Open Access
Open access
volume 8 issue 1 publication number 41

A novel negative regulatory mechanism of Smurf2 in BMP/Smad signaling in bone

Junichi Kushioka 1
Takashi Kaito 1
Rintaro Okada 1
Hiroyuki Ishiguro 1
Zeynep Bal 1
Joe Kodama 1
Ryota Chijimatsu 2
Melanie Pye 3
Masahiro Narimatsu 3
Jeffrey L. Wrana 3
Yasumichi Inoue 4
Hiroko NINOMIYA 5
Shin Yamamoto 6
TAKASHI SAITOU 5, 7
HIDEKI YOSHIKAWA 1
Takeshi Imamura 5, 7
Publication typeJournal Article
Publication date2020-11-23
scimago Q1
wos Q1
SJR4.048
CiteScore23.3
Impact factor15.0
ISSN20954700, 20956231
Histology
Physiology
Endocrinology, Diabetes and Metabolism
Abstract
Transforming growth factor-β (TGF-β) and bone morphogenetic protein (BMP) play important roles in bone metabolism. Smad ubiquitination regulatory factors (Smurfs) regulate TGF-β/BMP signaling via ubiquitination, resulting in degradation of signaling molecules to prevent excessive activation of TGF-β/BMP signaling. Though Smurf2 has been shown to negatively regulate TGF-β/Smad signaling, its involvement in BMP/Smad signaling in bone metabolism has not been thoroughly investigated. In the present study, we sought to evaluate the role of Smurf2 in BMP/Smad signaling in bone metabolism. Absorbable collagen sponges containing 3 μg of recombinant human BMP2 (rhBMP2) were implanted in the dorsal muscle pouches of wild type (WT) and Smurf2−/− mice. The rhBMP2-induced ectopic bone in Smurf2−/− mice showed greater bone mass, higher mineral apposition and bone formation rates, and greater osteoblast numbers than the ectopic bone in WT mice. In WT mice, the ectopic bone consisted of a thin discontinuous outer cortical shell and scant inner trabecular bone. In contrast, in Smurf2−/− mice, the induced bone consisted of a thick, continuous outer cortical shell and abundant inner trabecular bone. Additionally, rhBMP2-stimulated bone marrow stromal cells (BMSCs) from Smurf2−/− mice showed increased osteogenic differentiation. Smurf2 induced the ubiquitination of Smad1/5. BMP/Smad signaling was enhanced in Smurf2−/− BMSCs stimulated with rhBMP2, and the inhibition of BMP/Smad signaling suppressed osteogenic differentiation of these BMSCs. These findings demonstrate that Smurf2 negatively regulates BMP/Smad signaling, thereby identifying a new regulatory mechanism in bone metabolism.
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GOST Copy
Kushioka J. et al. A novel negative regulatory mechanism of Smurf2 in BMP/Smad signaling in bone // Bone Research. 2020. Vol. 8. No. 1. 41
GOST all authors (up to 50) Copy
Kushioka J., Kaito T., Okada R., Ishiguro H., Bal Z., Kodama J., Chijimatsu R., Pye M., Narimatsu M., Wrana J., Inoue Y., NINOMIYA H., Yamamoto S., SAITOU T., YOSHIKAWA H., Imamura T. A novel negative regulatory mechanism of Smurf2 in BMP/Smad signaling in bone // Bone Research. 2020. Vol. 8. No. 1. 41
RIS |
Cite this
RIS Copy
TY - JOUR
DO - 10.1038/s41413-020-00115-z
UR - https://doi.org/10.1038/s41413-020-00115-z
TI - A novel negative regulatory mechanism of Smurf2 in BMP/Smad signaling in bone
T2 - Bone Research
AU - Kushioka, Junichi
AU - Kaito, Takashi
AU - Okada, Rintaro
AU - Ishiguro, Hiroyuki
AU - Bal, Zeynep
AU - Kodama, Joe
AU - Chijimatsu, Ryota
AU - Pye, Melanie
AU - Narimatsu, Masahiro
AU - Wrana, Jeffrey L.
AU - Inoue, Yasumichi
AU - NINOMIYA, Hiroko
AU - Yamamoto, Shin
AU - SAITOU, TAKASHI
AU - YOSHIKAWA, HIDEKI
AU - Imamura, Takeshi
PY - 2020
DA - 2020/11/23
PB - Springer Nature
IS - 1
VL - 8
PMID - 33298874
SN - 2095-4700
SN - 2095-6231
ER -
BibTex
Cite this
BibTex (up to 50 authors) Copy
@article{2020_Kushioka,
author = {Junichi Kushioka and Takashi Kaito and Rintaro Okada and Hiroyuki Ishiguro and Zeynep Bal and Joe Kodama and Ryota Chijimatsu and Melanie Pye and Masahiro Narimatsu and Jeffrey L. Wrana and Yasumichi Inoue and Hiroko NINOMIYA and Shin Yamamoto and TAKASHI SAITOU and HIDEKI YOSHIKAWA and Takeshi Imamura},
title = {A novel negative regulatory mechanism of Smurf2 in BMP/Smad signaling in bone},
journal = {Bone Research},
year = {2020},
volume = {8},
publisher = {Springer Nature},
month = {nov},
url = {https://doi.org/10.1038/s41413-020-00115-z},
number = {1},
pages = {41},
doi = {10.1038/s41413-020-00115-z}
}