Novel gain-of-function mutation of TRPV4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia

Metatropic dysplasia is a congenital skeletal dysplasia characterized by severe platyspondyly, dumbbell-like deformity of long tubular bones, and progressive kyphoscoliosis with growth. It is caused by mutations in the gene TRPV4, encoding the transient receptor potential vanilloid 4, which acts as...

Descripción completa

Detalles Bibliográficos
Autores principales: Nonaka, Kentaro, Han, Xu, Kato, Hiroki, Sato, Hiroshi, Yamaza, Haruyoshi, Hirofuji, Yuta, Masuda, Keiji
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6709385/
https://www.ncbi.nlm.nih.gov/pubmed/31463371
http://dx.doi.org/10.1016/j.bbrep.2019.100648
_version_ 1783446198075523072
author Nonaka, Kentaro
Han, Xu
Kato, Hiroki
Sato, Hiroshi
Yamaza, Haruyoshi
Hirofuji, Yuta
Masuda, Keiji
author_facet Nonaka, Kentaro
Han, Xu
Kato, Hiroki
Sato, Hiroshi
Yamaza, Haruyoshi
Hirofuji, Yuta
Masuda, Keiji
author_sort Nonaka, Kentaro
collection PubMed
description Metatropic dysplasia is a congenital skeletal dysplasia characterized by severe platyspondyly, dumbbell-like deformity of long tubular bones, and progressive kyphoscoliosis with growth. It is caused by mutations in the gene TRPV4, encoding the transient receptor potential vanilloid 4, which acts as a calcium channel. Many heterozygous single base mutations of this gene have been associated with the disorder, showing autosomal dominant inheritance. Although abnormal endochondral ossification has been observed by histological examination of bone in a patient with lethal metatropic dysplasia, the etiology of the disorder remains largely unresolved. As dental pulp stem cells (DPSCs) are mesenchymal stem cells that differentiate into bone lineage cells, DPSCs derived from patients with congenital skeletal dysplasia might be useful as a disease-specific cellular model for etiological investigation. The purpose of this study was to clarify the pathological association between TRPV4 mutation and chondrocyte differentiation by analyzing DPSCs from a patient with non-lethal metatropic dysplasia. We identified a novel heterozygous single base mutation, c.1855C>T in TRPV4. This was predicted to be a missense mutation, p.L619F, in putative transmembrane segment 5. The mutation was repaired by CRISPR/Cas9 system to obtain isogenic control DPSCs for further analysis. The expression of stem cell markers and fibroblast-like morphology were comparable between patient-derived mutant and control DPSCs, although expression of TRPV4 was lower in mutant DPSCs than control DPSCs. Despite the lower TRPV4 expression in mutant DPSCs, the intracellular Ca(2+) level was comparable at the basal level between mutant and control DPSCs, while its level was markedly higher following stimulation with 4α-phorbol 12,13-didecanoate (4αPDD), a specific agonist for TRPV4, in mutant DPSCs than in control DPSCs. In the presence of 4αPDD, we observed accelerated early chondrocyte differentiation and upregulated mRNA expression of SRY-box 9 (SOX9) in mutant DPSCs. Our findings suggested that the novel missense mutation c.1855C>T of TRPV4 was a gain-of-function mutation leading to enhanced intracellular Ca(2+) level, which was associated with accelerated chondrocyte differentiation and SOX9 upregulation. Our results also suggest that patient-derived DPSCs can be a useful disease-specific cellular model for elucidating the pathological mechanism of metatropic dysplasia.
format Online
Article
Text
id pubmed-6709385
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-67093852019-08-28 Novel gain-of-function mutation of TRPV4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia Nonaka, Kentaro Han, Xu Kato, Hiroki Sato, Hiroshi Yamaza, Haruyoshi Hirofuji, Yuta Masuda, Keiji Biochem Biophys Rep Research Article Metatropic dysplasia is a congenital skeletal dysplasia characterized by severe platyspondyly, dumbbell-like deformity of long tubular bones, and progressive kyphoscoliosis with growth. It is caused by mutations in the gene TRPV4, encoding the transient receptor potential vanilloid 4, which acts as a calcium channel. Many heterozygous single base mutations of this gene have been associated with the disorder, showing autosomal dominant inheritance. Although abnormal endochondral ossification has been observed by histological examination of bone in a patient with lethal metatropic dysplasia, the etiology of the disorder remains largely unresolved. As dental pulp stem cells (DPSCs) are mesenchymal stem cells that differentiate into bone lineage cells, DPSCs derived from patients with congenital skeletal dysplasia might be useful as a disease-specific cellular model for etiological investigation. The purpose of this study was to clarify the pathological association between TRPV4 mutation and chondrocyte differentiation by analyzing DPSCs from a patient with non-lethal metatropic dysplasia. We identified a novel heterozygous single base mutation, c.1855C>T in TRPV4. This was predicted to be a missense mutation, p.L619F, in putative transmembrane segment 5. The mutation was repaired by CRISPR/Cas9 system to obtain isogenic control DPSCs for further analysis. The expression of stem cell markers and fibroblast-like morphology were comparable between patient-derived mutant and control DPSCs, although expression of TRPV4 was lower in mutant DPSCs than control DPSCs. Despite the lower TRPV4 expression in mutant DPSCs, the intracellular Ca(2+) level was comparable at the basal level between mutant and control DPSCs, while its level was markedly higher following stimulation with 4α-phorbol 12,13-didecanoate (4αPDD), a specific agonist for TRPV4, in mutant DPSCs than in control DPSCs. In the presence of 4αPDD, we observed accelerated early chondrocyte differentiation and upregulated mRNA expression of SRY-box 9 (SOX9) in mutant DPSCs. Our findings suggested that the novel missense mutation c.1855C>T of TRPV4 was a gain-of-function mutation leading to enhanced intracellular Ca(2+) level, which was associated with accelerated chondrocyte differentiation and SOX9 upregulation. Our results also suggest that patient-derived DPSCs can be a useful disease-specific cellular model for elucidating the pathological mechanism of metatropic dysplasia. Elsevier 2019-05-17 /pmc/articles/PMC6709385/ /pubmed/31463371 http://dx.doi.org/10.1016/j.bbrep.2019.100648 Text en © 2019 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Article
Nonaka, Kentaro
Han, Xu
Kato, Hiroki
Sato, Hiroshi
Yamaza, Haruyoshi
Hirofuji, Yuta
Masuda, Keiji
Novel gain-of-function mutation of TRPV4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia
title Novel gain-of-function mutation of TRPV4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia
title_full Novel gain-of-function mutation of TRPV4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia
title_fullStr Novel gain-of-function mutation of TRPV4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia
title_full_unstemmed Novel gain-of-function mutation of TRPV4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia
title_short Novel gain-of-function mutation of TRPV4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia
title_sort novel gain-of-function mutation of trpv4 associated with accelerated chondrogenic differentiation of dental pulp stem cells derived from a patient with metatropic dysplasia
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6709385/
https://www.ncbi.nlm.nih.gov/pubmed/31463371
http://dx.doi.org/10.1016/j.bbrep.2019.100648
work_keys_str_mv AT nonakakentaro novelgainoffunctionmutationoftrpv4associatedwithacceleratedchondrogenicdifferentiationofdentalpulpstemcellsderivedfromapatientwithmetatropicdysplasia
AT hanxu novelgainoffunctionmutationoftrpv4associatedwithacceleratedchondrogenicdifferentiationofdentalpulpstemcellsderivedfromapatientwithmetatropicdysplasia
AT katohiroki novelgainoffunctionmutationoftrpv4associatedwithacceleratedchondrogenicdifferentiationofdentalpulpstemcellsderivedfromapatientwithmetatropicdysplasia
AT satohiroshi novelgainoffunctionmutationoftrpv4associatedwithacceleratedchondrogenicdifferentiationofdentalpulpstemcellsderivedfromapatientwithmetatropicdysplasia
AT yamazaharuyoshi novelgainoffunctionmutationoftrpv4associatedwithacceleratedchondrogenicdifferentiationofdentalpulpstemcellsderivedfromapatientwithmetatropicdysplasia
AT hirofujiyuta novelgainoffunctionmutationoftrpv4associatedwithacceleratedchondrogenicdifferentiationofdentalpulpstemcellsderivedfromapatientwithmetatropicdysplasia
AT masudakeiji novelgainoffunctionmutationoftrpv4associatedwithacceleratedchondrogenicdifferentiationofdentalpulpstemcellsderivedfromapatientwithmetatropicdysplasia

Ejemplares similares