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    Selective Retinoic Acid Receptor γ Antagonist 7C is a Potent Enhancer of BMP-Induced Ectopic Endochondral Bone Formation.

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    Author
    Tateiwa, Daisuke
    Kaito, Takashi
    Hashimoto, Kunihiko
    Okada, Rintaro
    Kodama, Joe
    Kushioka, Junichi
    Bal, Zeynep
    Tsukazaki, Hiroyuki
    Nakagawa, Shinichi
    Ukon, Yuichiro
    Hirai, Hiromasa
    Tian, Hongying
    Alferiev, Ivan
    Chorny, Michael
    Otsuru, Satoru
    Okada, Seiji
    Iwamoto, Masahiro
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    Date
    2022-03-14
    Journal
    Frontiers in Cell and Developmental Biology
    Publisher
    Frontiers Media S.A.
    Type
    Article
    
    Metadata
    Show full item record
    See at
    https://doi.org/10.3389/fcell.2022.802699
    Abstract
    Bone morphogenetic proteins (BMPs) have been clinically applied for induction of bone formation in musculoskeletal disorders such as critical-sized bone defects, nonunions, and spinal fusion surgeries. However, the use of supraphysiological doses of BMP caused adverse events, which were sometimes life-threatening. Therefore, safer treatment strategies for bone regeneration have been sought for decades. Systemic administration of a potent selective antagonist of retinoic acid nuclear receptor gamma (RARγ) (7C) stimulated BMP-induced ectopic bone formation. In this study, we developed 7C-loaded poly lactic nanoparticles (7C-NPs) and examined whether local application of 7C enhances BMP-induced bone regeneration. The collagen sponge discs that absorbed recombinant human (rh) BMP-2 were implanted into the dorsal fascia of young adult mice to induce ectopic bone. The combination of rhBMP-2 and 7C-NP markedly increased the total bone volume and thickness of the bone shell of the ectopic bone in a dose-dependent manner compared to those with rhBMP-2 only. 7C stimulated sulfated proteoglycan production, expression of chondrogenic marker genes, and Sox9 reporter activity in both chondrogenic cells and MSCs. The findings suggest that selective RARγ antagonist 7C or the related compounds potentiate the bone inductive ability of rhBMP-2, as well as support any future research to improve the BMP-2 based bone regeneration procedures in a safe and efficient manner.
    Rights/Terms
    Copyright © 2022 Tateiwa, Kaito, Hashimoto, Okada, Kodama, Kushioka, Bal, Tsukazaki, Nakagawa, Ukon, Hirai, Tian, Alferiev, Chorny, Otsuru, Okada and Iwamoto.
    Keyword
    Bmp/Smad signaling
    RARγ inverse agonist
    bone morphogenetic protein
    bone regeneration
    endochondral bone formation
    retinoic acid receptor γ
    Identifier to cite or link to this item
    http://hdl.handle.net/10713/18442
    ae974a485f413a2113503eed53cd6c53
    10.3389/fcell.2022.802699
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