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Bone morphogenetic proteins
and the induction of periodontal
      tissue regeneration



          INDIAN DENTAL ACADEMY
       Leader in Continuing Dental Education

        www.indiandentalacademy.com
Introduction:
   Tissue engineering defined as the science of
    fabrication of new tissues for replacement and
    the regeneration of lost or destroyed tissues.
   The three critical ingredients for optimal tissue
    engineering are;
     Soluble molecular signals,
     Responding     cells with associated    cell-surface
      receptors, and
     Assembly of the extracellular matrix
   This knowledge can now be applied not only to
    bone regeneration but also to alveolar bone with
    associated cementum and periodontal ligament
    regeneration.
                www.indiandentalacademy.com
   Substantial knowledge has now been gained
    about the molecular signals that determine the
    emergence of the complex tissue morphologies
    during regeneration of the periodontal tissues.
   The      molecular    mechanisms        for  such
    regeneration are the osteogenic proteins of the
    transforming growth factor-β superfamily of
    which the bone morphogenetic and osteogenic
    proteins (BMPs/OPs) are a class of powerful
    inducers of endochondral bone differentiation.
   Lacroix in 1945 hypothesized that bone contains
    substances which he named osteogenins, that
    initiate bone growth and differentiation.
              www.indiandentalacademy.com
   Urist 1964 made the key discovery that Demineralized
    bone matrix when implanted heterotopically in
    intramuscular sites of allogenic rat recipients, induces de
    novo endochondral bone formation by induction.

   BMP is the generic name for proteins which are
    extracted from bone matrix with agents such as 4M
    guanidine hydrochloride, 6M urea in 0.5M CaCl2 or
    ethylene glycol in an aqueous/nonaqueous solvent
    mixture.

   Reddi and Huggins showed that subcutaneous
    implantation of Demineralized bone matrix results in de
    novo local endochondral bone differentiation.
                www.indiandentalacademy.com
Endochondral bone formation in subcutaneous space ( rodent)
5–20µg of BMPs/OPs.




                www.indiandentalacademy.com
The sequential developmental cascade In
  endochondral bone formation;
activation and migration of undifferentiated mesenchymal cells by
                             chemotaxis

anchorage dependent cell attachment to the matrix via fibronectin

    mitosis and proliferation of responding mesenchymal cells

    differentiation of chondroblasts and deposition of cartilage

                  mineralization of the cartilage

        angiogenesis, vascular invasion and chondrolysis

    differentiation of osteoblasts and bone matrix deposition

          mineralization of the newly induced bone and
                www.indiandentalacademy.com
differentiation of hemopoietic marrow in the newly formed ossicles
   The dissociative extraction of the demineralized bone
    matrix with agents (urea and guanidinium hydrochloride)
    yielded an insoluble component mainly type I collagen
    (insoluble collagenous bone matrix) and a soluble protein
    extract containing the putative osteogenic proteins.
   The operational reconstitution of the inactive and
    insoluble collagenous bone matrix with protein extracts
    after a single step of gel-filtration chromatography
    restored the biological activity yielding endochondral
    bone differentiation by induction after recombining the
    insoluble with the soluble signals.
   Endochondral bone induction is the result of the
    combined action of BMPs/OPs and the complementary
    substratum that delivers the osteogenic activity of the
    soluble molecular signal.

                www.indiandentalacademy.com
BMPs/OPs induction of cementogenesis and PDL
regeneration:
   More than 40 related proteins with BMP/OP-like
    sequences and activities have been sequenced and
    cloned.
   each protein either purified to BMPs and the induction of
    periodontal tissue regeneration homogeneity from
    natural sources or cloned and expressed by recombinant
    DNA technology induces endochondral bone formation,
    by induction in heterotopic sites of a variety of animal
    models including adult primates.
   In addition to bone induction, BMPs/OPs are expressed
    during early development and organogenesis indicating
    that BMPs/OPs are related members play critical roles
    as soluble mediators of epithelial–mesenchymal
    interactions and inductive events unrelated to bone
    induction. (Hogan 1996; Nakashima 2003)
                 www.indiandentalacademy.com
Bone induction in implantation of highly purified
bone-derived bovine (BMPs/OPs)




           www.indiandentalacademy.com
   The induction of bone by hOP-1 develops as a mosaic
    structure with distinct spatial and temporal patterns of
    gene expression of members of the transforming growth
    factor-β superfamily that singly, synergistically initiate
    and maintain tissue induction and morphogenesis.
   The expression of OP-1, type IV collagen, BMP-3 and
    transforming growth factor-β1 mRNAs by Northern blot
    analyses showed progressing stages of osteogenic
    differentiation during the initiation of bone formation by
    the hOP-1 osteogenic device. (Ripamonti 2005)
   The continuous high-expression patterns of type IV
    collagen mRNA indicates the critical role of hOP-1 in the
    induction of angiogenesis.



                www.indiandentalacademy.com
   BMPs/OPs are involved in tooth morphogenesis at different
    stages of development. During the later developmental
    stages of tooth morphogenesis, the induction of
    cementogenesis, PDL and alveolar bone differentiation
    which are regulated by the co-ordinated expression of
    BMPs/OPs.

   A systematic analysis of the expression of six different
    BMPs in tooth morphogenesis has shown that the
    expression patterns of each BMP is different and there is
    co-distribution between specific family members.

   Root morphogenesis is a classical example of epithelial–
    mesenchymal interactions. The localization of BMP-3 and
    OP-1 during morphogenesis of the mouse root suggests
    that these proteins play a role during cementogenesis and
    the assembly www.indiandentalacademy.com periodontal ligament
                   of a functionally oriented
    fiber syste. (Thomadakis et al 1999)
Imuuno-localization of BMP- 3 & OP- 1:




             www.indiandentalacademy.com
   The localization of BMP-2 in alveolar bone only and
    BMP-3 and OP-1 in all three components of the
    periodontium, indicates that the morphogenesis of
    periodontal tissues may involve a composite pattern of
    co-ordinated expression of different signaling isoforms.
   The mosaicism of BMP/OP expression during root
    morphogenesis indicates that optimal therapeutic
    regeneration and tissue engineering may entail binary
    combinations of osteogenic gene products based on
    recapitulation of embryonic development.
   Amino acid sequence variations in the active C-terminal
    domain of each morphogenetic protein confer
    specialized activities to BMP/OP isoforms and this is the
    molecular basis that determines the structure–activity
    profile of single BMPs/OPs.


                www.indiandentalacademy.com
Periodontal tissue regeneration by naturally derived and
recombinant human BMPs/OPs in the nonhuman primate
   To induce the cascade of bone differentiation, the
    soluble osteogenic molecular signals of the transforming
    growth factor-β superfamily must be reconstituted with
    an insoluble signal or substratum that triggers the bone
    differentiation cascade.
   Different BMPs/OPs and combinations of these have
    been implanted in furcation defects of the mandibular
    first and second molars of adult baboons, which are
    delivered by insoluble collagenous bone matrices as a
    carrier.
   Naturally derived BMPs/Ops induced cementum,
    periodontal ligament and alveolar bone regeneration in
    surgically created class II furcation defects of mandibular
    molars.
                www.indiandentalacademy.com
www.indiandentalacademy.com
   The newly formed Sharpey’s fibers were inserted
    perpendicularly into the newly formed cementum
    covered by a thin layer of cementoid.

   The sources of responding cells that initiate
    cementogenesis and periodontal ligament regeneration
    are still not well understood. Recent studies have
    indicated that the periodontal ligament system contains
    stem cells that have the potential to regenerate
    cementum and periodontal ligament in vivo (Seo et al
    2004).




               www.indiandentalacademy.com
   Synchronous but spatially distinct OP-1 and BMP-2
    expression during murine root formation points to
    specific functions of OP-1 and BMP-2 in periodontal
    tissue morphogenesis and thus regeneration in postnatal
    life.

   The co-localization findings of OP-1 and BMP-2 during
    tooth morphogenesis has suggested that co-
    administration of OP-1 and BMP-2 in recombinant form
    would result in synergistic tissue morphogenesis as a
    recapitulation of memory of developmental events in the
    embryo.

   hBMP-2 was found to be more osteogenic than
    cementogenic in both beagle dogs and baboons.
               www.indiandentalacademy.com
   hOP-1 clearly modulates the expression of the
    cementogenic phenotype and the induction of
    cementogenesis in both animal models, and also on root
    surfaces exposed by disease (Ripamonti 2002).

   hBMP-6 has also been investigated in a periodontal
    fenestration defect model in rodents. The study indicated
    that hBMP-6 induced significantly more new cementum
    formation as compared to control fenestration defects
    (Huang et al 2005).

   hBMP-12 has also become the focus of attention for
    periodontal regenerative studies. (Wikesjo¨ et al. 2004)

                www.indiandentalacademy.com
Perspectives in periodontal tissue
    engineering by BMPs:
   The capacity of mammalian BMPs/OPs to initiate a
    programmed cellular cascade that results in the induction of
    bone is a functionally conserved process utilized in
    embryonic development, recapitulated in post-fetal
    osteogenesis and can be re-exploited for the therapeutic
    initiation of periodontal tissue regeneration.

   The presence of the structure–activity profile amongst
    soluble osteogenic molecular signals indicates a therapeutic
    significance in clinical contexts (Ripamonti 2006).

   A soluble osteogenic and recombinant molecular signals
    when combined with an insoluble signal, triggers periodontal
    tissue regeneration with the induction of cementogenesis
    and insertion of Sharpey’s fibers. Therfore these signals are
    essential ingredients to engineer periodontal tissue
                  www.indiandentalacademy.com
    regeneration (Ripamonti 2002 & 2006).

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Bone morphogenetic proteins /certified fixed orthodontic courses by Indian dental academy

  • 1. Bone morphogenetic proteins and the induction of periodontal tissue regeneration INDIAN DENTAL ACADEMY Leader in Continuing Dental Education www.indiandentalacademy.com
  • 2. Introduction:  Tissue engineering defined as the science of fabrication of new tissues for replacement and the regeneration of lost or destroyed tissues.  The three critical ingredients for optimal tissue engineering are;  Soluble molecular signals,  Responding cells with associated cell-surface receptors, and  Assembly of the extracellular matrix  This knowledge can now be applied not only to bone regeneration but also to alveolar bone with associated cementum and periodontal ligament regeneration. www.indiandentalacademy.com
  • 3. Substantial knowledge has now been gained about the molecular signals that determine the emergence of the complex tissue morphologies during regeneration of the periodontal tissues.  The molecular mechanisms for such regeneration are the osteogenic proteins of the transforming growth factor-β superfamily of which the bone morphogenetic and osteogenic proteins (BMPs/OPs) are a class of powerful inducers of endochondral bone differentiation.  Lacroix in 1945 hypothesized that bone contains substances which he named osteogenins, that initiate bone growth and differentiation. www.indiandentalacademy.com
  • 4. Urist 1964 made the key discovery that Demineralized bone matrix when implanted heterotopically in intramuscular sites of allogenic rat recipients, induces de novo endochondral bone formation by induction.  BMP is the generic name for proteins which are extracted from bone matrix with agents such as 4M guanidine hydrochloride, 6M urea in 0.5M CaCl2 or ethylene glycol in an aqueous/nonaqueous solvent mixture.  Reddi and Huggins showed that subcutaneous implantation of Demineralized bone matrix results in de novo local endochondral bone differentiation. www.indiandentalacademy.com
  • 5. Endochondral bone formation in subcutaneous space ( rodent) 5–20µg of BMPs/OPs. www.indiandentalacademy.com
  • 6. The sequential developmental cascade In endochondral bone formation; activation and migration of undifferentiated mesenchymal cells by chemotaxis anchorage dependent cell attachment to the matrix via fibronectin mitosis and proliferation of responding mesenchymal cells differentiation of chondroblasts and deposition of cartilage mineralization of the cartilage angiogenesis, vascular invasion and chondrolysis differentiation of osteoblasts and bone matrix deposition mineralization of the newly induced bone and www.indiandentalacademy.com differentiation of hemopoietic marrow in the newly formed ossicles
  • 7. The dissociative extraction of the demineralized bone matrix with agents (urea and guanidinium hydrochloride) yielded an insoluble component mainly type I collagen (insoluble collagenous bone matrix) and a soluble protein extract containing the putative osteogenic proteins.  The operational reconstitution of the inactive and insoluble collagenous bone matrix with protein extracts after a single step of gel-filtration chromatography restored the biological activity yielding endochondral bone differentiation by induction after recombining the insoluble with the soluble signals.  Endochondral bone induction is the result of the combined action of BMPs/OPs and the complementary substratum that delivers the osteogenic activity of the soluble molecular signal. www.indiandentalacademy.com
  • 8. BMPs/OPs induction of cementogenesis and PDL regeneration:  More than 40 related proteins with BMP/OP-like sequences and activities have been sequenced and cloned.  each protein either purified to BMPs and the induction of periodontal tissue regeneration homogeneity from natural sources or cloned and expressed by recombinant DNA technology induces endochondral bone formation, by induction in heterotopic sites of a variety of animal models including adult primates.  In addition to bone induction, BMPs/OPs are expressed during early development and organogenesis indicating that BMPs/OPs are related members play critical roles as soluble mediators of epithelial–mesenchymal interactions and inductive events unrelated to bone induction. (Hogan 1996; Nakashima 2003) www.indiandentalacademy.com
  • 9. Bone induction in implantation of highly purified bone-derived bovine (BMPs/OPs) www.indiandentalacademy.com
  • 10. The induction of bone by hOP-1 develops as a mosaic structure with distinct spatial and temporal patterns of gene expression of members of the transforming growth factor-β superfamily that singly, synergistically initiate and maintain tissue induction and morphogenesis.  The expression of OP-1, type IV collagen, BMP-3 and transforming growth factor-β1 mRNAs by Northern blot analyses showed progressing stages of osteogenic differentiation during the initiation of bone formation by the hOP-1 osteogenic device. (Ripamonti 2005)  The continuous high-expression patterns of type IV collagen mRNA indicates the critical role of hOP-1 in the induction of angiogenesis. www.indiandentalacademy.com
  • 11. BMPs/OPs are involved in tooth morphogenesis at different stages of development. During the later developmental stages of tooth morphogenesis, the induction of cementogenesis, PDL and alveolar bone differentiation which are regulated by the co-ordinated expression of BMPs/OPs.  A systematic analysis of the expression of six different BMPs in tooth morphogenesis has shown that the expression patterns of each BMP is different and there is co-distribution between specific family members.  Root morphogenesis is a classical example of epithelial– mesenchymal interactions. The localization of BMP-3 and OP-1 during morphogenesis of the mouse root suggests that these proteins play a role during cementogenesis and the assembly www.indiandentalacademy.com periodontal ligament of a functionally oriented fiber syste. (Thomadakis et al 1999)
  • 12. Imuuno-localization of BMP- 3 & OP- 1: www.indiandentalacademy.com
  • 13. The localization of BMP-2 in alveolar bone only and BMP-3 and OP-1 in all three components of the periodontium, indicates that the morphogenesis of periodontal tissues may involve a composite pattern of co-ordinated expression of different signaling isoforms.  The mosaicism of BMP/OP expression during root morphogenesis indicates that optimal therapeutic regeneration and tissue engineering may entail binary combinations of osteogenic gene products based on recapitulation of embryonic development.  Amino acid sequence variations in the active C-terminal domain of each morphogenetic protein confer specialized activities to BMP/OP isoforms and this is the molecular basis that determines the structure–activity profile of single BMPs/OPs. www.indiandentalacademy.com
  • 14. Periodontal tissue regeneration by naturally derived and recombinant human BMPs/OPs in the nonhuman primate  To induce the cascade of bone differentiation, the soluble osteogenic molecular signals of the transforming growth factor-β superfamily must be reconstituted with an insoluble signal or substratum that triggers the bone differentiation cascade.  Different BMPs/OPs and combinations of these have been implanted in furcation defects of the mandibular first and second molars of adult baboons, which are delivered by insoluble collagenous bone matrices as a carrier.  Naturally derived BMPs/Ops induced cementum, periodontal ligament and alveolar bone regeneration in surgically created class II furcation defects of mandibular molars. www.indiandentalacademy.com
  • 16. The newly formed Sharpey’s fibers were inserted perpendicularly into the newly formed cementum covered by a thin layer of cementoid.  The sources of responding cells that initiate cementogenesis and periodontal ligament regeneration are still not well understood. Recent studies have indicated that the periodontal ligament system contains stem cells that have the potential to regenerate cementum and periodontal ligament in vivo (Seo et al 2004). www.indiandentalacademy.com
  • 17. Synchronous but spatially distinct OP-1 and BMP-2 expression during murine root formation points to specific functions of OP-1 and BMP-2 in periodontal tissue morphogenesis and thus regeneration in postnatal life.  The co-localization findings of OP-1 and BMP-2 during tooth morphogenesis has suggested that co- administration of OP-1 and BMP-2 in recombinant form would result in synergistic tissue morphogenesis as a recapitulation of memory of developmental events in the embryo.  hBMP-2 was found to be more osteogenic than cementogenic in both beagle dogs and baboons. www.indiandentalacademy.com
  • 18. hOP-1 clearly modulates the expression of the cementogenic phenotype and the induction of cementogenesis in both animal models, and also on root surfaces exposed by disease (Ripamonti 2002).  hBMP-6 has also been investigated in a periodontal fenestration defect model in rodents. The study indicated that hBMP-6 induced significantly more new cementum formation as compared to control fenestration defects (Huang et al 2005).  hBMP-12 has also become the focus of attention for periodontal regenerative studies. (Wikesjo¨ et al. 2004) www.indiandentalacademy.com
  • 19. Perspectives in periodontal tissue engineering by BMPs:  The capacity of mammalian BMPs/OPs to initiate a programmed cellular cascade that results in the induction of bone is a functionally conserved process utilized in embryonic development, recapitulated in post-fetal osteogenesis and can be re-exploited for the therapeutic initiation of periodontal tissue regeneration.  The presence of the structure–activity profile amongst soluble osteogenic molecular signals indicates a therapeutic significance in clinical contexts (Ripamonti 2006).  A soluble osteogenic and recombinant molecular signals when combined with an insoluble signal, triggers periodontal tissue regeneration with the induction of cementogenesis and insertion of Sharpey’s fibers. Therfore these signals are essential ingredients to engineer periodontal tissue www.indiandentalacademy.com regeneration (Ripamonti 2002 & 2006).