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XENOGRAFTS
Dr. Dandu Sivasai Prasad Reddy
II yr Post graduate
Department of Periodontics
Mamata Dental College
Dr. Dandu Sivasai Prasad Reddy
II yr Post graduate
Department of Periodontics
Mamata Dental College
Introduction
Terminologies
Bone graft
History
Mechanism of bone grafting
Clinical objectives of bone grafting for periodontal regeneration
Ideal properties of grafts
Indications of periodontal bone graft
CONTENTS
Classification of bone grafts
Xenografts
Calf bone
kiel bone
Anorganic bovine bone
Bio oss
Pepgen 15
Porcine derived bone graft
Osteobiol
Corrolline calcium carbonate
Combination procedures
Risk of disease transmission
Conclusion
References
INTRODUCTION
 Periodontal diseases
 Graft ????
TERMINOLOGY
Reattachment
New attachment
Periodontal repair
Periodontal regeneration
Regenerative therapy
Historically, bone grafting has consisted of:
A surgical procedure to harvest the patients own bone from a secondary site
Utilization of an organic or artificial material to replace missing bone
Structural scaffolds &
matrices for attachment &
proliferation of anchorage
dependent osteoblasts
Evolution
Bone grafting accomplished through
Formation and development of new bone by viable cells
contained in the graft
Eg: Autogenous graft
Provide a biologic stimulus (proteins and growth factors) that
induces the progression of mesenchymal stem cells and other
osteoprogenitor cells toward the osteoblast lineage
Eg: DFDBA
Is the process by which the graft material acts as a nonviable
scaffold onto and within which the patients own natural bone
grows
They allow apposition from existing bone, but do not produce
or trigger bone formation.
Eg Alloplastic material
OsteopromotionOsteopromotion
Osteopromotion involves the enhancement of
osteoinduction without the possession of osteoinductive
properties.
Clinical objectives of bone grafting for periodontal regeneration
     Probing depth reduction
     Clinical attachment gain
    Bone fill of the osseous defect and
   Regeneration of new bone, cementum and periodontal ligament as
determined by histologic analysis.
 
In a review of animal histologic studies, Mellonig found that 75% of these
studies indicated favorable regenerative results when periodontal
defects were treated with grafting; none showed that non-graft control
sites were superior to grafted ones.
 
 Non-toxic-Non-antigenic with patient acceptance
 Resistant to infection
 Facilitate vascularization
 No root resorption or ankylosis
 Strong and resistant
 Stimulates osteoinduction- & framework for osteoconduction
 Easily adaptable
 Readily and sufficiently available
 Minimal surgical procedure with minimal post-operative
sequelae
 Predictability
 Completely replaced by host bone of the same quality – quantity
 Induce & enhance cementogenesis.
CONTD..,CONTD..,
Indications of periodontal bone graft
1.Deep intraosseous defect
2.Tooth retention
3.Support for critical teeth
4.Defects associated with aggressive
periodontitis
5.Esthetics
6.Furcation
Classification
 Conge et al, 1978
 AAP 1986
 Carranza FA 1990
 Rosenberg& Rose 1998
 Nasr et al, 1999
 Resorption of the graft and replacement by new bone
depends upon
Particle size
Pore size
Xenografts
Source
 CALF BONE - treated by detergent, sterilized and freeze dried. Used for treatment
of osseous defects.
 KIEL BONE - Calf or Ox bone denaturated with 20% H2O2, dried with acetone, and
sterilized with ethylene oxide.
 ANORGANIC BONE - Ox bone from which the organic material has been extracted by
ethylene diamine. Then sterilized by autoclaving.
 Recently a natural, anorganic, microporous, bovine-derived hydroxyapatite bone
matrix, in combination with a cell-binding polypeptide that is a synthetic clone of 15
amino acid sequence of type I collagen is been used.
ANORGANIC BOVINE
BONE(ABB(
New processing and purification methods have been
utilized which make it possible to remove all organic
components from a bovine bone source and leaving
behind a non-organic bone matrix in an unchanged
inorganic form.
Commercially available
Bio – Oss
Bio – Oss Collagen
Pepgen-P15
Osteoconductive
Chemical & physical characteristics
similar to human mineral matrix
Porosity similar to human cancellous
bone
Large mesh interconnecting pore
system facilitates angiogenesis and
migration of osteoblasts.
Bio - Oss®
PACKAGING: 1. SPONGIOSA GRANULAT
Particle Size: 0.25 – 1mm
Quantity: 0.5, 2gms.
2. SPONGIOSA GRANULAT
Particle Size: 1 – 2mm
Quantity: 0.5, 2gms
 
3. SPONGIOSA BLOCK
Block 1x1x2 cm
 
4. BIO-OSS COLLAGEN
100mg Spongiosa Granulat + 10% Collagen
b
BIO-OSS CONTD..,
USES:
1. Treatment of defect sizes up to 2 alveoli, but can be used for
defect size larger than 2 alveoli.
2. Sinus floor elevations.
3. When combined with autogenous bone, it can be used for large
ridge augmentation.
BIO-OSS CONTD..,
Bio – Oss Collagen®
(Osteohealth Co., Shirley, NY)
Bio Oss spongiosa granules + 10% highly purified porcine collagen
Collagen component enables convenient handling to be easily
adapted in the defect but does not function as a barrier
Collagen component is resorbed within 4 – 6 weeks.
Studies
Stefano Sartori et al., analyse the amount of Bio-Oss
ossification in a case of maxillary sinus augmentation,
recording and comparing histomorphometric data 8 months, 2
and 10 years after surgery.
Eight months after surgery they observed a mean amount of bone tissue
(including medullar spaces) of 29.8% (and 70.2% of Bio-Oss) . At 2years the
bone tissue increased to 69.7% and 10years after surgery it was 86.7% .
Effect of low-level laser therapy irradiation and Bio-Oss graft
material on the osteogenesis process in rabbit calvarium defects:
a double blind experimental study- Alireza Rasouli et al., 2014
The mean amount of new bone was 15.83 and 18.5 % in the controls on the
4th and 8th week; 27.66 and 25.16 % in the laser-irradiated group; 35.0
and 41.83 % in Bio-Oss and 41.83 and 47.0 % in the laser + Bio-Oss
treated specimens with significant statistical differences. Application of
LLLT in combination with Bio-Oss can promote bone healing.
ABB plus P-15 cell binding
peptide
(pentadecapeptide)
Mimics the cell binding
domain of type I collagen
PepGen P-15
Hanadi Baeissa
Available forms
Clinical and radiographic evaluation of human periodontal
osseous defect (mandibular grade II furcation) treated with
PepGen P-15 and a bioresorbable membrane (Atrisorb)- 2012 KL
Vandana et.,al .
It can be concluded from this study that the reduction in furcation
defect using PepGen P-15 alone and a combination of PepGen P-15
and Atrisorb were equivocal. It can be suggested that the combined
use of GTR barrier and bone graft did not prove beneficial for the
clinical outcome of the mandibular grade II furcation defect
treatment. Hence, the cost effective and economical treatment of
choice for grade II furcation defects may be bone graft alone.
A Novel Combination Of Platelet Rich Fibrin And Pepgen P-15
Xenograft, In The Treatment Of Intrabony Defects: A Volumetric CT
Scan Analysis. 2013
At 6 and 9 month follow-up examination, it was observed that PD
reduced in range of 3 to 5 mm with 1 to 2 mm coronal shift in PGM and
again in CAL of 2 to 5 mm . A three-dimensional (3D) reconstructed
Dentascanimages acquired at 9 month interval, confirmed positive
changes in the defect morphology, with a linear bone growth of 1.5-
3mm( 33 to 37 %).The volumetric analysis showed a bone fill of 55 to
81% at the defect sites
Interdisciplinary Management of an Isolated Intrabony Defect- 2014
A 24 year male patient reported with the complaint of food lodgment and
occasional pain in relation to right lower first molar. Clinical examination
revealed deep periodontal pocket measuring 9mm on distal aspect of 46 and no 
mobility 
Treatment of Intrabony Defects with Anorganic Bone Matrix/P-15
or Guided Tissue Regeneration in Patients with Aggressive
Periodontitis -2013
Treatment of intrabony periodontal defects in patients with G-
AgP with ABM/P-15 and GTR improved significantly the clinical
outcomes. The use of ABM/P-15 promoted a better
radiographic bone fill.
Porcine derived bone graft:
Xenografts derived from porcine cortical and cancellous bone
have also been developed to be used as bone substitutes
OsteoBiol® It is a commercially available xenograft of porcine origin.
It is heterologous cortico cancellous collagenated bone mix. It always
be hydrated before use
Advantages:
It can act as a carrier for various therapeutic agents.
The collagen present in this bio material facilitates blood clotting
and the subsequent invasion of repairing and regenerative cells thus
favouring bone formation.
It also provides cohesive environment for graft particle.
Experimental Model of Bone Response to Collagenized Xenografts
of Porcine Origin (OsteoBiol® mp3): A Radiological and
Histomorphometric Study
After 4 months, radiological images revealed bone defects with
a decrease in graft volume and the complete repair of the
osseous defect.
The biomaterial used proved to be biocompatible,
bioabsorbable, and osteoconductive and as such, a possible
bone substitute that did not interfere with the bone’s normal
CORROLLINE CALCIUM CARBONATE
Biocoral is a calcium carbonate
Natural coral,
Primarily of aragonite.
It is biocompatible and resorbable
Porous size of 100-200um
Combination procedures
A combination of autogenous bone and bone substitute is widely used in
oral surgery procedures
Systematic review recommended a proportion of 1:2 (Merkx et al. 2003).
Pripatnanont et al. (2009) assessed new bone formation generated using
three different proportions of autogenous bone (AB) and deproteinized
bovine bone (BDX) in cortical skull defects in rabbits.
1:1 1:2 1:4
In deep intrabony defects treatment, at 12 months evaluation,
the combined use of autogenous spongiosa with bovine-derived
xenograft led to significantly greater gain of clinical attachment and
hard tissue formation compared to the use of autogenous
spongiosa alone
- (Zafiropoulos et al. 2007)
Efficacy of Using PDGF and Xenograft With or Without Collagen
Membrane for Bone Regeneration Around Immediate Implants
With Induced Dehiscence-Type Defects: A Microcomputed
Tomographic Study in Dogs- 2013
GBR around immediate implants with dehiscence defects using PDGF
and xenograft alone resulted in higher BBT, BBV, VBH, and BIC than
when performed in combination with CM.
A clinical and radiological evaluation of the relative efficacy of
demineralized freeze-dried bone allograft versus anorganic bovine bone
xenograft in the treatment of human infrabony periodontal defects: A 6
months follow-up study- 2014
The use of anorganic bovine bone mineral matrix combined with TGFβ-1
seemed to be effective in the treatment of intrabony defects. This showed an
improvement in the clinical outcome of periodontal therapy superior to the use
of anorganic bovine bone on its own.
Risk of transmission of prion mediated diseases – bovine
spongiform encephalopahty
In humans – Creutzfeldt – Jakob disease
WHO – bone as type IV (no transmission)for prion diseases
Segal and Tofe (1999) conducted an extensive review of current
literature on the status of risk assessment of BSE transmission the
risk of disease (BSE) transmission was negligible
Risk of diseasetransmission
CONCLUSION
Although complete periodontal regeneration is unpredictable with any
regenerative therapy currently used, periodontal bone grafts show strong
potential. Requirements for a successful graft includes Patient Selection,
material Selection, Proper Flap Reflection and Wound Stability,
Revascularization, Root Debridement, Postsurgical care .A large body of
clinical evidence clearly indicates that grafts consistently lead to better bone
fill than nongrafted controls. As more is learned about the biologic process of
periodontal regeneration, new graft materials are expected to make the task
of periodontal regeneration even more predictable.
REFERENCES
•Nasr HF, Reidy AME, Yukna RA. Bone and bone substitutes. Periodontology
2000, 1999; 19: 74-86.
•Carranza FA, Takei HH, Cochran DL. Chapter-67, Reconstructive Periodontal
Surgery. Carranza's Clinical Periodontology, 10th
edition: 968-969.
•Reynolds MA, Reidy AME, Branch-May GL, Gunsolley JC. The efficacy of bone
replacement grafts in the treatment of periodontal osseous defects. Ann
Periodontol 2003; 8(1): 227-265.
•Dental & Medical Device. Product information on Osteo-Biol ®, 2008.
•Dentsply-Friadent. Product information on PepGen P-15®, 2008.
•Rita Singh, Lanka Mahesh. Infections Resulting from Bone Grafting Biomaterials.
International Journal of Oral Implantology and Clinical Research, May-August
2013;4(2):68-71
•A.L. Dumitrescu, Chemicals in Surgical Periodontal Therapy, Bone Grafts and
Bone Graft Substitutes in Periodontal Therapy.
•Emmings et al. Chemically modified osseous material for restoration of bone
defects. J Periodontol 1974; 45:385.
•Boyne et al. Transplantation, implantation and grafts. Dent Clin N Am 1971; 15:
434.
•Krejci et al. Osseous grafting in periodontal therapy. Part I - Osseous graft
material. Comp. Cont. Edu. Dent. VIII 1987, No.10.
Thank you.,

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XENOGRAFTS IN DENTISTRY

  • 1. XENOGRAFTS Dr. Dandu Sivasai Prasad Reddy II yr Post graduate Department of Periodontics Mamata Dental College Dr. Dandu Sivasai Prasad Reddy II yr Post graduate Department of Periodontics Mamata Dental College
  • 2. Introduction Terminologies Bone graft History Mechanism of bone grafting Clinical objectives of bone grafting for periodontal regeneration Ideal properties of grafts Indications of periodontal bone graft CONTENTS
  • 3. Classification of bone grafts Xenografts Calf bone kiel bone Anorganic bovine bone Bio oss Pepgen 15 Porcine derived bone graft Osteobiol
  • 4. Corrolline calcium carbonate Combination procedures Risk of disease transmission Conclusion References
  • 7. Historically, bone grafting has consisted of: A surgical procedure to harvest the patients own bone from a secondary site Utilization of an organic or artificial material to replace missing bone Structural scaffolds & matrices for attachment & proliferation of anchorage dependent osteoblasts
  • 10. Formation and development of new bone by viable cells contained in the graft Eg: Autogenous graft
  • 11. Provide a biologic stimulus (proteins and growth factors) that induces the progression of mesenchymal stem cells and other osteoprogenitor cells toward the osteoblast lineage Eg: DFDBA
  • 12. Is the process by which the graft material acts as a nonviable scaffold onto and within which the patients own natural bone grows They allow apposition from existing bone, but do not produce or trigger bone formation. Eg Alloplastic material
  • 13. OsteopromotionOsteopromotion Osteopromotion involves the enhancement of osteoinduction without the possession of osteoinductive properties.
  • 14. Clinical objectives of bone grafting for periodontal regeneration      Probing depth reduction      Clinical attachment gain     Bone fill of the osseous defect and    Regeneration of new bone, cementum and periodontal ligament as determined by histologic analysis.   In a review of animal histologic studies, Mellonig found that 75% of these studies indicated favorable regenerative results when periodontal defects were treated with grafting; none showed that non-graft control sites were superior to grafted ones.  
  • 15.  Non-toxic-Non-antigenic with patient acceptance  Resistant to infection  Facilitate vascularization  No root resorption or ankylosis  Strong and resistant  Stimulates osteoinduction- & framework for osteoconduction  Easily adaptable
  • 16.  Readily and sufficiently available  Minimal surgical procedure with minimal post-operative sequelae  Predictability  Completely replaced by host bone of the same quality – quantity  Induce & enhance cementogenesis. CONTD..,CONTD..,
  • 17. Indications of periodontal bone graft 1.Deep intraosseous defect 2.Tooth retention 3.Support for critical teeth 4.Defects associated with aggressive periodontitis 5.Esthetics 6.Furcation
  • 18. Classification  Conge et al, 1978  AAP 1986  Carranza FA 1990  Rosenberg& Rose 1998  Nasr et al, 1999
  • 19.  Resorption of the graft and replacement by new bone depends upon Particle size Pore size
  • 21.  CALF BONE - treated by detergent, sterilized and freeze dried. Used for treatment of osseous defects.  KIEL BONE - Calf or Ox bone denaturated with 20% H2O2, dried with acetone, and sterilized with ethylene oxide.  ANORGANIC BONE - Ox bone from which the organic material has been extracted by ethylene diamine. Then sterilized by autoclaving.  Recently a natural, anorganic, microporous, bovine-derived hydroxyapatite bone matrix, in combination with a cell-binding polypeptide that is a synthetic clone of 15 amino acid sequence of type I collagen is been used.
  • 22. ANORGANIC BOVINE BONE(ABB( New processing and purification methods have been utilized which make it possible to remove all organic components from a bovine bone source and leaving behind a non-organic bone matrix in an unchanged inorganic form. Commercially available Bio – Oss Bio – Oss Collagen Pepgen-P15
  • 23. Osteoconductive Chemical & physical characteristics similar to human mineral matrix Porosity similar to human cancellous bone Large mesh interconnecting pore system facilitates angiogenesis and migration of osteoblasts. Bio - Oss®
  • 24. PACKAGING: 1. SPONGIOSA GRANULAT Particle Size: 0.25 – 1mm Quantity: 0.5, 2gms. 2. SPONGIOSA GRANULAT Particle Size: 1 – 2mm Quantity: 0.5, 2gms   3. SPONGIOSA BLOCK Block 1x1x2 cm   4. BIO-OSS COLLAGEN 100mg Spongiosa Granulat + 10% Collagen b BIO-OSS CONTD..,
  • 25. USES: 1. Treatment of defect sizes up to 2 alveoli, but can be used for defect size larger than 2 alveoli. 2. Sinus floor elevations. 3. When combined with autogenous bone, it can be used for large ridge augmentation. BIO-OSS CONTD..,
  • 26. Bio – Oss Collagen® (Osteohealth Co., Shirley, NY) Bio Oss spongiosa granules + 10% highly purified porcine collagen Collagen component enables convenient handling to be easily adapted in the defect but does not function as a barrier Collagen component is resorbed within 4 – 6 weeks.
  • 27. Studies Stefano Sartori et al., analyse the amount of Bio-Oss ossification in a case of maxillary sinus augmentation, recording and comparing histomorphometric data 8 months, 2 and 10 years after surgery. Eight months after surgery they observed a mean amount of bone tissue (including medullar spaces) of 29.8% (and 70.2% of Bio-Oss) . At 2years the bone tissue increased to 69.7% and 10years after surgery it was 86.7% .
  • 28. Effect of low-level laser therapy irradiation and Bio-Oss graft material on the osteogenesis process in rabbit calvarium defects: a double blind experimental study- Alireza Rasouli et al., 2014 The mean amount of new bone was 15.83 and 18.5 % in the controls on the 4th and 8th week; 27.66 and 25.16 % in the laser-irradiated group; 35.0 and 41.83 % in Bio-Oss and 41.83 and 47.0 % in the laser + Bio-Oss treated specimens with significant statistical differences. Application of LLLT in combination with Bio-Oss can promote bone healing.
  • 29. ABB plus P-15 cell binding peptide (pentadecapeptide) Mimics the cell binding domain of type I collagen PepGen P-15
  • 31. Clinical and radiographic evaluation of human periodontal osseous defect (mandibular grade II furcation) treated with PepGen P-15 and a bioresorbable membrane (Atrisorb)- 2012 KL Vandana et.,al . It can be concluded from this study that the reduction in furcation defect using PepGen P-15 alone and a combination of PepGen P-15 and Atrisorb were equivocal. It can be suggested that the combined use of GTR barrier and bone graft did not prove beneficial for the clinical outcome of the mandibular grade II furcation defect treatment. Hence, the cost effective and economical treatment of choice for grade II furcation defects may be bone graft alone.
  • 32. A Novel Combination Of Platelet Rich Fibrin And Pepgen P-15 Xenograft, In The Treatment Of Intrabony Defects: A Volumetric CT Scan Analysis. 2013 At 6 and 9 month follow-up examination, it was observed that PD reduced in range of 3 to 5 mm with 1 to 2 mm coronal shift in PGM and again in CAL of 2 to 5 mm . A three-dimensional (3D) reconstructed Dentascanimages acquired at 9 month interval, confirmed positive changes in the defect morphology, with a linear bone growth of 1.5- 3mm( 33 to 37 %).The volumetric analysis showed a bone fill of 55 to 81% at the defect sites
  • 33. Interdisciplinary Management of an Isolated Intrabony Defect- 2014 A 24 year male patient reported with the complaint of food lodgment and occasional pain in relation to right lower first molar. Clinical examination revealed deep periodontal pocket measuring 9mm on distal aspect of 46 and no  mobility 
  • 34. Treatment of Intrabony Defects with Anorganic Bone Matrix/P-15 or Guided Tissue Regeneration in Patients with Aggressive Periodontitis -2013 Treatment of intrabony periodontal defects in patients with G- AgP with ABM/P-15 and GTR improved significantly the clinical outcomes. The use of ABM/P-15 promoted a better radiographic bone fill.
  • 35. Porcine derived bone graft: Xenografts derived from porcine cortical and cancellous bone have also been developed to be used as bone substitutes OsteoBiol® It is a commercially available xenograft of porcine origin. It is heterologous cortico cancellous collagenated bone mix. It always be hydrated before use
  • 36. Advantages: It can act as a carrier for various therapeutic agents. The collagen present in this bio material facilitates blood clotting and the subsequent invasion of repairing and regenerative cells thus favouring bone formation. It also provides cohesive environment for graft particle.
  • 37. Experimental Model of Bone Response to Collagenized Xenografts of Porcine Origin (OsteoBiol® mp3): A Radiological and Histomorphometric Study After 4 months, radiological images revealed bone defects with a decrease in graft volume and the complete repair of the osseous defect. The biomaterial used proved to be biocompatible, bioabsorbable, and osteoconductive and as such, a possible bone substitute that did not interfere with the bone’s normal
  • 38. CORROLLINE CALCIUM CARBONATE Biocoral is a calcium carbonate Natural coral, Primarily of aragonite. It is biocompatible and resorbable Porous size of 100-200um
  • 39. Combination procedures A combination of autogenous bone and bone substitute is widely used in oral surgery procedures Systematic review recommended a proportion of 1:2 (Merkx et al. 2003). Pripatnanont et al. (2009) assessed new bone formation generated using three different proportions of autogenous bone (AB) and deproteinized bovine bone (BDX) in cortical skull defects in rabbits. 1:1 1:2 1:4
  • 40. In deep intrabony defects treatment, at 12 months evaluation, the combined use of autogenous spongiosa with bovine-derived xenograft led to significantly greater gain of clinical attachment and hard tissue formation compared to the use of autogenous spongiosa alone - (Zafiropoulos et al. 2007)
  • 41. Efficacy of Using PDGF and Xenograft With or Without Collagen Membrane for Bone Regeneration Around Immediate Implants With Induced Dehiscence-Type Defects: A Microcomputed Tomographic Study in Dogs- 2013 GBR around immediate implants with dehiscence defects using PDGF and xenograft alone resulted in higher BBT, BBV, VBH, and BIC than when performed in combination with CM.
  • 42. A clinical and radiological evaluation of the relative efficacy of demineralized freeze-dried bone allograft versus anorganic bovine bone xenograft in the treatment of human infrabony periodontal defects: A 6 months follow-up study- 2014 The use of anorganic bovine bone mineral matrix combined with TGFβ-1 seemed to be effective in the treatment of intrabony defects. This showed an improvement in the clinical outcome of periodontal therapy superior to the use of anorganic bovine bone on its own.
  • 43. Risk of transmission of prion mediated diseases – bovine spongiform encephalopahty In humans – Creutzfeldt – Jakob disease WHO – bone as type IV (no transmission)for prion diseases Segal and Tofe (1999) conducted an extensive review of current literature on the status of risk assessment of BSE transmission the risk of disease (BSE) transmission was negligible Risk of diseasetransmission
  • 44.
  • 45. CONCLUSION Although complete periodontal regeneration is unpredictable with any regenerative therapy currently used, periodontal bone grafts show strong potential. Requirements for a successful graft includes Patient Selection, material Selection, Proper Flap Reflection and Wound Stability, Revascularization, Root Debridement, Postsurgical care .A large body of clinical evidence clearly indicates that grafts consistently lead to better bone fill than nongrafted controls. As more is learned about the biologic process of periodontal regeneration, new graft materials are expected to make the task of periodontal regeneration even more predictable.
  • 46. REFERENCES •Nasr HF, Reidy AME, Yukna RA. Bone and bone substitutes. Periodontology 2000, 1999; 19: 74-86. •Carranza FA, Takei HH, Cochran DL. Chapter-67, Reconstructive Periodontal Surgery. Carranza's Clinical Periodontology, 10th edition: 968-969. •Reynolds MA, Reidy AME, Branch-May GL, Gunsolley JC. The efficacy of bone replacement grafts in the treatment of periodontal osseous defects. Ann Periodontol 2003; 8(1): 227-265. •Dental & Medical Device. Product information on Osteo-Biol ®, 2008. •Dentsply-Friadent. Product information on PepGen P-15®, 2008.
  • 47. •Rita Singh, Lanka Mahesh. Infections Resulting from Bone Grafting Biomaterials. International Journal of Oral Implantology and Clinical Research, May-August 2013;4(2):68-71 •A.L. Dumitrescu, Chemicals in Surgical Periodontal Therapy, Bone Grafts and Bone Graft Substitutes in Periodontal Therapy. •Emmings et al. Chemically modified osseous material for restoration of bone defects. J Periodontol 1974; 45:385. •Boyne et al. Transplantation, implantation and grafts. Dent Clin N Am 1971; 15: 434. •Krejci et al. Osseous grafting in periodontal therapy. Part I - Osseous graft material. Comp. Cont. Edu. Dent. VIII 1987, No.10.

Notas do Editor

  1. . It is thoroughly mixed with few drops of sterile physiologic solution to activate collagen matrix and to enhance its adhesivity. It can also be mixed with osteoBiol gel or with patients blood.