Osteogenic potential of Gingival Mesenchymal Stem Cells on Chitosan scaffold for Treatment of Peri-implant Defects (An Experimental Study)
Adel, G., Khalil, A., Moustafa, A., Abdelfatah, D., Shamaa, A. (2022). Osteogenic potential of Gingival Mesenchymal Stem Cells on Chitosan scaffold for Treatment of Peri-implant Defects (An Experimental Study). EKB Journal Management System, 33(3), 51-56. doi: 10.21608/mjmr.2022.266371
Ghadeer M. Adel; Ahmed A. Khalil; Ahmed A. Moustafa; Dina S. Abdelfatah; Ashraf Ali Shamaa. "Osteogenic potential of Gingival Mesenchymal Stem Cells on Chitosan scaffold for Treatment of Peri-implant Defects (An Experimental Study)". EKB Journal Management System, 33, 3, 2022, 51-56. doi: 10.21608/mjmr.2022.266371
Adel, G., Khalil, A., Moustafa, A., Abdelfatah, D., Shamaa, A. (2022). 'Osteogenic potential of Gingival Mesenchymal Stem Cells on Chitosan scaffold for Treatment of Peri-implant Defects (An Experimental Study)', EKB Journal Management System, 33(3), pp. 51-56. doi: 10.21608/mjmr.2022.266371
Adel, G., Khalil, A., Moustafa, A., Abdelfatah, D., Shamaa, A. Osteogenic potential of Gingival Mesenchymal Stem Cells on Chitosan scaffold for Treatment of Peri-implant Defects (An Experimental Study). EKB Journal Management System, 2022; 33(3): 51-56. doi: 10.21608/mjmr.2022.266371

Osteogenic potential of Gingival Mesenchymal Stem Cells on Chitosan scaffold for Treatment of Peri-implant Defects (An Experimental Study)

Minia Journal of Medical Research
Volume 33, Issue 3, July 2022, Page 51-56  XML PDF (376.72 K)
Document Type: Original Article
DOI: 10.21608/mjmr.2022.266371
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Authors
Ghadeer M. Adel1; Ahmed A. Khalil1; Ahmed A. Moustafa1; Dina S. Abdelfatah2; Ashraf Ali Shamaa3
1Oral medicine, Diagnosis and periodontology department, Faculty of Dentistry Minia University Egypt
2Medical Biochemistry and Molecular Biology, Faculty of Medicine Cairo University
3Surgery, Anesthesiology and Radiology, Faculty of Veterinary, Medicine Cairo University
Abstract
Background: Implant therapy is now considered an acceptable successful way to replace hopeless teeth. the purpose of this study was to Evaluate the use of gingival mesenchymal stem cell (GMSC) on chitosan scaffold in the treatment of peri-implant defects. Method: A total of ten mongral dogs age ranging between 1 to 2 years old weight from 20 to 25kg were used in the current study. Dogs were scheduled for first premolars extraction one on each side and immediate replacement by immediate implant at mesial socket with creation of peri-implant defect at distal socket. Sites were randomly assigned in a split mouth design into two groups: control group in which the defects were filled with chitosan only, intervention group in which the defects were filled by Gingival Mesenchymal Stem Cells (GMSCs) carried on chitosan scaffold. Five dogs will be sacrificed 1month and the others will be sacrificed at 3 months post operation. Bone density was measured around each implant at defect sides at baseline (implant insertion), 1 month and 3 months. Results IBM SPSS 28 for windows software was used for the analysis, there was a significant difference in bone density change, as bone density change was higher in intervention group, p-value > 0.05 at one month but there was no statistically significant difference observed between the two groups at three Oral medicine, Diagnosis and periodontology department Faculty of Dentistry Minia University Egypt  Conclusion:using gingival mesenchymal stem cells in treatment of peri-implant defects gives better results in shorter duration, but same results can be reached with chitosan alone in longer duration and less costs. More studies with larger sample size are recommended.
 
 
 

Highlights

conclusion

Stem-cell-based therapies have been a promising alternative for bone regeneration. Selection of appropriate donor cell types plays an important role in successful cell transplantation. The present study provides evidence that systemically transplanted GMSCs can not only home to the peri-implant defect but also promote bone regeneration. Given the basic characteristics of MSCs and advantages such as ease of isolation, high proliferation capacity, uniformly homogenous property, and so on, GMSCs are considered as an ideal candidate cell resource for cell-based therapies. Future studies using large animal numbers and longer duration are needed to assess the long term safety and efficacy of GMSCs for bone regeneration.

Keywords
Gingival Mesenchymal Stem Cells;   Peri-implant Defects; Chitosan scaffold
Full Text

.Introduction

Implant therapy is now considered an acceptable successful way to replace hopeless teeth (1). Immediate implantation has many advantages like proper implant placement, decrease time needed for to receive prosthesis and patient satisfying with function and esthetics at time of implantation (2).

However, the main challenge of immediate post extraction implants is significant alveolar bone loss due to periodontal disease, abnormalities, traumatic injury, or physiological bone resorption. Many modalities are used nowadays to deal with these challenges. One of them the technology of tissue engineering that has proven to be a promising therapy for bone regeneration with the establishment of an artificial biomaterial containing regenerating-competent cells and osteogenic growth factors achievable (3).

Today, using of stem cells is considered as a mainstream strategy for periodontal therapy, particularly for complete regeneration of the periodontal complex, which implies not only the reconstruction of appropriate alveolar bone but also the induction of cementogenesis along the root surfaces with the oriented insertion of newly formed periodontal tissue (4).Regarding dental originated sources, gingival mesenchymal stem cells (GMSCs) considered more interesting alternatives to the other dental MSCs as they are much easier to get from the clinically resected gingival tissues. Therefore, it is of great concern to prove the multiple differentiation potentials of GMSCs for possible tissue engineering applications (5).

For tissue engineering, scaffolds are needed to provide a three-dimensional microenvironment to accommodate cells and guide their adhesion, growth, and subsequent differentiation. A plethora of materials have been developed for tissue engineering approaches, namely natural and synthetic polymers, metals, ceramics, and composites, which have been fabricated into porous scaffolds, microparticles, sponges, meshes, nanofibers, and gels.

 

Natural polymers are preferred over synthetic or metallic materials, since they have better biocompatibility and ability to degrade in vivo without releasing toxic substances (6). One of these natural polymers commonly used is chitosan which is biocompatible and biodegradable and is currently used with other polymers in a variety of tissue engineering applications.

 

Many studies revealed that using autogenous or xenogenous (human) mesenchymal stem cell MSC to treat peri-implant defects gives higher results in bone formation and bone implant contact than using synthetic bone graft alone.

 

Also, treatment of peri-implant defects with bone marrow derived MSC and bone marrow mononuclear cells that had undergone ex vivo osteogenic differentiation prior to clinical use (7) resulted in higher new bone apposition than scaffolds alone.

 

Materials and Method

A total of ten mongral dogs age ranging between 1 to 2 years old weight from 20 to 25kg were used in this study. All experiments were conducted in the animal house of the Faculty of Medicine, Cairo University, Egypt according to the recommendations and approval of the Ethics Committee on animal’s experimentation of the Faculty of Medicine, Cairo University.

  • Isolation of gingival mesenchymal stem cell (GMSC):

Gingival sample will be obtained by resecting a small piece of gingiva to prepare gingival mesenchymal stem cell (GMSC). G-MSCs will be obtained from the healthy gingival collars around partially impacted third molars. Cells’ isolation and culture will be done as formerly described (8).

  • Biodegradable scaffold synthesis: A biodegradable composite made of Chitosan (Ch) will be generated by a simple molding method as previously described (9).
  • Animal preparation: The animal model will be prepared as previously described by Boix and colleagues (10).
  • Surgical procedures: dogs will be anesthetized by intramuscular injection of ketamine (10 mg/kg) and xylazine (4 mg/kg), measures will be taken to minimize pain to the dogs. Under sterile conditions, the first mandibular premolar teeth will be extracted bilaterally. Immediately, distal bone defects adjacent to the mesial socket 6 mm in height, 4 mm in the bucco-lingual direction, and 5 mm in the mesio-distal direction were created in the mandible bone. Then titanium implants were installed into the mesial area of the bone defect in each side. The primary stability was assessed.
  • Defects were randomly divided into 2 groups, control group in which defects were filled with chitosan scaffold alone and intervention group in which defects were filled with GMSCs carried on chitosan scaffold. Five dogs were sacrificed 1 month, and the others were sacrificed at 3 months post operation.
  • Radiological evaluation was done by taking periapical radiographs at baseline, 1month and 3 months after implant placement according to time of scarification. Bone density was measured using Digora software.
  • Data were collected, tabulated and statistically examined.

 

Fig.1 after extraction of 1st          fig.2 after implant placement bilaterally

premolar bilaterally

 

Fig.3 placement of stem cell on   fig.4 placement of chitosan scaffold                              

 chitosan scaffold

Fig. suturing bilaterally

   

Fig.6 Right side after one month

Fig.7 Left side after one month
   

Fig.8 Right side three month

 Fig.9 Left side three month

 

3.Results:

Paired sample t-test was done to compare bone density at baseline and after one and three months between control group and intervention group.

 

Intervention group

Control group

Mean difference

P-value

 

Mean

SD

Mean

SD

Bone density change

58.73

11

19.71

2.6

39.02

*0.003

There was a significant difference in bone density change, as bone density change was higher in intervention group (mean= 58.73, SD= 11.00) than in control group (mean= 19.71, SD=2.60), p-value= 0.003.

 

 

 

 

Intervention group

control group

Mean difference

P-value

 

Mean

SD

Mean

SD

Bone density change

41.14

6.61

44.29

5.45

-3.15

0.343

No statistically significant difference was observed between the two groups regarding bone density change.

 

  1. Discussion

Stem-cell-based therapies aiming at regeneration of bone defects have been a promising alternative for clinical trial (11). As novel postnatal stem cells, GMSCs have been paid extensive attention for their therapeutic potential in regenerative medicine (12).

GMSCs can be easily isolated from human gingival tissue which is usually discarded as biological waste in the clinic and proliferate rapidly in vitro to meet the transplantation requirement for cell amount.

The contribution of GMSCs to bone regeneration was confirmed by radiologic assessment of the bone density in the present study. As we found, at 1- and 3-months post transplantation, the newly formed bone in intervention group was significantly higher than that in control group at one month and it was also higher at 3 months at intervention than control but without significance.

In addition to the osteogenenic potential of GMSCs to promote the new bone forming, another possible explanation responsible for the therapeutic effects of GMSCs on bone injuries was the transplanted GMSCs triggered the endogenous MSCs recruitment which is known to be crucial for successful bone repair (13), though the mechanisms of MSCs recruitment to the injury sites were unclear.

References
References

1- Esposito M, Grusovin MG, Polyzos IP, Felice P and Worthington HV.Interventions for replacing missing teeth: Dental implants in fresh extraction sockets (immediate, immediate-delayed and delayed implants). Cochrane Database Syst Rev 2010.

2- Bhola M, Neely AL, Kolhatkar S. Immediate implant placement: clinical decisions, advantages, and disadvantages. J Prosthodont 2008; 17:576–581.

3- Kaigler D, Avila G, Wisner-Lynch L, et al. Platelet-derived growth factor applications in periodontal and peri-implant bone regeneration. Expert Opin Biol Ther 2011; 11:375–385.

4- Chen FM, Gao LN, Tian BM, Zhang XY, Zhang YJ, Dong GY, Lu H, Chu Q, Xu J, Yu Y, Wu RX, Yin Y, Shi S, Jin Y. Treatment of periodontal intrabony defects using autologous periodontal ligament stem cells: a randomized clinical trial. Stem Cell Res Ther. 2016 Feb 19;7:33.

5- Iman M. Aboushady , Zeinab A. Salem , Dina Sabry and Abbas Mohamed. Comparative study of the osteogenic potential of mesenchymal stem cells derived from different sources. J Clin Exp Dent. 2018;10(1):e7-13.

6- Edgar L, McNamara K,Wong T, Tamburrini R, Katari R, Orlando G. Heterogeneity of scaffold biomaterials in tissue engineering. Materials (Basel, Switzerland). 2016;9(5). https://doi.org/10. 3390/ma9050332.

7-Suaid FF, Ribeiro FV, Rodrigues TL, Silvério KG, Carvalho MD, Nociti FH Jr, Casati MZ, Sallum EA. Autologous periodontal ligament cells in the treatment of Class III furcation defects: a study in dogs. J Clin Periodontol. 2012;39(4): 377-84. [Medline: 21392047].

8-K. Fawzy-El-Sayed, M. Mekhemar, S. Adam-Klages, D. Kabelitz, and C. Dörfer, ―TlR expression profile of human gingival margin-derived stem progenitor cells ,‖ Medicina Oral, Patología Oral y Cirugía Bucal,2016. vol. 21, no. 1, pp. e30–e38.].

9- Rodríguez-Vázquez M, Ramos-ZúñigaR. Chitosan Hydroxyapatite Scaffold for Tissue Engineering in Experimental Lumbar Laminectomy and Posterolateral Spinal Fusion in Wistar Rats. Asian Spine J. 2019.

10- Boix D, Ganthier O, Guicheux J, et al. Alveolar bone regeneration for immediate implant placement using an injectable bone substitute: an experimental study in dogs. J Periodontol 2004; 75:663–671.

 11- Rose FR and Oreffo RO. Bone tissue engineering: hope vs hype.        Biochem Biophys Res Commun 2002; 292: 1-7

12- Fawzy El-Sayed KM, Paris S, Becker ST, Neuschl M, De Buhr W, Sälzer S, Wulff A, Elrefai M, Darhous MS, El-Masry M, Wiltfang J, Dörfer CE. Periodontal regeneration employing gingival margin derived stem/progenitor cells: an animal study. J Clin Periodontol 2012; 39: 861- 870.

13- Zhang J, Tu Q, Grosschedl R, Kim MS, Griffin T, Drissi H, Yang P and Chen J. Roles of SATB2 in osteogenic differentiation and bone regeneration. Tissue Eng Part A 2011; 17: 1767-17.

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