Notch Signaling Inhibition by LY411575 Attenuates Osteoblast Differentiation and Decreased Ectopic Bone Formation Capacity of Human Skeletal (Mesenchymal) Stem Cells

BACKGROUND: Chemical biology approaches using small molecule inhibitors targeting specific signaling pathways are useful tools to dissect the molecular mechanisms governing stem cell differentiation and for their possible use in therapeutic interventions. METHODS: Stem cell signaling small molecule...

Descripción completa

Detalles Bibliográficos
Autores principales: AlMuraikhi, Nihal, Ali, Dalia, Vishnubalaji, Radhakrishnan, Manikandan, Muthurangan, Atteya, Muhammad, Siyal, Abdulaziz, Alfayez, Musaad, Aldahmash, Abdullah, Kassem, Moustapha, Alajez, Nehad M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6724428/
https://www.ncbi.nlm.nih.gov/pubmed/31534459
http://dx.doi.org/10.1155/2019/3041262
_version_ 1783448990895833088
author AlMuraikhi, Nihal
Ali, Dalia
Vishnubalaji, Radhakrishnan
Manikandan, Muthurangan
Atteya, Muhammad
Siyal, Abdulaziz
Alfayez, Musaad
Aldahmash, Abdullah
Kassem, Moustapha
Alajez, Nehad M.
author_facet AlMuraikhi, Nihal
Ali, Dalia
Vishnubalaji, Radhakrishnan
Manikandan, Muthurangan
Atteya, Muhammad
Siyal, Abdulaziz
Alfayez, Musaad
Aldahmash, Abdullah
Kassem, Moustapha
Alajez, Nehad M.
author_sort AlMuraikhi, Nihal
collection PubMed
description BACKGROUND: Chemical biology approaches using small molecule inhibitors targeting specific signaling pathways are useful tools to dissect the molecular mechanisms governing stem cell differentiation and for their possible use in therapeutic interventions. METHODS: Stem cell signaling small molecule library functional screen was performed employing human bone marrow skeletal (mesenchymal) stem cells (hBMSCs). Alkaline phosphatase (ALP) activity and formation of mineralized matrix visualized by Alizarin red staining were employed as markers for osteoblastic differentiation. Global gene expression profiling was conducted using the Agilent microarray platform, and data normalization and bioinformatics were performed using GeneSpring software. Pathway analyses were conducted using the Ingenuity Pathway Analysis (IPA) tool. In vivo ectopic bone formation was performed using hBMSC mixed with hydroxyapatite–tricalcium phosphate granules that were implanted subcutaneously in 8-week-old female nude mice. Hematoxylin and eosin staining and Sirius red staining were performed to identify bone formation in vivo. RESULTS: Among the tested molecules, LY411575, a potent γ-secretase and Notch signaling inhibitor, exhibited significant inhibitory effects on osteoblastic differentiation of hBMSCs manifested by reduced ALP activity, mineralized matrix formation, and decreased osteoblast-specific gene expression as well as in vivo ectopic bone formation. Global gene expression profiling of LY411575-treated cells revealed changes in multiple signaling pathways, including focal adhesion, insulin, TGFβ, IL6, and Notch signaling, and decreased the expression of genes associated with functional categories of tissue development. Among the affected signaling networks were TGFβ1, SPP1, and ERK regulatory networks. CONCLUSIONS: We identified γ-secretase inhibitor (LY411575) as a potent regulator of osteoblastic differentiation of hBMSC that may be useful as a therapeutic option for treating conditions associated with ectopic bone formation.
format Online
Article
Text
id pubmed-6724428
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Hindawi
record_format MEDLINE/PubMed
spelling pubmed-67244282019-09-18 Notch Signaling Inhibition by LY411575 Attenuates Osteoblast Differentiation and Decreased Ectopic Bone Formation Capacity of Human Skeletal (Mesenchymal) Stem Cells AlMuraikhi, Nihal Ali, Dalia Vishnubalaji, Radhakrishnan Manikandan, Muthurangan Atteya, Muhammad Siyal, Abdulaziz Alfayez, Musaad Aldahmash, Abdullah Kassem, Moustapha Alajez, Nehad M. Stem Cells Int Research Article BACKGROUND: Chemical biology approaches using small molecule inhibitors targeting specific signaling pathways are useful tools to dissect the molecular mechanisms governing stem cell differentiation and for their possible use in therapeutic interventions. METHODS: Stem cell signaling small molecule library functional screen was performed employing human bone marrow skeletal (mesenchymal) stem cells (hBMSCs). Alkaline phosphatase (ALP) activity and formation of mineralized matrix visualized by Alizarin red staining were employed as markers for osteoblastic differentiation. Global gene expression profiling was conducted using the Agilent microarray platform, and data normalization and bioinformatics were performed using GeneSpring software. Pathway analyses were conducted using the Ingenuity Pathway Analysis (IPA) tool. In vivo ectopic bone formation was performed using hBMSC mixed with hydroxyapatite–tricalcium phosphate granules that were implanted subcutaneously in 8-week-old female nude mice. Hematoxylin and eosin staining and Sirius red staining were performed to identify bone formation in vivo. RESULTS: Among the tested molecules, LY411575, a potent γ-secretase and Notch signaling inhibitor, exhibited significant inhibitory effects on osteoblastic differentiation of hBMSCs manifested by reduced ALP activity, mineralized matrix formation, and decreased osteoblast-specific gene expression as well as in vivo ectopic bone formation. Global gene expression profiling of LY411575-treated cells revealed changes in multiple signaling pathways, including focal adhesion, insulin, TGFβ, IL6, and Notch signaling, and decreased the expression of genes associated with functional categories of tissue development. Among the affected signaling networks were TGFβ1, SPP1, and ERK regulatory networks. CONCLUSIONS: We identified γ-secretase inhibitor (LY411575) as a potent regulator of osteoblastic differentiation of hBMSC that may be useful as a therapeutic option for treating conditions associated with ectopic bone formation. Hindawi 2019-08-22 /pmc/articles/PMC6724428/ /pubmed/31534459 http://dx.doi.org/10.1155/2019/3041262 Text en Copyright © 2019 Nihal AlMuraikhi et al. http://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
AlMuraikhi, Nihal
Ali, Dalia
Vishnubalaji, Radhakrishnan
Manikandan, Muthurangan
Atteya, Muhammad
Siyal, Abdulaziz
Alfayez, Musaad
Aldahmash, Abdullah
Kassem, Moustapha
Alajez, Nehad M.
Notch Signaling Inhibition by LY411575 Attenuates Osteoblast Differentiation and Decreased Ectopic Bone Formation Capacity of Human Skeletal (Mesenchymal) Stem Cells
title Notch Signaling Inhibition by LY411575 Attenuates Osteoblast Differentiation and Decreased Ectopic Bone Formation Capacity of Human Skeletal (Mesenchymal) Stem Cells
title_full Notch Signaling Inhibition by LY411575 Attenuates Osteoblast Differentiation and Decreased Ectopic Bone Formation Capacity of Human Skeletal (Mesenchymal) Stem Cells
title_fullStr Notch Signaling Inhibition by LY411575 Attenuates Osteoblast Differentiation and Decreased Ectopic Bone Formation Capacity of Human Skeletal (Mesenchymal) Stem Cells
title_full_unstemmed Notch Signaling Inhibition by LY411575 Attenuates Osteoblast Differentiation and Decreased Ectopic Bone Formation Capacity of Human Skeletal (Mesenchymal) Stem Cells
title_short Notch Signaling Inhibition by LY411575 Attenuates Osteoblast Differentiation and Decreased Ectopic Bone Formation Capacity of Human Skeletal (Mesenchymal) Stem Cells
title_sort notch signaling inhibition by ly411575 attenuates osteoblast differentiation and decreased ectopic bone formation capacity of human skeletal (mesenchymal) stem cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6724428/
https://www.ncbi.nlm.nih.gov/pubmed/31534459
http://dx.doi.org/10.1155/2019/3041262
work_keys_str_mv AT almuraikhinihal notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT alidalia notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT vishnubalajiradhakrishnan notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT manikandanmuthurangan notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT atteyamuhammad notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT siyalabdulaziz notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT alfayezmusaad notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT aldahmashabdullah notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT kassemmoustapha notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells
AT alajeznehadm notchsignalinginhibitionbyly411575attenuatesosteoblastdifferentiationanddecreasedectopicboneformationcapacityofhumanskeletalmesenchymalstemcells

Ejemplares similares