring. OBJECTIVES: This study focused on further exploring mol...

Descripción completa

Detalles Bibliográficos
Autores principales: Liu, Liang, Li, Bin, Li, Qingxian, Han, Hui, Zhou, Siqi, Wu, Zhixin, Gao, Hui, Zhu, Jiayong, Gu, Hanwen, Chen, Liaobin, Wang, Hui
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10173161/
https://www.ncbi.nlm.nih.gov/pubmed/35953031
http://dx.doi.org/10.1016/j.jare.2022.08.002
_version_ 1785039759976955904
author Liu, Liang
Li, Bin
Li, Qingxian
Han, Hui
Zhou, Siqi
Wu, Zhixin
Gao, Hui
Zhu, Jiayong
Gu, Hanwen
Chen, Liaobin
Wang, Hui
author_facet Liu, Liang
Li, Bin
Li, Qingxian
Han, Hui
Zhou, Siqi
Wu, Zhixin
Gao, Hui
Zhu, Jiayong
Gu, Hanwen
Chen, Liaobin
Wang, Hui
author_sort Liu, Liang
collection PubMed
description INTRODUCTION: Fetal-originated osteoarthritis is relative to poor cartilage quality and may exhibit transgenerational genetic effects. Previous findings revealed prenatal dexamethasone exposure (PDE) induced poor cartilage quality in offspring. OBJECTIVES: This study focused on further exploring molecular mechanism, heritability, and early intervention of fetal-originated osteoarthritis. METHODS: Pregnant rats (F0) were segregated into control and PDE groups depending upon whether dexamethasone was administered on gestational days (GDs) 9–20. Some female offspring were bred with healthy males during postnatal week (PW) 8 to attain the F2 and F3 generations. The F3-generation rats were administrated with glucosamine intragastrically at PW12 for 6 weeks. The knee cartilages of male and female rats at different time points were harvested to assay their morphologies and functions. Furthermore, primary chondrocytes from the F3-generation rats were isolated to confirm the mechanism and intervention target of glucosamine. RESULTS: Compared with the control, female and male rats in each generation of PDE group showed thinner cartilage thicknesses; shallower and uneven staining; fewer chondrocytes; higher Osteoarthritis Research Society International scores; and lower mRNA and protein expression of SP1, TGFβR1, Smad2, SOX9, ACAN and COL2A1. After F3-generation rats were treated with glucosamine, all of the above changes could be reversed. In primary chondrocytes isolated from the F3-generation rats of PDE group, glucosamine promoted SP1 expression and binding to TGFβR1 promoter to increase the expression of TGFβR1, p-Smad2, SOX9, ACAN and COL2A1, but these were prevented by SB431542 (a potent and selective inhibitor of TGFβR1). CONCLUSIONS: PDE induced chondrodysplasia in offspring and stably inherited in F3-generation rats, which was related to decreased expression of SP1/TGFβR1/Smad2/SOX9 pathway to reduce the cartilage matrix synthesis, without major sex-based variations. Glucosamine could alleviate the poor genetic cartilage quality in offspring induced by PDE by up-regulating SP1/TGFβR1 signaling, which was prevented by a TGFβR1 inhibitor. This study elucidated the molecular mechanism and therapeutic target (TGFβR1) of genetic chondrodysplasia caused by PDE, which provides a research basis for precisely treating fetal-originated osteoarthritis.
format Online
Article
Text
id pubmed-10173161
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-101731612023-05-12 Transforming growth factor-β receptor 1: An intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure Liu, Liang Li, Bin Li, Qingxian Han, Hui Zhou, Siqi Wu, Zhixin Gao, Hui Zhu, Jiayong Gu, Hanwen Chen, Liaobin Wang, Hui J Adv Res Original Article INTRODUCTION: Fetal-originated osteoarthritis is relative to poor cartilage quality and may exhibit transgenerational genetic effects. Previous findings revealed prenatal dexamethasone exposure (PDE) induced poor cartilage quality in offspring. OBJECTIVES: This study focused on further exploring molecular mechanism, heritability, and early intervention of fetal-originated osteoarthritis. METHODS: Pregnant rats (F0) were segregated into control and PDE groups depending upon whether dexamethasone was administered on gestational days (GDs) 9–20. Some female offspring were bred with healthy males during postnatal week (PW) 8 to attain the F2 and F3 generations. The F3-generation rats were administrated with glucosamine intragastrically at PW12 for 6 weeks. The knee cartilages of male and female rats at different time points were harvested to assay their morphologies and functions. Furthermore, primary chondrocytes from the F3-generation rats were isolated to confirm the mechanism and intervention target of glucosamine. RESULTS: Compared with the control, female and male rats in each generation of PDE group showed thinner cartilage thicknesses; shallower and uneven staining; fewer chondrocytes; higher Osteoarthritis Research Society International scores; and lower mRNA and protein expression of SP1, TGFβR1, Smad2, SOX9, ACAN and COL2A1. After F3-generation rats were treated with glucosamine, all of the above changes could be reversed. In primary chondrocytes isolated from the F3-generation rats of PDE group, glucosamine promoted SP1 expression and binding to TGFβR1 promoter to increase the expression of TGFβR1, p-Smad2, SOX9, ACAN and COL2A1, but these were prevented by SB431542 (a potent and selective inhibitor of TGFβR1). CONCLUSIONS: PDE induced chondrodysplasia in offspring and stably inherited in F3-generation rats, which was related to decreased expression of SP1/TGFβR1/Smad2/SOX9 pathway to reduce the cartilage matrix synthesis, without major sex-based variations. Glucosamine could alleviate the poor genetic cartilage quality in offspring induced by PDE by up-regulating SP1/TGFβR1 signaling, which was prevented by a TGFβR1 inhibitor. This study elucidated the molecular mechanism and therapeutic target (TGFβR1) of genetic chondrodysplasia caused by PDE, which provides a research basis for precisely treating fetal-originated osteoarthritis. Elsevier 2022-08-09 /pmc/articles/PMC10173161/ /pubmed/35953031 http://dx.doi.org/10.1016/j.jare.2022.08.002 Text en © 2023 The Authors. Published by Elsevier B.V. on behalf of Cairo University. 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 Original Article
Liu, Liang
Li, Bin
Li, Qingxian
Han, Hui
Zhou, Siqi
Wu, Zhixin
Gao, Hui
Zhu, Jiayong
Gu, Hanwen
Chen, Liaobin
Wang, Hui
Transforming growth factor-β receptor 1: An intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure
title Transforming growth factor-β receptor 1: An intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure
title_full Transforming growth factor-β receptor 1: An intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure
title_fullStr Transforming growth factor-β receptor 1: An intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure
title_full_unstemmed Transforming growth factor-β receptor 1: An intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure
title_short Transforming growth factor-β receptor 1: An intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure
title_sort transforming growth factor-β receptor 1: an intervention target for genetic poor cartilage quality induced by prenatal dexamethasone exposure
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10173161/
https://www.ncbi.nlm.nih.gov/pubmed/35953031
http://dx.doi.org/10.1016/j.jare.2022.08.002
work_keys_str_mv AT liuliang transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT libin transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT liqingxian transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT hanhui transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT zhousiqi transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT wuzhixin transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT gaohui transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT zhujiayong transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT guhanwen transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT chenliaobin transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure
AT wanghui transforminggrowthfactorbreceptor1aninterventiontargetforgeneticpoorcartilagequalityinducedbyprenataldexamethasoneexposure

Ejemplares similares