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An HDAC inhibitor, entinostat/MS-275, partially prevents delayed cranial suture closure in heterozygous Runx2 null mice

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Version 2 2024-06-13, 10:32
Version 1 2017-05-16, 14:49
journal contribution
posted on 2024-06-13, 10:32 authored by HS Bae, WJ Yoon, YD Cho, R Islam, HR Shin, BS Kim, JM Lim, MS Seo, SA Cho, KY Choi, SH Baek, HG Kim, KM Woo, JH Baek, YS Lee, HM Ryoo
Cleidocranial dysplasia (CCD) is an autosomal dominant skeletal disorder caused by mutations in RUNX2, coding a key transcription factor of early osteogenesis. CCD patients suffer from developmental defects in cranial bones. Despite numerous investigations and clinical approaches, no therapeutic strategy has been suggested to prevent CCD. Here, we show that fetal administration of Entinostat/MS-275, a class I histone deacetylase (HDAC)-specific inhibitor, partially prevents delayed closure of cranial sutures in Runx2 +/- mice strain of C57BL/6J by two mechanisms: 1) posttranslational acetylation of Runx2 protein, which stabilized the protein and activated its transcriptional activity; and 2) epigenetic regulation of Runx2 and other bone marker genes. Moreover, we show that MS-275 stimulates osteoblast proliferation effectively both in vivo and in vitro, suggesting that delayed skeletal development in CCD is closely related to the decreased number of progenitor cells as well as the delayed osteogenic differentiation. These findings provide the potential benefits of the therapeutic strategy using MS-275 to prevent CCD.

History

Journal

Journal of bone and mineral research

Volume

32

Pagination

951-961

Location

Chichester, Eng.

Open access

  • Yes

ISSN

0884-0431

eISSN

1523-4681

Language

eng

Publication classification

C Journal article, C1.1 Refereed article in a scholarly journal

Copyright notice

2017, American Society for Bone and Mineral Research

Issue

5

Publisher

John Wiley & Sons

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