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Bone Grafting and Bone Graft 
Substitutes 
Dr. Gurvinder Singh 
Dr. Siddharth Gupta 
Residents UCMS & GTB, HOSPITAL ,DELHI
Bone Graft Uses 
• To fill cavities or defects resulting from cysts, tumors, 
or other cause 
• To bridge joints and provide arthrodesis 
• To bridge major defects or establish the continuity 
of a long bone 
• To provide bone blocks to limit joint motion 
(arthroereisis) 
• To establish union in a pseudarthrosis 
• To promote union or fill defects in delayed union, 
malunion, fresh fractures, or osteotomies
s
Mesenchymal Stem cells 
• Progenitor cells that provide a source of cells 
to differentiate into chondroblasts and 
osteoblasts during endochondral and 
intramembranous bone formation 
• In the elderly the pool of these cells 
diminishes 
• Bone marrow is the source of adult MSCs
Types of Bone Grafts:on the basis 
of source 
• Autogenous: source is the patient , usually 
from tibia , fibula or ilium. Also rib 
• Allogenic : source is an individual other than 
the patient 
• Xenograft: derived from different species
Properties of auto and allografts
Autogenous Bone Graft 
• “Gold standard” 
• May provide osteoconduction, osteoinduction 
and osteogenesis 
• Drawbacks 
– Limited supply 
– Donor site pain, haematoma, neuromas , fracture 
and heterotopic bone formation
Autogenous Bone Grafts 
• Cancellous 
• Cortical 
• Free vascular transfers 
• Muscle pedicle bone graft 
• Bone marrow aspirate
Autogenous Cancellous Bone 
Grafts 
• Three dimensional scaffold 
(osteoconductive) 
• Osteocytes and stem cells (osteogenic) 
• A small quantity of growth factors 
(osteoinductive)ss 
• CREEPING SUBSTITUION: process by which 
graft is replaced by new bone (I year) 
• Used in boneloss: depressed tibial plateau 
fractures, revision hip and knee arthroplasty
Creeping Substituition 
• Creeping substitution, the process of bone 
remodeling by osteoclastic resorption and 
creation of new vascular channels with 
osteoblastic bone formation resulting in new 
haversian systems, is the method by which 
strong cortical bone is formed from grafted 
material.
Autogenous Cortical Bone Grafts 
Sources: 
• Ribs 
• Fibula 
• Crest of the ilium (also called as tricortical graft) 
• It can be of two types: 
• Conventinal nov vascular 
• Vascularised bone graft
Non vascular versus vascular bone 
graft 
Non vascular 
• Mainly osteoconductive 
with littile 
osteoinductive and no 
osteogenic properties. 
• Revascularisation is 
slow till cortex is 
resorbed. 
• Remodelling -2years 
• Used in defects <6cm 
Vascular 
• It has immediately 
restored blood 
supply 
• More viable, more 
survival of osteocytes 
• Can be used in 
defects upto 12 cm 
or even in 
inadequate host.
Bone Marrow Aspirate 
• RIA(REAMER IRRIGATOR AND ASPIRATOR) 
• It is a technique to harvest sizable amount of 
bone marrow,which is particularly rich in 
mesenchymal stem cells . 
• Growth factors supplied: 
Fibroblasts growth factor(FGF)-2 
Insulin like growth factor(IGF)-2 
Transforming growth factor(TGF) beta 
Absence of bone morphogenetic protein-2
Advantages of RIA 
• Provides enriched osteogenesis 
• Decrease intramedullary canal pressure 
• Minimal risk of fat embolism 
• Potential source of autologous bone, 
mesenchymal cells and bone growth factors.
s
Complications of RIA 
• Perforation of the meduallary canal which 
may require prophylactic intramedullary 
fixation. 
• Significant blood loss
Steps to minimize risks 
• Preoperatively donor radigraph should be 
used to measure isthmus 
• Blood should be arranged for replacement. 
• Switch off the aspirator when there is no 
reaming 
• Postp of ambulation should be protective 
• Check haematocrit 
• Avoid in metabolic bone diseases
Wolfe kawamatto technique
Complications of iliac crest graft 
• Full thickness iliac crest graft lead to 
herniation. 
• The lateral femoral cutaneous and ilioinguinal 
nerves are at risk during harvest of bone from 
the anterior ilium 
• Alter the contour of the anterior crest, 
producing significant cosmetic deformity 
• Arteriovenous fistula, pseudoaneurysm, 
ureteral injury, anterior superior iliac spine 
avulsion, and pelvic instability
Iliac crest graft
Grafts from tibia 
• The subcutaneous anteromedial aspect of 
tibia is the source of structural autografts. 
• The plateau of tibia supplies cancellous bone.
Tibial graft harvest
Disadvantages of tibial graft 
 Normal limb is jeopardized 
 Increased duration of surgery 
 Protected weight bearing for atleast 6 to 12 
months .
Bone graft from fibula 
• Entire proximal two third of the fibula can be 
used for bone graft 
• The proximal rounded configuration of the 
fibula is covered with hyaline cartilage. 
• May replace distal radius or even distal third 
of fibula 
• The middle third of fibula can serve as the 
peroneal artery based vascular graft
Points to remember for fibular 
bone graft 
• The peroneal nerve must not be damaged; 
• The distal fourth of the bone must be left to 
maintain a stable ankle 
• The peroneal muscles should not be cut.
Phemister bone graft 
• It is subcortical cancellous bone grafting 
• A bone graft of cortical bone with cancellous 
bone chips to enhance callus formation. 
• Bone-grafting without disturbing the pre-existing 
callus 
• Bone graft is taken by elevating the 
osteoperiosteal flaps.
Requisites for phemister graft 
• Petalling should carried out at the fracture site 
• The mobility at the fracture site should be 
minimal 
• The fracture should have an acceptable 
alignment 
• The knee joint should have a good range of 
motion
Urist AAA bone graft 
• Composed of bone morphogenic protein and 
autolysed , antigen-extracted and autogenic 
bone. 
• h-BMP/AAA composite implants represent 
adjunctive treatment of difficult nonunions 
• Composite implants may be implanted in 
either partial or complete segmental defects 
of long bones
Allograft 
The morbidity and limited amount of autogenic 
bone graft calls for a need of allogenic bone 
Graft. 
They are indicated in 
1.Children 2. Elderly 3.Poor surgical risk 
4.Enough graft cannot be harvested
Allograft types 
Cortical 
• Frozen 
• Freeze dried 
Cancellous 
• Frozen 
• Freeze dried
Bone Allografts 
• Cancellous or cortical 
– Plentiful supply 
– Limited infection risk (varies based on processing 
method) 
– Provide osteoconductive scaffold 
– May provide structural support
Bone Allografts 
• Freeze-dried 
– Even less antigenic 
– Time to test for diseases 
– Strictly regulated by FDA 
– Can be stored at room temperature up to 5 years 
– Mechanical properties degrade
Bone Bank 
• It is a facilitiy to provide safe and efficient 
allograft material. 
• Hosts should be screened for : 
infections,malignancies(except for basal cell 
carcinoma of the skin), collagen vascular 
diseases, metabolic bone diseases and 
presence of toxins.
Technique 
• Bone is collected in clean and unsterile 
environment. 
• It is nibbled to remove the articular cartilage. 
• It can be sterilized by irradiation, ethylene 
oxide or strong acid( 0.55 % HCl) 
• It is subject to deep freeze upto -70 to -80 
degrees celcius(frozen) 
• Freeze drying involves removal of water and 
vacuum packaging of the tissue
Freeze dried bone graft 
• Decreases expression of MHC 1 complex in 
osteoblasts 
• Decreased osteoinductive properties 
• Reduced mechanical integrity 
• Decreased number of viable cells 
• Slow revascularisation and delaye remodelling 
• Histologically mono nuclear cells surround the 
newly developed blood vessels
Demineralized Bone Matrix 
• Prepared from cadaveric human bone 
• Acid extraction of bone leaving 
– Collagen(type 1) 
– Noncollagenous proteins 
– Bone growth factors 
• BMP quantity extremely low and variable 
• Sterilized which may decrease the availability of BMP
Demineralized Bone Matrix 
• Available from multiple vendors in multiple 
preparations 
– Gel 
– Putty 
– Strip 
– Combination products with cancellous bone and 
other bone graft substitute products
Demineralized Bone Matrix 
• Growth factor activity varies between tissue 
banks and between batches 
• While they may offer some osteoinductive 
potential because of available growth factors, 
they mainly act as an osteoconductive agents 
Han B et al. J Orthop Res. 21(4):648-54, 2003. 
Blum B, et al. Orthopedics. 27 (1 Suppl): S161 – S165, 2004.
Graft Incorporation 
• Hematoma formation 
– Release of cytokines and growth factors
Graft Incorporation 
• Hematoma formation 
– Release of cytokines and growth factors 
• Inflammation 
– Development of fibrovascular tissue (18 hours)
Graft Incorporation 
• Hematoma formation 
– Release of cytokines and growth factors 
• Inflammation 
– Development of fibrovascular tissue 
• Vascular ingrowth 
– Often extending Haversian canals
Graft Incorporation 
• Hematoma formation 
– Release of cytokines and growth factors 
• Inflammation 
– Development of fibrovascular tissue(18 hours) 
• Vascular ingrowth 
– Often extending Haversian canals (10 -12 days) 
• Focal osteoclastic resorption of graft
Graft Incorporation 
• Hematoma formation 
– Release of cytokines and growth factors 
• Inflammation 
– Development of fibrovascular tissue 
• Vascular ingrowth 
– Often extending Haversian canals 
• Focal osteoclastic resorption of graft 
• Intramembranous and/or endochondral bone 
formation on graft surfaces…….
Graft Incorporation 
• Cortical allograft strut 
graft placed next to 
cortex of host 
• After 4 years of 
incorporation
Bone Graft Substitutes 
• Need for bone graft alternatives has lead to 
development of numerous bone graft substitutes 
• Avoid morbidity of autogenous bone graft harvest 
• Mechanical properties vary 
• Most offer osteoconductive properties 
• Some provide osteoinductive properties
Bone Graft Substitutes 
Potential Roles 
• Extender for autogenous bone graft 
– Large defects 
– Multiple level spinal fusion 
• Enhancer 
– To improve success of autogenous bone graft 
• Substitute 
– To replace autogenous bone graft
Properties of bone graft 
substitutes
Classification
Laurencin et al, classification 
• Allograft based 
• Factor based 
• Cell based 
• Ceramic based 
• Polymer based 
• Composite
Ideal bone graft substitute 
• Scaffolding for osteoconduction 
• Growth factors for osteoinduction 
• Progenitor cells for osteogenesis 
• Biocompatible and biodegradable and 
mechanical properties similar to the 
surrounding bone 
• Each substitute available nowadays fulfill only 
some of the criteria
Bone Graft Substitutes 
• Resorption rates vary widely 
– Dependant on composition 
• Calcium sulfate - very rapid 
• Hydroxyapatite (HA) – very, very slow 
• Some products may be combined to optimize 
resorption rate 
– Also dependant on porosity, geometry
Bone Graft Substitutes 
• Mechanical properties vary widely 
– Dependant on composition 
• Calcium phosphate cement has highest compressive 
strength 
• Cancellous bone compressive strength is relatively low 
• Many substitutes have compressive strengths similar to 
cancellous bone 
• All designed to be used with internal fixation
Allograft based 
• Includes allograft bone used alone or in 
combination with other materials 
• Available as demineralised bone matrix
Factor based 
• Involves natural or recombinant factors 
• Factors responsible for differentiation of 
progenitor cells and regulation of activities 
• Mechanism of action: based mostly on 
activation of protein kinase 
• Combined and simultaneous activity of 
various factors controlled resorption and 
formation of new bone
• Factor + receptors on the cell surface 
• Activation of protein kinase 
• Transcription of mRNA 
• Protein synthesis 
• Regulation of cell activities
• Includes TGF-beta, IGF-I&II,PDGF,FGF and 
BMPs 
• Mostly in research phase 
• Recombinant BMP-2 as INFUSE bone graft
Bone Morphogenic Proteins
BMP 2 and 7 
BMP 2 
• Acts as a disulfide 
linked homodimer 
and helps in bone 
and cartilage 
formation 
• It is a candidate as 
retinoid mediator 
and helps 
osteoblastic 
differentiation 
BMP 7 
• It plays a key role in 
osteoblastic 
differentiation 
• It induces the 
prodution of SMAD 1 
• It plays a key role in 
renal development 
and repair
Bone Morphogenetic Proteins 
• Produced by recombinant technology 
• Two most extensively studied and 
commercially available 
– BMP-2 (Infuse) Medtronics 
– BMP-7 (OP-1)Stryker ss 
– BMP-2 and BMP-7 are water soluble and 
require a carrier to remain in the operative 
area to be effective
BMP-2 for Open Tibial Fractures 
• Prospective, randomized 
study 
• 450 patients 
· All received IM nail (vast 
majority with UNREAMED 
technique) and appropriate 
soft tissue management 
· Randomized to 3 treatments at 
time of definitive wound 
closure 
· Placebo 
· 0.75 mg/ml BMP-2/ACS 
· 1.50 mg/ml BMP-2/ACS 
BESTT Study Group, et al. J Bone Joint Surg 84A: 2123, 2002.
Results 
• 44% reduction in risk of 
nonunion/delayed union with 
high dose BMP-2 
• Significantly faster fracture 
healing 
• Significantly fewer 
– invasive interventions 
– hardware failures 
– infections 
BESTT Study Group, et al. J Bone Joint Surg 84A: 2123, 2002.
Cell Based 
• Based on in vitro differentiation of 
mesenchymal stem cells to osteoblastic 
lineage 
• They have been used along with ceramics 
• Proposed to be used in bone repair prosthetic 
setting
Ceramic based 
• About 60% BGS involves ceramics- alone or in 
combination 
• Eg : calcium sulfate, calcium phosphate, 
bioactive glass 
• Primary inorganic componet is calcium 
hyroxyapatite 
• Property of osteointegration, newly formed 
mineralised tissue forms intimate bond with 
implant materials
Calcium Phosphate Ceramics 
• Enable osteoconduction but use is limited 
due to poor tensile strength and brittleness 
• Injectable pastes of calcium and phospate 
– Norian SRS (Synthes/Stratec) 
– Alpha BSM (Etex/Depuy) 
– Callos Bone Void Filler (Skeletal Kinetics)
Calcium Phosphat 
Ceramics 
• It is produced by the process of 
Sintering(heating over 1000degrees C) 
• Injectable 
• Very high compressive strength once 
hardens 
• Some studies of its use have allowed 
earlier weightbearing and range of 
motion
Calcium 
Sulfate(plaster of 
paris) 
· Osteoconductive void filler 
· Low compressive strength – no structural 
support 
· Rapidly and complete resorption 
· May be used as a autogenous graft extender 
- Available from numerous companies 
- Osteoset, Calceon 6, Bone Blast, etc.
Calcium Sulfate 
• Pellets 
– Pellet injectors 
• Bead kits 
– Allows addition of 
antibiotics 
• Injectable 
– May be used to augment 
screw purchase 
• Combination of DMB and 
calcium sulfate
Hydroxyapatite(HA) 
• It is a slowly resorbing compound of calcium 
phosphate 
• Source :synthetic and animal 
• Hydrothermal process converts it from its 
native coral form to more stable HA form with 
pore diameters between 200 to 400 micron
Hydroxyapatite 
• Interconnected porous 
structure closely resembles the 
porosity of human cancellous 
bone 
Cancellous Bone 
Coralline hydroxyapatite
Hydroxyapatite 
• Interpore(Interpore International, Irvine,CA):first 
calcium phosphate based BGS approved by FDA 
• Marketed as ProOsteon by Interpore Cross 
• Available in various size blocks & granules 
• ProOsteon 500 
– Very slow resorption 
• ProOsteon 500 R 
– Only a thin layer of HA 
– Faster resorption
Hydroxyapatite:indications 
• Valgus instability following lateral tibial 
plateau fracture 
• Varus instability following medial condyle 
fracture of tibia 
• Articular incongruence of 10 mm or more 
• Translation of major condylar fragment of 
more than 5mm
Tricalcium Phosphate(TCP) 
• TCP composition is similar to calcium and 
phosphate phase of human bone and has 
porous nature 
• TCP undergoes partial resorption and some of 
it may be converted to HA once implanted in 
the human body 
• Complete resorption at 6 months
Tricalcium Phosphate 
• Wet compressive strength slightly less than 
cancellous bone 
• Available as blocks, wedges, and granules 
• Numerous tradenames 
– Vitoss (Orthovita) 
– ChronOS (Synthes) 
– Conduit (DePuy) 
– Cellplex TCP (Wright Medical) 
– Various Theri__ names (Therics)
Calcium Phosphate Cements(CPC) 
• CPC is used as void filler in defects 
• It consists of inorganic calcium and phosphate 
combined to form an injectable paste
Polymer based 
• Can be divided: natural/synthetic 
• Further divided into: biodegradable/non 
biodegradable 
• eg: Healoss(depuy)-natural 
• Eg :Cortoss- injectable resin based product 
• Eg : Rhakoss(Orthovita)
Collagen Based Matrices 
• Highly purified Type 1 bovine 
dermal fibrillar collagen 
• Bone marrow is added to 
provide bone forming cells 
• Collagraft (Zimmer) 
– Collagen / HA / Tricalcium 
phosphate 
• Healos (Depuy) 
– Collagen / HA
Composite graft 
• In this two or more type of bone graft 
substitutes combined together 
• So that osteoconductive and osteoinductive 
properties of different BGS, is combined
Calcium Phosphate-Collagen 
Composite 
• Collagen provides binding sites for matrix 
proteins 
• Type I and III is added to HA,TCP and 
autologous bone marrow to form a graft 
material 
• Although no structural support but augments 
frature healing
Bone Graft Substitute Incorporation 
• Partial incorporation of 
hydroxyapatite bone 
graft substitute 
• Biopsy of material 
obtained 1 year post-op

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Bone Grafting and Substitutes Guide

  • 1. Bone Grafting and Bone Graft Substitutes Dr. Gurvinder Singh Dr. Siddharth Gupta Residents UCMS & GTB, HOSPITAL ,DELHI
  • 2. Bone Graft Uses • To fill cavities or defects resulting from cysts, tumors, or other cause • To bridge joints and provide arthrodesis • To bridge major defects or establish the continuity of a long bone • To provide bone blocks to limit joint motion (arthroereisis) • To establish union in a pseudarthrosis • To promote union or fill defects in delayed union, malunion, fresh fractures, or osteotomies
  • 3. s
  • 4. Mesenchymal Stem cells • Progenitor cells that provide a source of cells to differentiate into chondroblasts and osteoblasts during endochondral and intramembranous bone formation • In the elderly the pool of these cells diminishes • Bone marrow is the source of adult MSCs
  • 5. Types of Bone Grafts:on the basis of source • Autogenous: source is the patient , usually from tibia , fibula or ilium. Also rib • Allogenic : source is an individual other than the patient • Xenograft: derived from different species
  • 6. Properties of auto and allografts
  • 7. Autogenous Bone Graft • “Gold standard” • May provide osteoconduction, osteoinduction and osteogenesis • Drawbacks – Limited supply – Donor site pain, haematoma, neuromas , fracture and heterotopic bone formation
  • 8. Autogenous Bone Grafts • Cancellous • Cortical • Free vascular transfers • Muscle pedicle bone graft • Bone marrow aspirate
  • 9. Autogenous Cancellous Bone Grafts • Three dimensional scaffold (osteoconductive) • Osteocytes and stem cells (osteogenic) • A small quantity of growth factors (osteoinductive)ss • CREEPING SUBSTITUION: process by which graft is replaced by new bone (I year) • Used in boneloss: depressed tibial plateau fractures, revision hip and knee arthroplasty
  • 10. Creeping Substituition • Creeping substitution, the process of bone remodeling by osteoclastic resorption and creation of new vascular channels with osteoblastic bone formation resulting in new haversian systems, is the method by which strong cortical bone is formed from grafted material.
  • 11. Autogenous Cortical Bone Grafts Sources: • Ribs • Fibula • Crest of the ilium (also called as tricortical graft) • It can be of two types: • Conventinal nov vascular • Vascularised bone graft
  • 12. Non vascular versus vascular bone graft Non vascular • Mainly osteoconductive with littile osteoinductive and no osteogenic properties. • Revascularisation is slow till cortex is resorbed. • Remodelling -2years • Used in defects <6cm Vascular • It has immediately restored blood supply • More viable, more survival of osteocytes • Can be used in defects upto 12 cm or even in inadequate host.
  • 13. Bone Marrow Aspirate • RIA(REAMER IRRIGATOR AND ASPIRATOR) • It is a technique to harvest sizable amount of bone marrow,which is particularly rich in mesenchymal stem cells . • Growth factors supplied: Fibroblasts growth factor(FGF)-2 Insulin like growth factor(IGF)-2 Transforming growth factor(TGF) beta Absence of bone morphogenetic protein-2
  • 14. Advantages of RIA • Provides enriched osteogenesis • Decrease intramedullary canal pressure • Minimal risk of fat embolism • Potential source of autologous bone, mesenchymal cells and bone growth factors.
  • 15.
  • 16.
  • 17. s
  • 18. Complications of RIA • Perforation of the meduallary canal which may require prophylactic intramedullary fixation. • Significant blood loss
  • 19. Steps to minimize risks • Preoperatively donor radigraph should be used to measure isthmus • Blood should be arranged for replacement. • Switch off the aspirator when there is no reaming • Postp of ambulation should be protective • Check haematocrit • Avoid in metabolic bone diseases
  • 21. Complications of iliac crest graft • Full thickness iliac crest graft lead to herniation. • The lateral femoral cutaneous and ilioinguinal nerves are at risk during harvest of bone from the anterior ilium • Alter the contour of the anterior crest, producing significant cosmetic deformity • Arteriovenous fistula, pseudoaneurysm, ureteral injury, anterior superior iliac spine avulsion, and pelvic instability
  • 22.
  • 24. Grafts from tibia • The subcutaneous anteromedial aspect of tibia is the source of structural autografts. • The plateau of tibia supplies cancellous bone.
  • 26. Disadvantages of tibial graft  Normal limb is jeopardized  Increased duration of surgery  Protected weight bearing for atleast 6 to 12 months .
  • 27. Bone graft from fibula • Entire proximal two third of the fibula can be used for bone graft • The proximal rounded configuration of the fibula is covered with hyaline cartilage. • May replace distal radius or even distal third of fibula • The middle third of fibula can serve as the peroneal artery based vascular graft
  • 28. Points to remember for fibular bone graft • The peroneal nerve must not be damaged; • The distal fourth of the bone must be left to maintain a stable ankle • The peroneal muscles should not be cut.
  • 29. Phemister bone graft • It is subcortical cancellous bone grafting • A bone graft of cortical bone with cancellous bone chips to enhance callus formation. • Bone-grafting without disturbing the pre-existing callus • Bone graft is taken by elevating the osteoperiosteal flaps.
  • 30. Requisites for phemister graft • Petalling should carried out at the fracture site • The mobility at the fracture site should be minimal • The fracture should have an acceptable alignment • The knee joint should have a good range of motion
  • 31. Urist AAA bone graft • Composed of bone morphogenic protein and autolysed , antigen-extracted and autogenic bone. • h-BMP/AAA composite implants represent adjunctive treatment of difficult nonunions • Composite implants may be implanted in either partial or complete segmental defects of long bones
  • 32. Allograft The morbidity and limited amount of autogenic bone graft calls for a need of allogenic bone Graft. They are indicated in 1.Children 2. Elderly 3.Poor surgical risk 4.Enough graft cannot be harvested
  • 33. Allograft types Cortical • Frozen • Freeze dried Cancellous • Frozen • Freeze dried
  • 34. Bone Allografts • Cancellous or cortical – Plentiful supply – Limited infection risk (varies based on processing method) – Provide osteoconductive scaffold – May provide structural support
  • 35. Bone Allografts • Freeze-dried – Even less antigenic – Time to test for diseases – Strictly regulated by FDA – Can be stored at room temperature up to 5 years – Mechanical properties degrade
  • 36. Bone Bank • It is a facilitiy to provide safe and efficient allograft material. • Hosts should be screened for : infections,malignancies(except for basal cell carcinoma of the skin), collagen vascular diseases, metabolic bone diseases and presence of toxins.
  • 37. Technique • Bone is collected in clean and unsterile environment. • It is nibbled to remove the articular cartilage. • It can be sterilized by irradiation, ethylene oxide or strong acid( 0.55 % HCl) • It is subject to deep freeze upto -70 to -80 degrees celcius(frozen) • Freeze drying involves removal of water and vacuum packaging of the tissue
  • 38.
  • 39.
  • 40. Freeze dried bone graft • Decreases expression of MHC 1 complex in osteoblasts • Decreased osteoinductive properties • Reduced mechanical integrity • Decreased number of viable cells • Slow revascularisation and delaye remodelling • Histologically mono nuclear cells surround the newly developed blood vessels
  • 41. Demineralized Bone Matrix • Prepared from cadaveric human bone • Acid extraction of bone leaving – Collagen(type 1) – Noncollagenous proteins – Bone growth factors • BMP quantity extremely low and variable • Sterilized which may decrease the availability of BMP
  • 42. Demineralized Bone Matrix • Available from multiple vendors in multiple preparations – Gel – Putty – Strip – Combination products with cancellous bone and other bone graft substitute products
  • 43. Demineralized Bone Matrix • Growth factor activity varies between tissue banks and between batches • While they may offer some osteoinductive potential because of available growth factors, they mainly act as an osteoconductive agents Han B et al. J Orthop Res. 21(4):648-54, 2003. Blum B, et al. Orthopedics. 27 (1 Suppl): S161 – S165, 2004.
  • 44. Graft Incorporation • Hematoma formation – Release of cytokines and growth factors
  • 45. Graft Incorporation • Hematoma formation – Release of cytokines and growth factors • Inflammation – Development of fibrovascular tissue (18 hours)
  • 46. Graft Incorporation • Hematoma formation – Release of cytokines and growth factors • Inflammation – Development of fibrovascular tissue • Vascular ingrowth – Often extending Haversian canals
  • 47. Graft Incorporation • Hematoma formation – Release of cytokines and growth factors • Inflammation – Development of fibrovascular tissue(18 hours) • Vascular ingrowth – Often extending Haversian canals (10 -12 days) • Focal osteoclastic resorption of graft
  • 48. Graft Incorporation • Hematoma formation – Release of cytokines and growth factors • Inflammation – Development of fibrovascular tissue • Vascular ingrowth – Often extending Haversian canals • Focal osteoclastic resorption of graft • Intramembranous and/or endochondral bone formation on graft surfaces…….
  • 49.
  • 50. Graft Incorporation • Cortical allograft strut graft placed next to cortex of host • After 4 years of incorporation
  • 51. Bone Graft Substitutes • Need for bone graft alternatives has lead to development of numerous bone graft substitutes • Avoid morbidity of autogenous bone graft harvest • Mechanical properties vary • Most offer osteoconductive properties • Some provide osteoinductive properties
  • 52. Bone Graft Substitutes Potential Roles • Extender for autogenous bone graft – Large defects – Multiple level spinal fusion • Enhancer – To improve success of autogenous bone graft • Substitute – To replace autogenous bone graft
  • 53. Properties of bone graft substitutes
  • 55. Laurencin et al, classification • Allograft based • Factor based • Cell based • Ceramic based • Polymer based • Composite
  • 56. Ideal bone graft substitute • Scaffolding for osteoconduction • Growth factors for osteoinduction • Progenitor cells for osteogenesis • Biocompatible and biodegradable and mechanical properties similar to the surrounding bone • Each substitute available nowadays fulfill only some of the criteria
  • 57. Bone Graft Substitutes • Resorption rates vary widely – Dependant on composition • Calcium sulfate - very rapid • Hydroxyapatite (HA) – very, very slow • Some products may be combined to optimize resorption rate – Also dependant on porosity, geometry
  • 58. Bone Graft Substitutes • Mechanical properties vary widely – Dependant on composition • Calcium phosphate cement has highest compressive strength • Cancellous bone compressive strength is relatively low • Many substitutes have compressive strengths similar to cancellous bone • All designed to be used with internal fixation
  • 59. Allograft based • Includes allograft bone used alone or in combination with other materials • Available as demineralised bone matrix
  • 60. Factor based • Involves natural or recombinant factors • Factors responsible for differentiation of progenitor cells and regulation of activities • Mechanism of action: based mostly on activation of protein kinase • Combined and simultaneous activity of various factors controlled resorption and formation of new bone
  • 61. • Factor + receptors on the cell surface • Activation of protein kinase • Transcription of mRNA • Protein synthesis • Regulation of cell activities
  • 62. • Includes TGF-beta, IGF-I&II,PDGF,FGF and BMPs • Mostly in research phase • Recombinant BMP-2 as INFUSE bone graft
  • 64. BMP 2 and 7 BMP 2 • Acts as a disulfide linked homodimer and helps in bone and cartilage formation • It is a candidate as retinoid mediator and helps osteoblastic differentiation BMP 7 • It plays a key role in osteoblastic differentiation • It induces the prodution of SMAD 1 • It plays a key role in renal development and repair
  • 65. Bone Morphogenetic Proteins • Produced by recombinant technology • Two most extensively studied and commercially available – BMP-2 (Infuse) Medtronics – BMP-7 (OP-1)Stryker ss – BMP-2 and BMP-7 are water soluble and require a carrier to remain in the operative area to be effective
  • 66. BMP-2 for Open Tibial Fractures • Prospective, randomized study • 450 patients · All received IM nail (vast majority with UNREAMED technique) and appropriate soft tissue management · Randomized to 3 treatments at time of definitive wound closure · Placebo · 0.75 mg/ml BMP-2/ACS · 1.50 mg/ml BMP-2/ACS BESTT Study Group, et al. J Bone Joint Surg 84A: 2123, 2002.
  • 67. Results • 44% reduction in risk of nonunion/delayed union with high dose BMP-2 • Significantly faster fracture healing • Significantly fewer – invasive interventions – hardware failures – infections BESTT Study Group, et al. J Bone Joint Surg 84A: 2123, 2002.
  • 68. Cell Based • Based on in vitro differentiation of mesenchymal stem cells to osteoblastic lineage • They have been used along with ceramics • Proposed to be used in bone repair prosthetic setting
  • 69. Ceramic based • About 60% BGS involves ceramics- alone or in combination • Eg : calcium sulfate, calcium phosphate, bioactive glass • Primary inorganic componet is calcium hyroxyapatite • Property of osteointegration, newly formed mineralised tissue forms intimate bond with implant materials
  • 70. Calcium Phosphate Ceramics • Enable osteoconduction but use is limited due to poor tensile strength and brittleness • Injectable pastes of calcium and phospate – Norian SRS (Synthes/Stratec) – Alpha BSM (Etex/Depuy) – Callos Bone Void Filler (Skeletal Kinetics)
  • 71. Calcium Phosphat Ceramics • It is produced by the process of Sintering(heating over 1000degrees C) • Injectable • Very high compressive strength once hardens • Some studies of its use have allowed earlier weightbearing and range of motion
  • 72. Calcium Sulfate(plaster of paris) · Osteoconductive void filler · Low compressive strength – no structural support · Rapidly and complete resorption · May be used as a autogenous graft extender - Available from numerous companies - Osteoset, Calceon 6, Bone Blast, etc.
  • 73. Calcium Sulfate • Pellets – Pellet injectors • Bead kits – Allows addition of antibiotics • Injectable – May be used to augment screw purchase • Combination of DMB and calcium sulfate
  • 74. Hydroxyapatite(HA) • It is a slowly resorbing compound of calcium phosphate • Source :synthetic and animal • Hydrothermal process converts it from its native coral form to more stable HA form with pore diameters between 200 to 400 micron
  • 75. Hydroxyapatite • Interconnected porous structure closely resembles the porosity of human cancellous bone Cancellous Bone Coralline hydroxyapatite
  • 76. Hydroxyapatite • Interpore(Interpore International, Irvine,CA):first calcium phosphate based BGS approved by FDA • Marketed as ProOsteon by Interpore Cross • Available in various size blocks & granules • ProOsteon 500 – Very slow resorption • ProOsteon 500 R – Only a thin layer of HA – Faster resorption
  • 77. Hydroxyapatite:indications • Valgus instability following lateral tibial plateau fracture • Varus instability following medial condyle fracture of tibia • Articular incongruence of 10 mm or more • Translation of major condylar fragment of more than 5mm
  • 78. Tricalcium Phosphate(TCP) • TCP composition is similar to calcium and phosphate phase of human bone and has porous nature • TCP undergoes partial resorption and some of it may be converted to HA once implanted in the human body • Complete resorption at 6 months
  • 79. Tricalcium Phosphate • Wet compressive strength slightly less than cancellous bone • Available as blocks, wedges, and granules • Numerous tradenames – Vitoss (Orthovita) – ChronOS (Synthes) – Conduit (DePuy) – Cellplex TCP (Wright Medical) – Various Theri__ names (Therics)
  • 80. Calcium Phosphate Cements(CPC) • CPC is used as void filler in defects • It consists of inorganic calcium and phosphate combined to form an injectable paste
  • 81. Polymer based • Can be divided: natural/synthetic • Further divided into: biodegradable/non biodegradable • eg: Healoss(depuy)-natural • Eg :Cortoss- injectable resin based product • Eg : Rhakoss(Orthovita)
  • 82. Collagen Based Matrices • Highly purified Type 1 bovine dermal fibrillar collagen • Bone marrow is added to provide bone forming cells • Collagraft (Zimmer) – Collagen / HA / Tricalcium phosphate • Healos (Depuy) – Collagen / HA
  • 83. Composite graft • In this two or more type of bone graft substitutes combined together • So that osteoconductive and osteoinductive properties of different BGS, is combined
  • 84. Calcium Phosphate-Collagen Composite • Collagen provides binding sites for matrix proteins • Type I and III is added to HA,TCP and autologous bone marrow to form a graft material • Although no structural support but augments frature healing
  • 85. Bone Graft Substitute Incorporation • Partial incorporation of hydroxyapatite bone graft substitute • Biopsy of material obtained 1 year post-op

Notes de l'éditeur

  1. Bone grafts, and bone graft substitutes, are used primarily for three main purposes. One, to provide structural support, such as after elevation of a depressed tibial plateau fracture. Second, to fill a void, such as after excision of a bone cyst in an area that does not demand any structural support. Third, to improve fracture healing. Either by speeding healing or increasing the successful union rate.
  2. The most common form of autogenous bone graft is cancellous bone, usually harvested from either anterior or posterior iliac crests, but which also may be harvested locally such as in the proximal tibia or distal radius. Cortical bone strips may be harvested from the inner table of the pelvis. Occasionally a vascularized bone graft may be used, such ass a free fibular transfer. Another option for obtaining osteogenic cells is by bone marrow aspirate.
  3. Two bone morphogenetic proteins are commercially available. These are BMP-2,marketed by Medtronics, and BMP-7, more commonly known of osteogenic protein 1, produced by Stryker Biotech. These products are produced by recombinant technology in which large quantities of the material are produced in cell culture.
  4. BMPs have been studies in several human investigations including open fractures and nonunions. BMP-2 was studied in a prospective, randomized study of 450 patients with open tibial shaft fractures treated with fracture debridement and an IM nail. At the time of definitive wound closure patients were randomized to one of three treatments placebo 0.75 mg/ml BMP-2/ACS (lower BMP dose) 1.50 mg/ml BMP-2/ACS (higher BMP dose)
  5. The primary outcome measure was the proportion of patients requiring secondary intervention because of delayed union or nonunion within twelve months postoperatively. In the group treated with the higher dose BMP-2 there was a 44% reduction in risk of nonunion/delayed union Significantly faster fracture healing Significantly fewer invasive interventions Significantly fewer hardware failures and fewer infections The graph from their publication shows the placebo control groups in black representing the standard of care. The Gustilo IIIB&amp;apos;s are on the left and the Gustilo I, II and IIIA&amp;apos;s on the right. There is a statistically significant reduction in the number of secondary interventions in those fractures treated with the higher dose of BMP-2.
  6. Calcium phosphate products are an injectable paste of calcium and phosphate. Norian SRS was the first such product available and is marketed by Synthes / Stratec. Two other calcium phosphate type products are also available in the U.S.
  7. Medical grade calcium sulfate is an osteoconductive void filler. It has low compressive strength so doesn’t offer structural support. Another disadvantage of the product is that it resorbs rather rapidly, perhaps more rapidly then it can be replaced by new bone. One way it which it may be used is an extender for autogenous bone graft.
  8. Calcium sulfate products are available both as pellets, bead kits, and injectable preparations. The pellets can be poured into position, but some companies also provide an injector apparatus. The bead kits allow the addition of antibiotics if desired.