BMP binding peptide: A BMP‐2 enhancing factor deduced from the sequence of native bovine bone morphogenetic protein/non‐collagenous protein

Behnam, Keyvan; Phillips, Martin; Silva, Jose Denison Prado; Brochmann, Elsa J.; Duarte, Maria Eugênia Leite; Murray, Samuel S.

doi:10.1016/j.orthres.2004.05.001

Cited by 40 publications

(110 citation statements)

References 5 publications

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“…The estimated dissociation constant (K D ) between BBP and rhBMP-2 was 3 Â 10 À5 M, which was similar to that between BBP and TGF-B receptor II. 10 Our results suggest that BBP can bind to rhBMP-7 and enhance its osteogenic activity. Furthermore, this enhancement appears to be dose-dependent.…”

Section: Discussionmentioning

confidence: 56%

“…This peptide contains a cystatin-like domain that is a fragment of secreted phosphoprotein-24 (SPP-24), which belongs to cystatin family. 10 The N-terminal 107 residues of SPP-24 are related to the cystatine family of thiol protease inhibitors, which are known to be involved in bone turnover. 19 Other members of the cystatin family, such as fetuin, have an affinity to TGF-B and BMPs because the cystatin domain contains a region similar to the TGF-B receptor II homology 1 domain (TRH1).…”

Section: Discussionmentioning

confidence: 99%

“…Similar results were reported by previous studies. 9,10 However, when 1000 mg of BBP was combined with either 2 mg rhBMP-7 or 5 mg rhBMP-7, significant differences were seen in radiographic scores, manual palpation, and bone volume compared to 2 mg rhBMP-7 or 5 mg rhBMP-7 alone, suggesting that BBP itself does not have osteoinductive potential but can enhance the osteogenic activity of rhBMP-7. The estimated dissociation constant (K D ) between BBP and rhBMP-2 was 3 Â 10 À5 M, which was similar to that between BBP and TGF-B receptor II.…”

Section: Discussionmentioning

confidence: 99%

“…BBP enhanced rhBMP-2 induced ectopic bone formation in a mouse muscle pouch implantation model. 10 Furthermore, this peptide also accelerated rhBMP-2 induced radiographic fusion in a rat spine model. 9 We hypothesized that BBP can be used to enhance bone healing of rhBMP-7 and that the effect is dose related.…”

mentioning

confidence: 93%

“…These strategies include the use of delivery devices that allow better application of rhBMP-7 and obtain better retention at the surgery site, 7 the use of carriers that control the release of rhBMP-7, 8 and the use of a specific binding peptide that enhances the effect of rhBMP-2 in bone healing. 9 BMP binding peptide (BBP) was developed by Behnam et al 10 They isolated an 18.5 kDa fragment of the human bone matrix protein that has the chemical and physical properties of Urist's ''BMP.'' BBP enhanced rhBMP-2 induced ectopic bone formation in a mouse muscle pouch implantation model.…”

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confidence: 99%

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Enhancement of recombinant human BMP‐7 bone formation with bmp binding peptide in a rodent femoral defect model

Liao

Tzeng

Keorochana

et al. 2010

Journal Orthopaedic Research

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Bone morphogenetic binding peptide (BBP) is an 18.5 kDa fragment of a bone matrix protein peptide. A rat femoral defect model was used to test the effect of BBP combined with recombinant human bone morphogenetic protein-7 (rhBMP-7) to induced bone healing. Two doses of BBP (500 and 1000 mg) were tested with two doses of rhBMP-7 (2 and 5 mg), and the results were compared with a positive control (10 mg rhBMP-7). Bone healing was evaluated by radiology, manual palpation, microcomputed tomography, and histology. The high dose of 10 mg of rhBMP-7 resulted in a consistent 100% bone union rate and a mature histological appearance on histology, and was used as a positive control. When 1000 mg of BBP was combined with lower doses of BMP-7 (2 mg rhBMP-7 or 5 mg rhBMP-7) significant differences were seen in radiographic scores, manual palpation, and bone volume, when compared to 2 mg rhBMP-7 or 5 mg rhBMP-7 alone. The combination of 1000 mg of BBP and 5 mg rhBMP-7 also achieved 100% fusion rate, induced a larger amount of bone formation, and yielded similar maturity of bone marrow when compared with the high dosage 10 mg rhBMP-7 group. This study demonstrated that when combined together, BBP can enhance the bone healing of rhBMP-7. Improved healing imparted by the addition of BBP may result in lesser amounts of rhBMP-7 needed to achieve union in the clinical setting. ß

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Section: Discussionmentioning

confidence: 56%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 93%

mentioning

confidence: 99%

See 3 more Smart Citations

Enhancement of recombinant human BMP‐7 bone formation with bmp binding peptide in a rodent femoral defect model

Liao

Tzeng

Keorochana

et al. 2010

Journal Orthopaedic Research

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Nanoparticles for Stem‐Cell Engineering

Jabbari

2015

Stem‐Cell Nanoengineering

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Multifunctional Hydrogels that Promote Osteogenic Human Mesenchymal Stem Cell Differentiation Through Stimulation and Sequestering of Bone Morphogenic Protein 2

Benoit

Collins

Anseth

2007

Adv Funct Materials

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The extracellular environment controls many cellular activities thereby linking external material cues to internal cell function. By better understanding these processes, synthetic extracellular material niches can be tailored to present cells with highly regulated physical and/or chemical cues that promote or suppress selected cell functions. Here, poly(ethylene glycol) (PEG) hydrogels were functionalized with fluvastatin-releasing grafts and growth factor binding heparin domains to enable the dynamic exchange of information between the material and cells from the outside-in and inside-out (i.e., bidirectional signaling). By incorporating a fluvastatin-releasing graft and carefully controlling the dose and temporal release, materials were designed to promote bone morphogenic protein (BMP2) and alkaline phosphatase (ALP) production by human mesenchymal stem cells (hMSCs). When the release of fluvastatin was controlled to occur over 2 weeks, BMP2 and ALP production was increased 2.2-fold and 1.7-fold, respectively, at day 28 compared to hMSCs cultured in the absence of fluvastatin. By introducing a heparin functionality into the gel to sequester and localize the hMSC-produced BMP2, the osteogenic differentiation of hMSCs was further augmented over fluvastatin delivery alone. Osteopontin and core binding factor α1 gene expression was 6-fold and 4-fold greater for hMSCs exposed to fluvastatin in the presence of the heparin functionalities, respectively. These results demonstrate how multifunctional gels that interact with cells in a bidirectional manner can efficiently promote selected cell functions, such as the osteogenic differentiation of hMSCs.

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BMP binding peptide: A BMP‐2 enhancing factor deduced from the sequence of native bovine bone morphogenetic protein/non‐collagenous protein

Cited by 40 publications

References 5 publications

Enhancement of recombinant human BMP‐7 bone formation with bmp binding peptide in a rodent femoral defect model

Enhancement of recombinant human BMP‐7 bone formation with bmp binding peptide in a rodent femoral defect model

Nanoparticles for Stem‐Cell Engineering

Multifunctional Hydrogels that Promote Osteogenic Human Mesenchymal Stem Cell Differentiation Through Stimulation and Sequestering of Bone Morphogenic Protein 2

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