| Literature DB >> 22550505 |
Andreas Schmitt1, Martijn van Griensven, Andreas B Imhoff, Stefan Buchmann.
Abstract
Stem cell research plays an important role in orthopedic regenerative medicine today. Current literature provides us with promising results from animal research in the fields of bone, tendon, and cartilage repair. While early clinical results are already published for bone and cartilage repair, the data about tendon repair is limited to animal studies. The success of these techniques remains inconsistent in all three mentioned areas. This may be due to different application techniques varying from simple mesenchymal stem cell injection up to complex tissue engineering. However, the ideal carrier for the stem cells still remains controversial. This paper aims to provide a better understanding of current basic research and clinical data concerning stem cell research in bone, tendon, and cartilage repair. Furthermore, a focus is set on different stem cell application techniques in tendon reconstruction, cartilage repair, and filling of bone defects.Entities:
Year: 2012 PMID: 22550505 PMCID: PMC3328166 DOI: 10.1155/2012/394962
Source DB: PubMed Journal: Stem Cells Int Impact factor: 5.443
Figure 1The two strategies of stem cell application in regenerative medicine. Stem cells are either isolated from the patient (autologous transplantation) or from other donors (allogenous transplantation). The cells are expanded in vitro and either applied directly to the patient to substitute lost cells (“cell therapy”), or seeded into 3 dimensional scaffolds (“Tissue engineering”) and differentiated into the demanded cell type. The composed artificial tissue construct is subsequently implanted into patients' tissue defect.
Figure 2Stem cells participate in tissue regeneration in different ways. They directly differentiate into tissue-specific cells and thus substitute damaged or lost cells (A). They indirectly influence tissue regeneration by secretion of soluble factors. Here they promote vascularization, cell proliferation, differentiation within the tissue (B) and modulate inflammatory processes (C).
Clinical applications of mesenchymal stem cells in bone regeneration.
| Author | Diagnosis | Application |
| Results |
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| Treatment of nonunions | ||||
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| Connolly et al. 1991 [ | Atrophic pseudarthrosis | Percutaneous autologous bone marrow injection | 20 | Healing capacity comparable to autologous cancellous bone grafting |
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| Garg et al. 1993 [ | Nonunion in long bones | Percutaneous autologous bone marrow injection | 20 | 17 out of 20 cases united in 5 months |
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| Kettunen et al. 2002 [ | Tibially delayed or non-union | Percutaneous autologous bone marrow injection | 41 | Appeared to be as effective as open techniques |
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| Hernigou et al. 2005 [ | Atrophic pseudarthrosis | Percutaneous autologous bone marrow injection | 60 | Application is effective and safe Positive correlation between number of progenitor cells and callus volume |
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| Goel et al. 2005 [ | Tibial non-union | Percutaneous autologous bone marrow injection | 20 | 15 out of 20 patients showed bone union |
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| Treatment of osteonecrosis | ||||
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| Hernigou and Beaujean 2002 [ | Osteonecrosis femoral head | Injection of autologous bone marrow concentrate | 116 (189 hips) | Very good results in early stages Injection of greater number of progenitor cells transplanted had better outcomes |
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| Gangji et al. 2004 [ | Osteonecrosis femoral head | Injection of autologous bone marrow concentrate | 13 (18 hips) | Significant reduction of pain, progression and improvement of function |
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| Hernigou et al. 2009 [ | Osteonecrosis femoral head | Injection of autologous bone marrow concentrate | 342 (534 hips) | High amount of progenitor cells as predictor for successful outcome |
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| Enhancing spinal fusions | ||||
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| Neen et al. 2006 [ | Spinal fusions | Autologous bone marrow aspirate on hydroxyapatite-collagen I-composite | 50 | Similar healing capacity as autologous cancellous bone grafting in posterolateral fusion Inferior results in interbody fusions |
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| Gan et al. 2008 [ | Spinal fusions | Bone marrow concentrate on tricalciumphosphate | 41 | After 34.5 months 95.1% cases showed good spinal fusion |
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| Filling bone cysts | ||||
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| Wright et al. 2008 [ | Simple bone cysts | Intralesional injection of autologous bone marrow aspirate | 77 | Inferior results compared to injection of methylprednisolone |
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| Park et al. 2008 [ | Simple bone cysts | Implantation of autologous bone marrow aspirate implanted in combination with either nonvital allogenic bone graft or injected with bone powder | 20 (23 cysts) | Injection of bone marrow-bone powder mix is effective alternative to open treatment |
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| Zamzam et al. 2009 [ | Simple bone cysts | Percutaneous autologous bone marrow injection | 28 | Application is a safe and effective treatment |
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| Filling of bone defects | ||||
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| Salama and Weissman 1978 [ | Different bone defects | Xenograft with bone marrow aspirate | 28 | Results have been “most satisfactory” |
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| Jäger et al. 2009 [ | volumetric bone deficiencies | local autologous bone marrow/mesenchymal stem cell injection | 10 | May be a promising alternative to autogenous bone grafting |
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| Marcacci et al. 2007 [ | Large bone diaphysis defect | autologous MSCs were expanded | 4 | Followup up to 7 years after surgery, good integration of implant, no secondary fractures |
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| Various applications | ||||
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| Hendrich et al. 2009 [ | various bone healing disturbances | Bone marrow concentrate | 101 | Autogenous bone marrow concentrate application is safe |
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| Giannini et al. 2009 [ | Osteochondral talus defects | arthroscopic-assisted injection of autologous bone marrow aspirate | 48 | Functional improvement |
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| Dallari et al. 2007 [ | High tibial osteotomy | Lyophilized bone chips with platelets-enriched plasma with bone marrow aspirate | 33 | Lyophilized bone chips with platelets-enriched plasma with or without bone marrow aspirate enhance healing |
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| Kitoh et al. 2009 [ | femoral and tibial lengthenings | Application of MSC expanded | 28 (51 osteotomies) | No enhancement of bone healing by MSC/PRP |