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RESEARCH PRODUCT

Heterogeneity of biomaterial-induced multinucleated giant cells: Possible importance for the regeneration process?

Shahram GhanaatiShahram GhanaatiCharles James KirkpatrickMike BarbeckMike BarbeckClaudio MigliaresiAntonella MottaRobert Sader

subject

0301 basic medicineRegeneration (biology)Metals and AlloysBiomedical EngineeringMacrophage polarizationBiomaterialInflammationC-C chemokine receptor type 702 engineering and technologyBiology021001 nanoscience & nanotechnologyCell biologyBiomaterials03 medical and health sciencesChemokine receptor030104 developmental biologyGiant cellCeramics and Compositesmedicinemedicine.symptom0210 nano-technologyMannose receptorBiomedical engineering

description

Biomaterial-associated multinucleated giant cells (BMGCs) have been found within the implantation beds of many different biomaterials. However, their exact differentiation and their involvement in the inflammatory and healing events of the foreign body response still remain mostly unclear. Silk fibroin (SF) scaffolds, which induces a tissue reaction involving both macrophages and BMGCs, was implanted in the subcutaneous connective tissue of four CD-1 mice for 15 days using an established subcutaneous implantation model. Analysis of macrophage polarization and BMGCs was performed by immunohistochemcial detection of pro- (cyclooxygenase-2 (COX-2), C-C chemokine receptor type 7 (CCR7), nuclear factor "kappa-light-chain-enhancer" (NF-κB)) and anti-(heme oxygenase-1 (HO-1) and mannose receptor (MR, also known as CD206)). Furthermore, histochemical detection of tartrate-resistant acid phosphatase (TRAP) was conducted to test its predictive efficiency for the pro-inflammatory differentiation of cells. An established system for histomorphometrical analysis was used for counting of BMGCs expressing these molecules. The results show that BMGCs express both pro- and anti-inflammatory molecules within the implantation beds of SF scaffolds in comparable numbers, while only statistically significantly lower numbers of TRAP-positive BMGCs were measured in comparison to the BMGCs expressing the above-mentioned molecules. As these data substantiate the heterogeneity of BMGCs, the question arises to what extent BMGCs can "support" the process of tissue regeneration. Furthermore, the data prompt the question to what extent TRAP-expression within a biomaterial implantation bed can be seen as a predictive marker for an inflammatory condition, as in this study no obvious correlation between TRAP-expression and other pro-inflammatory markers could be observed.

https://doi.org/10.1002/jbm.a.35579