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Synergistic interactions of blood-borne immune cells, fibroblasts and extracellular matrix drive repair in an in vitro peri-implant wound healing model

机译:血型免疫细胞,成纤维细胞和细胞外基质驱动修复在体外植入伤口愈合模型中的协同相互作用

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Low correlations of cell culture data with clinical outcomes pose major medical challenges with costly consequences. While the majority of biomaterials are tested using in vitro cell monocultures, the importance of synergistic interactions between different cell types on paracrine signalling has recently been highlighted. In this proof-of-concept study, we asked whether the first contact of surfaces with whole human blood could steer the tissue healing response. This hypothesis was tested using alkali-treatment of rough titanium (Ti) surfaces since they have clinically been shown to improve early implant integration and stability, yet blood-free in vitro cell cultures poorly correlated with in vivo tissue healing. We show that alkali-treatment, compared to native Ti surfaces, increased blood clot thickness, including platelet adhesion. Strikingly, blood clots with entrapped blood cells in synergistic interactions with fibroblasts, but not fibroblasts alone, upregulated the secretion of major factors associated with fast healing. This includes matrix metalloproteinases (MMPs) to break down extracellular matrix and the growth factor VEGF, known for its angiogenic potential. Consequently, in vitro test platforms, which consider whole blood-implant interactions, might be superior in predicting wound healing in response to biomaterial properties.
机译:细胞培养数据与临床结果的低相关性具有昂贵的后果构成了主要的医疗挑战。虽然大多数生物材料使用体外细胞单一栽培进行测试,但最近突出了在旁静脉信号传导上不同细胞类型之间协同相互作用的重要性。在这种概念证明研究中,我们询问了整个人类血液的第一次接触是否可以转向组织愈合反应。使用粗钛(Ti)表面的碱处理测试了该假设,因为它们在临床上被证明改善早期植入物的整合和稳定性,但不含血液的体外细胞培养物与体内组织愈合不良相关。我们表明,与天然Ti表面相比,碱性处理增加,增加了血凝块厚度,包括血小板粘附。引人注目的是,血栓具有捕获的血细胞,其与成纤维细胞的协同相互作用,但单独的成纤维细胞,上调了与快速愈合相关的主要因素的分泌。这包括分解细胞外基质和生长因子VEGF的基质金属蛋白酶(MMP),以其血管生成潜力而已知。因此,考虑全血液植入物相互作用的体外测试平台可能在预测伤口愈合时响应于生物材料的伤口愈合。

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