Blockage of Src by Specific siRNA as a Novel Therapeutic Strategy to Prevent Destructive Repair in Steroid-Associated Osteonecrosis in Rabbits

Li Zhen Zheng; Hui Juan Cao; Shi Hui Chen; Tao Tang; Wei Min Fu; Le Huang; Dick Ho Kiu Chow; Yi Xiang Wang; James Francis Griffith; Wei He; Hong Zhou; De Wei Zhao; Ge Zhang; Xin Luan Wang; Ling Qin

doi:10.1002/jbmr.2542

Blockage of Src by Specific siRNA as a Novel Therapeutic Strategy to Prevent Destructive Repair in Steroid-Associated Osteonecrosis in Rabbits

Li Zhen Zheng, Hui Juan Cao, Shi Hui Chen, Tao Tang, Wei Min Fu, Le Huang, Dick Ho Kiu Chow, Yi Xiang Wang, James Francis Griffith, Wei He, Hong Zhou, De Wei Zhao, Ge Zhang, Xin Luan Wang, Ling Qin

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

37 Citations (Scopus)

Abstract

Vascular hyperpermeability and highly upregulated bone resorption in the destructive repair progress of steroid-associated osteonecrosis (SAON) are associated with a high expression of VEGF and high Src activity (Src is encoded by the cellular sarcoma [c-src] gene). This study was designed to prove our hypothesis that blocking the VEGF-Src signaling pathway by specific Src siRNA is able to prevent destructive repair in a SAON rabbit model. Destructive repair in SAON was induced in rabbits. At 2, 4, and 6 weeks after SAON induction, VEGF, anti-VEGF, Src siRNA, Src siRNA+VEGF, control siRNA, and saline were introduced via intramedullary injection into proximal femora for each group, respectively. Vascularization and permeability were quantified by dynamic contrast-enhanced (DCE) MRI. At week 6 after SAON induction, proximal femurs were dissected for micro-computed tomography (μCT)-based trabecular architecture with finite element analysis (FEA), μCT-based angiography, and histological analysis. Histological evaluation revealed that VEGF enhanced destructive repair, whereas anti-VEGF prevented destructive repair and Src siRNA and Src siRNA+VEGF prevented destructive repair and enhanced reparative osteogenesis. Findings of angiography and histomorphometry were consistent with those determined by DCE MRI. Src siRNA inhibited VEGF-mediated vascular hyperpermeability but preserved VEGF-induced neovascularization. Bone resorption was enhanced in the VEGF group and inhibited in the anti-VEGF, Src siRNA, Src siRNA+VEGF groups as determined by both 3D μCT and 2D histomorphometry. FEA showed higher estimated failure load in the Src siRNA and Src siRNA+VEGF groups when compared to the vehicle control group. Blockage of VEGF-Src signaling pathway by specific Src siRNA was able to prevent steroid-associated destructive repair while improving reconstructive repair in SAON, which might become a novel therapeutic strategy.

Original language	English
Pages (from-to)	2044-2057
Number of pages	14
Journal	Journal of Bone and Mineral Research
Volume	30
Issue number	11
DOIs	https://doi.org/10.1002/jbmr.2542
Publication status	Published - Nov 2015
Externally published	Yes

Keywords

OSTEONECROSIS
REPAIR
SIRNA
SRC

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1002/jbmr.2542

Cite this

Zheng, L. Z., Cao, H. J., Chen, S. H., Tang, T., Fu, W. M., Huang, L., Chow, D. H. K., Wang, Y. X., Griffith, J. F., He, W., Zhou, H., Zhao, D. W., Zhang, G., Wang, X. L., & Qin, L. (2015). Blockage of Src by Specific siRNA as a Novel Therapeutic Strategy to Prevent Destructive Repair in Steroid-Associated Osteonecrosis in Rabbits. Journal of Bone and Mineral Research, 30(11), 2044-2057. https://doi.org/10.1002/jbmr.2542

@article{0c22c2c0bd86459a8d78becff2d19d2b,

title = "Blockage of Src by Specific siRNA as a Novel Therapeutic Strategy to Prevent Destructive Repair in Steroid-Associated Osteonecrosis in Rabbits",

abstract = "Vascular hyperpermeability and highly upregulated bone resorption in the destructive repair progress of steroid-associated osteonecrosis (SAON) are associated with a high expression of VEGF and high Src activity (Src is encoded by the cellular sarcoma [c-src] gene). This study was designed to prove our hypothesis that blocking the VEGF-Src signaling pathway by specific Src siRNA is able to prevent destructive repair in a SAON rabbit model. Destructive repair in SAON was induced in rabbits. At 2, 4, and 6 weeks after SAON induction, VEGF, anti-VEGF, Src siRNA, Src siRNA+VEGF, control siRNA, and saline were introduced via intramedullary injection into proximal femora for each group, respectively. Vascularization and permeability were quantified by dynamic contrast-enhanced (DCE) MRI. At week 6 after SAON induction, proximal femurs were dissected for micro-computed tomography (μCT)-based trabecular architecture with finite element analysis (FEA), μCT-based angiography, and histological analysis. Histological evaluation revealed that VEGF enhanced destructive repair, whereas anti-VEGF prevented destructive repair and Src siRNA and Src siRNA+VEGF prevented destructive repair and enhanced reparative osteogenesis. Findings of angiography and histomorphometry were consistent with those determined by DCE MRI. Src siRNA inhibited VEGF-mediated vascular hyperpermeability but preserved VEGF-induced neovascularization. Bone resorption was enhanced in the VEGF group and inhibited in the anti-VEGF, Src siRNA, Src siRNA+VEGF groups as determined by both 3D μCT and 2D histomorphometry. FEA showed higher estimated failure load in the Src siRNA and Src siRNA+VEGF groups when compared to the vehicle control group. Blockage of VEGF-Src signaling pathway by specific Src siRNA was able to prevent steroid-associated destructive repair while improving reconstructive repair in SAON, which might become a novel therapeutic strategy.",

keywords = "OSTEONECROSIS, REPAIR, SIRNA, SRC",

author = "Zheng, {Li Zhen} and Cao, {Hui Juan} and Chen, {Shi Hui} and Tao Tang and Fu, {Wei Min} and Le Huang and Chow, {Dick Ho Kiu} and Wang, {Yi Xiang} and Griffith, {James Francis} and Wei He and Hong Zhou and Zhao, {De Wei} and Ge Zhang and Wang, {Xin Luan} and Ling Qin",

note = "Publisher Copyright: {\textcopyright} 2015 American Society for Bone and Mineral Research. {\textcopyright} 2015 American Society for Bone and Mineral Research.",

year = "2015",

month = nov,

doi = "10.1002/jbmr.2542",

language = "English",

volume = "30",

pages = "2044--2057",

number = "11",

}

Zheng, LZ, Cao, HJ, Chen, SH, Tang, T, Fu, WM, Huang, L, Chow, DHK, Wang, YX, Griffith, JF, He, W, Zhou, H, Zhao, DW, Zhang, G, Wang, XL & Qin, L 2015, 'Blockage of Src by Specific siRNA as a Novel Therapeutic Strategy to Prevent Destructive Repair in Steroid-Associated Osteonecrosis in Rabbits', Journal of Bone and Mineral Research, vol. 30, no. 11, pp. 2044-2057. https://doi.org/10.1002/jbmr.2542

TY - JOUR

T1 - Blockage of Src by Specific siRNA as a Novel Therapeutic Strategy to Prevent Destructive Repair in Steroid-Associated Osteonecrosis in Rabbits

AU - Zheng, Li Zhen

AU - Cao, Hui Juan

AU - Chen, Shi Hui

AU - Tang, Tao

AU - Fu, Wei Min

AU - Huang, Le

AU - Chow, Dick Ho Kiu

AU - Wang, Yi Xiang

AU - Griffith, James Francis

AU - He, Wei

AU - Zhou, Hong

AU - Zhao, De Wei

AU - Zhang, Ge

AU - Wang, Xin Luan

AU - Qin, Ling

PY - 2015/11

Y1 - 2015/11

N2 - Vascular hyperpermeability and highly upregulated bone resorption in the destructive repair progress of steroid-associated osteonecrosis (SAON) are associated with a high expression of VEGF and high Src activity (Src is encoded by the cellular sarcoma [c-src] gene). This study was designed to prove our hypothesis that blocking the VEGF-Src signaling pathway by specific Src siRNA is able to prevent destructive repair in a SAON rabbit model. Destructive repair in SAON was induced in rabbits. At 2, 4, and 6 weeks after SAON induction, VEGF, anti-VEGF, Src siRNA, Src siRNA+VEGF, control siRNA, and saline were introduced via intramedullary injection into proximal femora for each group, respectively. Vascularization and permeability were quantified by dynamic contrast-enhanced (DCE) MRI. At week 6 after SAON induction, proximal femurs were dissected for micro-computed tomography (μCT)-based trabecular architecture with finite element analysis (FEA), μCT-based angiography, and histological analysis. Histological evaluation revealed that VEGF enhanced destructive repair, whereas anti-VEGF prevented destructive repair and Src siRNA and Src siRNA+VEGF prevented destructive repair and enhanced reparative osteogenesis. Findings of angiography and histomorphometry were consistent with those determined by DCE MRI. Src siRNA inhibited VEGF-mediated vascular hyperpermeability but preserved VEGF-induced neovascularization. Bone resorption was enhanced in the VEGF group and inhibited in the anti-VEGF, Src siRNA, Src siRNA+VEGF groups as determined by both 3D μCT and 2D histomorphometry. FEA showed higher estimated failure load in the Src siRNA and Src siRNA+VEGF groups when compared to the vehicle control group. Blockage of VEGF-Src signaling pathway by specific Src siRNA was able to prevent steroid-associated destructive repair while improving reconstructive repair in SAON, which might become a novel therapeutic strategy.

AB - Vascular hyperpermeability and highly upregulated bone resorption in the destructive repair progress of steroid-associated osteonecrosis (SAON) are associated with a high expression of VEGF and high Src activity (Src is encoded by the cellular sarcoma [c-src] gene). This study was designed to prove our hypothesis that blocking the VEGF-Src signaling pathway by specific Src siRNA is able to prevent destructive repair in a SAON rabbit model. Destructive repair in SAON was induced in rabbits. At 2, 4, and 6 weeks after SAON induction, VEGF, anti-VEGF, Src siRNA, Src siRNA+VEGF, control siRNA, and saline were introduced via intramedullary injection into proximal femora for each group, respectively. Vascularization and permeability were quantified by dynamic contrast-enhanced (DCE) MRI. At week 6 after SAON induction, proximal femurs were dissected for micro-computed tomography (μCT)-based trabecular architecture with finite element analysis (FEA), μCT-based angiography, and histological analysis. Histological evaluation revealed that VEGF enhanced destructive repair, whereas anti-VEGF prevented destructive repair and Src siRNA and Src siRNA+VEGF prevented destructive repair and enhanced reparative osteogenesis. Findings of angiography and histomorphometry were consistent with those determined by DCE MRI. Src siRNA inhibited VEGF-mediated vascular hyperpermeability but preserved VEGF-induced neovascularization. Bone resorption was enhanced in the VEGF group and inhibited in the anti-VEGF, Src siRNA, Src siRNA+VEGF groups as determined by both 3D μCT and 2D histomorphometry. FEA showed higher estimated failure load in the Src siRNA and Src siRNA+VEGF groups when compared to the vehicle control group. Blockage of VEGF-Src signaling pathway by specific Src siRNA was able to prevent steroid-associated destructive repair while improving reconstructive repair in SAON, which might become a novel therapeutic strategy.

KW - OSTEONECROSIS

KW - REPAIR

KW - SIRNA

KW - SRC

UR - http://www.scopus.com/inward/record.url?scp=84945438370&partnerID=8YFLogxK

U2 - 10.1002/jbmr.2542

DO - 10.1002/jbmr.2542

M3 - Article

C2 - 25917347

AN - SCOPUS:84945438370

SN - 0884-0431

VL - 30

SP - 2044

EP - 2057

JO - Journal of Bone and Mineral Research

JF - Journal of Bone and Mineral Research

IS - 11

ER -

Blockage of Src by Specific siRNA as a Novel Therapeutic Strategy to Prevent Destructive Repair in Steroid-Associated Osteonecrosis in Rabbits

Abstract

Keywords

UN SDGs

Access to Document

Other files and links

Fingerprint

Cite this