Feasibility of an injectable and<i>in situ</i> gelling gelatin hydrogel for demineralized bone matrix powder delivery _Chinese Journal of Reparative and Reconstructive Surgery

Authors：

MA Lu ¹ ,  TIAN Meng ^1,2

1. Department of Neurosurgery, West China Hospital, Sichuan University, Chengdu Sichuan, 610041, P.R.China;
2. Neurosurgery Research Laboratory, West China Hospital, Sichuan University, Chengdu Sichuan, 610041, P.R.China;

Corresponding author：

TIAN Meng, Email: 6744710@qq.com

Keywords：

Injectable andin situ gelling hydrogel; gelatin; demineralized bone matrix; carrier

DOI：

10.7507/1002-1892.201611113

Video：

Export PDF Favorites Scan Get Citation

Abstract Full text Figures/Tables Video References Cited by

Objective To introduce an injectable andin situ gelling gelatin hydrogel, and to explore the possibility as a carrier for demineralized bone matrix (DBM) powder delivery. Methods First, thiolated gelatin was prepared and the thiol content was determined by Ellman method, and then the injectable andin situ gelling gelatin hydrogel (Gel) was formed by crosslinking of the thiolated gelatin and poly (ethylene oxide) diacrylate and the gelation time was determined by inverted method. Finally, the DBM-Gel composite was prepared by mixing Gel and DBM powder. The cytotoxicity was tested by live/dead staining and Alamar blue assay of the encapsulated cells in the DBM-Gel. Forin vitro cell induction, C2C12 cells were firstly incubated onto the surface of the DBM and then the composite was prepared. The experiment included two groups: DBM-Gel and DBM. The alkaline phosphatase (ALP) activity was determined at 1, 3, 5,and 7 days after culture.In vivo osteoinductivity was evaluated using ectopic bone formation model of nude rats. Histological observation and the ALP activity was measured in DBM-Gel and DBM groups at 4 weeks after implantation. Results The thiol content in the thiolated gelatin was (0.51±0.03) mmol/g determined by Ellman method. The gelation time of the hydrogel was (6±1) minutes. DBM powder can be mixed with the hydrogel and injected into the implantation site within the gelation time. The cells in the DBM-Gel exhibited spreading morphology and connected each other in part with increasing culture time. The viability of the cells was 95.4%±1.9%, 97.3%±1.3%, and 96.1%±1.6% at 1, 3, and 7 days after culture, respectively. The relative proliferation was 1.0±0.0, 1.1±0.1, 1.5±0.1, and 1.6±0.1 at 1, 3, 5, and 7 days after culture respectively.In vitro induction showed that the ALP activity of the DBM-Gel group was similar to that of the DBM group, showing no significant difference (P>0.05). With increasing culture time, the ALP activities in both groups increased gradually and the activity at 5 and 7 days was significantly higher than that at 1 and 3 days (P<0.05), while there was no significant difference between at 1 and 3 days, and between 5 and 7 days (P>0.05). At 4 weeks after implantationin vivo, new bone and cartilage were observed, but no bone marrow formation in DBM-Gel group; in DBM group, new bone, new cartilage, and bone marrow formation were observed. The histological osteoinduction scores of DBM-Gel and DBM groups were 4.0 and 4.5, respectively. The ALP activities of DBM-Gel and DBM groups were respectively (119.4±22.7) and (146.7±13.0) μmol/mg protein/min, showing no significant difference (t=–2.085,P=0.082). Conclusion The injectable andin situ gelling gelatin hydrogel for delivery of DBM is feasible.

Citation： MA Lu, TIAN Meng. Feasibility of an injectable andin situ gelling gelatin hydrogel for demineralized bone matrix powder delivery . Chinese Journal of Reparative and Reconstructive Surgery, 2017, 31(3): 300-305. doi: 10.7507/1002-1892.201611113 Copy

1.	Urist MR. Bone: formation by autoinduction. Science, 1965, 150(3698): 893-899.
2.	NaPier Z, Kanim L, Thordarson S,et al. Demineralized bone matrix bone biology and clinical use. Seminars in Spine Surgery, 2016, 28(4): 196-216.
3.	Moghadam HG, Sándor GK, Holmes HH,et al. Histomorphometric evaluation of bone regeneration using allogeneic and alloplastic bone substitutes. J Oral Maxillofac Surg, 2004, 62(2): 202-213.
4.	Wang ZX, Wu DY, Zou JW,et al. Development of demineralized bone matrix-based implantable and biomimetic microcarrier for stem cell expansion and single-step tissue-engineered bone graft construction. J Mater Chem B, 2017, 5: 62-73.
5.	Geisinger JR, Park DK. Allograft bone: Uses in spinal surgery. Seminars in Spine Surgery, 2016, 28(4): 190-195.
6.	Kayal T, Panetta D, Canciani B,et al. Evaluation of the effect of a gamma irradiated DBM-Pluronic F127 composite on bone regeneration in wistar rat. PLoS One, 2015, 10(4): e0125110.
7.	Ding X, Wei X, Huang Y,et al. Delivery of demineralized bone matrix powder using a salt-leached silk fibroin carrier for bone regeneration. J Mater Chem B, 2015, 3: 3177-3188.
8.	Schallenberger M, Lovick H, Locke J,et al. The effect of temperature exposure during shipment on a commercially available demineralized bone matrix putty. Cell and Tissue Banking, 2016, 17(4): 677-687.
9.	Man Z, Hu X, Liu Z,et al. Transplantation of allogenic chondrocytes with chitosan hydrogel-demineralized bone matrix hybrid scaffold to repair rabbit cartilage injury. Biomaterials, 2016, 108: 157-167.
10.	Liu GP, Yang DW, Yin XF. Influence of the bovine serum albumin residues on BMSC-DBM/TCP-based tissue-engineered bone implants. Journal of Biomaterials and Tissue Engineering, 2016, 6: 285-294.
11.	Zhao Y, Han L, Yan J,et al. Irradiation sterilized gelatin-water-glycerol ternary gel as an injectable carrier for bone tissue engineering. Advanced Healthcare Materials, 2016. [Epub ahead of print].
12.	Steven WM, Basil SS, Reginald QK,et al. Chitosan enhances osteogenetic potential of ethylene-oxide sterilized eemineralized bone matrix. Current Tissue Engineering, 2016, 5(7): 130-136.
13.	Murray T, Morscher MA, Kahe AM,et al. Fibular allograft and demineralized bone matrix for the treatment of slipped capital femoral epiphysis. Orthopedics, 2016, 39(3): e519-e525.
14.	Haastert RM, Grote JJ, Blitterswijk CA,et al. Osteoinduction within PEO/PBT copolymer implants in cranial defects using demineralized bone matrix. J Mater Sci Mater Med, 1994, 5: 764-769.
15.	Solheim E, Pinholt EM, Andersen R,et al. The effect of a composite of polyorthoester and demineralized bone on the healing of large segmental defects of the radius in rats. J Bone Joint Surg (Am), 1992, 74(10): 1456-1463.
16.	Butterworth PH, Baum H, Porter JW. A modification of the Ellman procedure for the estimation of protein sulfhydryl groups. Arch Biochem Biophys, 1967, 118(3): 716-723.
17.	Shu XZ, Liu Y, Palumbo FS,et al.In situ crosslinkable hyaluronan hydrogels for tissue engineering. Biomaterials, 2004, 25(7-8): 1339-1348.
18.	Tian M, Yang Z, Kuwahara K,et al. Delivery of demineralized bone matrix powder using a thermogelling chitosan carrier. Acta Biomaterialia, 2012, 8(2): 753-762.
19.	Han B, Tang B, Nimni ME. Quantitative and sensitivein vitro assay for osteoinductive activity of demineralized bone matrix. J Orthop Res, 2003, 21(4): 648-654.
20.	Barbieri D, Yuan H, de Groot F,et al. Influence of different polymeric gels on the ectopic bone forming ability of an osteoinductive biphasic calcium phosphate ceramic. Acta Biomater, 2011, 7(5): 2007-2014.

1. Urist MR. Bone: formation by autoinduction. Science, 1965, 150(3698): 893-899.
2. NaPier Z, Kanim L, Thordarson S,et al. Demineralized bone matrix bone biology and clinical use. Seminars in Spine Surgery, 2016, 28(4): 196-216.
3. Moghadam HG, Sándor GK, Holmes HH,et al. Histomorphometric evaluation of bone regeneration using allogeneic and alloplastic bone substitutes. J Oral Maxillofac Surg, 2004, 62(2): 202-213.
4. Wang ZX, Wu DY, Zou JW,et al. Development of demineralized bone matrix-based implantable and biomimetic microcarrier for stem cell expansion and single-step tissue-engineered bone graft construction. J Mater Chem B, 2017, 5: 62-73.
5. Geisinger JR, Park DK. Allograft bone: Uses in spinal surgery. Seminars in Spine Surgery, 2016, 28(4): 190-195.
6. Kayal T, Panetta D, Canciani B,et al. Evaluation of the effect of a gamma irradiated DBM-Pluronic F127 composite on bone regeneration in wistar rat. PLoS One, 2015, 10(4): e0125110.
7. Ding X, Wei X, Huang Y,et al. Delivery of demineralized bone matrix powder using a salt-leached silk fibroin carrier for bone regeneration. J Mater Chem B, 2015, 3: 3177-3188.
8. Schallenberger M, Lovick H, Locke J,et al. The effect of temperature exposure during shipment on a commercially available demineralized bone matrix putty. Cell and Tissue Banking, 2016, 17(4): 677-687.
9. Man Z, Hu X, Liu Z,et al. Transplantation of allogenic chondrocytes with chitosan hydrogel-demineralized bone matrix hybrid scaffold to repair rabbit cartilage injury. Biomaterials, 2016, 108: 157-167.
10. Liu GP, Yang DW, Yin XF. Influence of the bovine serum albumin residues on BMSC-DBM/TCP-based tissue-engineered bone implants. Journal of Biomaterials and Tissue Engineering, 2016, 6: 285-294.
11. Zhao Y, Han L, Yan J,et al. Irradiation sterilized gelatin-water-glycerol ternary gel as an injectable carrier for bone tissue engineering. Advanced Healthcare Materials, 2016. [Epub ahead of print].
12. Steven WM, Basil SS, Reginald QK,et al. Chitosan enhances osteogenetic potential of ethylene-oxide sterilized eemineralized bone matrix. Current Tissue Engineering, 2016, 5(7): 130-136.
13. Murray T, Morscher MA, Kahe AM,et al. Fibular allograft and demineralized bone matrix for the treatment of slipped capital femoral epiphysis. Orthopedics, 2016, 39(3): e519-e525.
14. Haastert RM, Grote JJ, Blitterswijk CA,et al. Osteoinduction within PEO/PBT copolymer implants in cranial defects using demineralized bone matrix. J Mater Sci Mater Med, 1994, 5: 764-769.
15. Solheim E, Pinholt EM, Andersen R,et al. The effect of a composite of polyorthoester and demineralized bone on the healing of large segmental defects of the radius in rats. J Bone Joint Surg (Am), 1992, 74(10): 1456-1463.
16. Butterworth PH, Baum H, Porter JW. A modification of the Ellman procedure for the estimation of protein sulfhydryl groups. Arch Biochem Biophys, 1967, 118(3): 716-723.
17. Shu XZ, Liu Y, Palumbo FS,et al.In situ crosslinkable hyaluronan hydrogels for tissue engineering. Biomaterials, 2004, 25(7-8): 1339-1348.
18. Tian M, Yang Z, Kuwahara K,et al. Delivery of demineralized bone matrix powder using a thermogelling chitosan carrier. Acta Biomaterialia, 2012, 8(2): 753-762.
19. Han B, Tang B, Nimni ME. Quantitative and sensitivein vitro assay for osteoinductive activity of demineralized bone matrix. J Orthop Res, 2003, 21(4): 648-654.
20. Barbieri D, Yuan H, de Groot F,et al. Influence of different polymeric gels on the ectopic bone forming ability of an osteoinductive biphasic calcium phosphate ceramic. Acta Biomater, 2011, 7(5): 2007-2014.

Chinese Journal of Reparative and Reconstructive Surgery

Feasibility of an injectable andin situ gelling gelatin hydrogel for demineralized bone matrix powder delivery

Abstract Full text Figures/Tables Video References Cited by

Previous Article

Next Article

Format

Content