Novel wnt regulator NEL-like molecule-1 antagonizes adipogenesis and augments osteogenesis induced by bone morphogenetic protein 2

Jia Shen; Aaron W. James; Xinli Zhang; Shen Pang; Janette N. Zara; Greg Asatrian; Michael Chiang; Min Lee; Kevork Khadarian; Alan Nguyen; Kevin S. Lee; Ronald K. Siu; Sotirios Tetradis; Kang Ting; Chia Soo

doi:10.1016/j.ajpath.2015.10.011

Novel wnt regulator NEL-like molecule-1 antagonizes adipogenesis and augments osteogenesis induced by bone morphogenetic protein 2

Jia Shen, Aaron W. James, Xinli Zhang, Shen Pang, Janette N. Zara, Greg Asatrian, Michael Chiang, Min Lee, Kevork Khadarian, Alan Nguyen, Kevin S. Lee, Ronald K. Siu, Sotirios Tetradis, Kang Ting, Chia Soo

Research output: Contribution to journal › Article › peer-review

51 Scopus citations

Abstract

The differentiation factor NEL-like molecule-1 (NELL-1) has been reported as osteoinductive in multiple in vivo preclinical models. Bone morphogenetic protein (BMP)-2 is used clinically for skeletal repair, but in vivo administration can induce abnormal, adipose-filled, poor-quality bone. We demonstrate that NELL-1 combined with BMP2 significantly optimizes osteogenesis in a rodent femoral segmental defect model by minimizing the formation of BMP2-induced adipose-filled cystlike bone. In vitro studies using the mouse bone marrow stromal cell line M2-10B4 and human primary bone marrow stromal cells have confirmed that NELL-1 enhances BMP2-induced osteogenesis and inhibits BMP2-induced adipogenesis. Importantly, the ability of NELL-1 to direct BMP2-treated cells toward osteogenesis and away from adipogenesis requires intact canonical Wnt signaling. Overall, these studies establish the feasibility of combining NELL-1 with BMP2 to improve clinical bone regeneration and provide mechanistic insight into canonical Wnt pathway activity during NELL-1 and BMP2 osteogenesis. The novel abilities of NELL-1 to stimulate Wnt signaling and to repress adipogenesis may highlight new treatment approaches for bone loss in osteoporosis.

Original language	English (US)
Pages (from-to)	419-434
Number of pages	16
Journal	American Journal of Pathology
Volume	186
Issue number	2
DOIs	https://doi.org/10.1016/j.ajpath.2015.10.011
State	Published - Feb 1 2016
Externally published	Yes

ASJC Scopus subject areas

Pathology and Forensic Medicine

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10.1016/j.ajpath.2015.10.011

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Shen, J., James, A. W., Zhang, X., Pang, S., Zara, J. N., Asatrian, G., Chiang, M., Lee, M., Khadarian, K., Nguyen, A., Lee, K. S., Siu, R. K., Tetradis, S., Ting, K., & Soo, C. (2016). Novel wnt regulator NEL-like molecule-1 antagonizes adipogenesis and augments osteogenesis induced by bone morphogenetic protein 2. American Journal of Pathology, 186(2), 419-434. https://doi.org/10.1016/j.ajpath.2015.10.011

Shen, J, James, AW, Zhang, X, Pang, S, Zara, JN, Asatrian, G, Chiang, M, Lee, M, Khadarian, K, Nguyen, A, Lee, KS, Siu, RK, Tetradis, S, Ting, K & Soo, C 2016, 'Novel wnt regulator NEL-like molecule-1 antagonizes adipogenesis and augments osteogenesis induced by bone morphogenetic protein 2', American Journal of Pathology, vol. 186, no. 2, pp. 419-434. https://doi.org/10.1016/j.ajpath.2015.10.011

@article{7fb79e57e8e44021abe771b971195213,

title = "Novel wnt regulator NEL-like molecule-1 antagonizes adipogenesis and augments osteogenesis induced by bone morphogenetic protein 2",

abstract = "The differentiation factor NEL-like molecule-1 (NELL-1) has been reported as osteoinductive in multiple in vivo preclinical models. Bone morphogenetic protein (BMP)-2 is used clinically for skeletal repair, but in vivo administration can induce abnormal, adipose-filled, poor-quality bone. We demonstrate that NELL-1 combined with BMP2 significantly optimizes osteogenesis in a rodent femoral segmental defect model by minimizing the formation of BMP2-induced adipose-filled cystlike bone. In vitro studies using the mouse bone marrow stromal cell line M2-10B4 and human primary bone marrow stromal cells have confirmed that NELL-1 enhances BMP2-induced osteogenesis and inhibits BMP2-induced adipogenesis. Importantly, the ability of NELL-1 to direct BMP2-treated cells toward osteogenesis and away from adipogenesis requires intact canonical Wnt signaling. Overall, these studies establish the feasibility of combining NELL-1 with BMP2 to improve clinical bone regeneration and provide mechanistic insight into canonical Wnt pathway activity during NELL-1 and BMP2 osteogenesis. The novel abilities of NELL-1 to stimulate Wnt signaling and to repress adipogenesis may highlight new treatment approaches for bone loss in osteoporosis.",

author = "Jia Shen and James, {Aaron W.} and Xinli Zhang and Shen Pang and Zara, {Janette N.} and Greg Asatrian and Michael Chiang and Min Lee and Kevork Khadarian and Alan Nguyen and Lee, {Kevin S.} and Siu, {Ronald K.} and Sotirios Tetradis and Kang Ting and Chia Soo",

note = "Funding Information: Supported by the California Institute for Regenerative Medicine Early Translational II Research Award TR2-01821 (C.S.); NIH/NIDCR grants R21 DE0177711 (C.S.), RO1 DE01607 (K.T.), and RO1 AR061399-01A1 (C.S.); University of California Discovery grant 07-10677 (C.S.); Eli & Edythe Broad Center of Regenerative Medicine; and a Stem Cell Research at UCLA Innovation Award. R.K.S. and A.W.J. were supported by T32 training fellowship 5T32DE007296-14. J.N.Z. was supported by CIRM training fellowship TG2-01169. Publisher Copyright: {\textcopyright} 2016 American Society for Investigative Pathology.",

year = "2016",

month = feb,

day = "1",

doi = "10.1016/j.ajpath.2015.10.011",

language = "English (US)",

volume = "186",

pages = "419--434",

journal = "American Journal of Pathology",

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T1 - Novel wnt regulator NEL-like molecule-1 antagonizes adipogenesis and augments osteogenesis induced by bone morphogenetic protein 2

AU - Shen, Jia

AU - James, Aaron W.

AU - Zhang, Xinli

AU - Pang, Shen

AU - Zara, Janette N.

AU - Asatrian, Greg

AU - Chiang, Michael

AU - Lee, Min

AU - Khadarian, Kevork

AU - Nguyen, Alan

AU - Lee, Kevin S.

AU - Siu, Ronald K.

AU - Tetradis, Sotirios

AU - Ting, Kang

AU - Soo, Chia

N1 - Funding Information: Supported by the California Institute for Regenerative Medicine Early Translational II Research Award TR2-01821 (C.S.); NIH/NIDCR grants R21 DE0177711 (C.S.), RO1 DE01607 (K.T.), and RO1 AR061399-01A1 (C.S.); University of California Discovery grant 07-10677 (C.S.); Eli & Edythe Broad Center of Regenerative Medicine; and a Stem Cell Research at UCLA Innovation Award. R.K.S. and A.W.J. were supported by T32 training fellowship 5T32DE007296-14. J.N.Z. was supported by CIRM training fellowship TG2-01169. Publisher Copyright: © 2016 American Society for Investigative Pathology.

PY - 2016/2/1

Y1 - 2016/2/1

N2 - The differentiation factor NEL-like molecule-1 (NELL-1) has been reported as osteoinductive in multiple in vivo preclinical models. Bone morphogenetic protein (BMP)-2 is used clinically for skeletal repair, but in vivo administration can induce abnormal, adipose-filled, poor-quality bone. We demonstrate that NELL-1 combined with BMP2 significantly optimizes osteogenesis in a rodent femoral segmental defect model by minimizing the formation of BMP2-induced adipose-filled cystlike bone. In vitro studies using the mouse bone marrow stromal cell line M2-10B4 and human primary bone marrow stromal cells have confirmed that NELL-1 enhances BMP2-induced osteogenesis and inhibits BMP2-induced adipogenesis. Importantly, the ability of NELL-1 to direct BMP2-treated cells toward osteogenesis and away from adipogenesis requires intact canonical Wnt signaling. Overall, these studies establish the feasibility of combining NELL-1 with BMP2 to improve clinical bone regeneration and provide mechanistic insight into canonical Wnt pathway activity during NELL-1 and BMP2 osteogenesis. The novel abilities of NELL-1 to stimulate Wnt signaling and to repress adipogenesis may highlight new treatment approaches for bone loss in osteoporosis.

AB - The differentiation factor NEL-like molecule-1 (NELL-1) has been reported as osteoinductive in multiple in vivo preclinical models. Bone morphogenetic protein (BMP)-2 is used clinically for skeletal repair, but in vivo administration can induce abnormal, adipose-filled, poor-quality bone. We demonstrate that NELL-1 combined with BMP2 significantly optimizes osteogenesis in a rodent femoral segmental defect model by minimizing the formation of BMP2-induced adipose-filled cystlike bone. In vitro studies using the mouse bone marrow stromal cell line M2-10B4 and human primary bone marrow stromal cells have confirmed that NELL-1 enhances BMP2-induced osteogenesis and inhibits BMP2-induced adipogenesis. Importantly, the ability of NELL-1 to direct BMP2-treated cells toward osteogenesis and away from adipogenesis requires intact canonical Wnt signaling. Overall, these studies establish the feasibility of combining NELL-1 with BMP2 to improve clinical bone regeneration and provide mechanistic insight into canonical Wnt pathway activity during NELL-1 and BMP2 osteogenesis. The novel abilities of NELL-1 to stimulate Wnt signaling and to repress adipogenesis may highlight new treatment approaches for bone loss in osteoporosis.

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DO - 10.1016/j.ajpath.2015.10.011

M3 - Article

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AN - SCOPUS:84955345106

SN - 0002-9440

VL - 186

SP - 419

EP - 434

JO - American Journal of Pathology

JF - American Journal of Pathology

IS - 2

ER -

Novel wnt regulator NEL-like molecule-1 antagonizes adipogenesis and augments osteogenesis induced by bone morphogenetic protein 2

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