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Minocycline enhances the mesenchymal stromal/stem cell pro-healing phenotype in triple antimicrobial-loaded hydrogels

机译:Minocycline增强三重加载抗生素的水凝胶中的间充质基质/干细胞促愈合表型

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摘要

Mesenchymal stromal/stem cells (MSCs) have demonstrated pro-healing properties including an anti-inflammatory cytokine profile and the promotion of angiogenesis via expression of growth factors in pre-clinical models. MSCs encapsulated in poly(ethylene glycol) diacrylate (PEGdA) and thiolated gelatin poly(ethylene glycol) (Gel-PEG-Cys) crosslinked hydrogels have led to controlled cellular presentation at wound sites with favorable wound healing outcomes. However, the therapeutic potential of MSC-loaded hydrogels may be limited by non-specific protein adsorption on the delivery matrix that could facilitate the initial adhesion of microorganisms and subsequent virulent biofilm formation. Antimicrobials loaded concurrently in the hydrogels with MSCs could reduce microbial bioburden and promote healing, but the antimicrobial effect on the MSC wound healing capacity and the antibacterial efficacy of the hydrogels is unknown. We demonstrate that minocycline specifically induces a favorable change in MSC migration capacity, proliferation, gene expression, extracellular matrix (ECM) attachment, and adhesion molecule and growth factor release with subsequent increased angiogenesis. We then demonstrate that hydrogels loaded with MSCs, minocycline, vancomycin, and linezolid can significantly decrease bacterial bioburden. Our study suggests that minocycline can serve as a dual mechanism for the regenerative capacity of MSCs and the reduction of bioburden in triple antimicrobial-loaded hydrogels.
机译:间充质基质/干细胞(MSC)已被证明具有治疗前的特性,包括抗炎性细胞因子谱以及通过在临床前模型中表达生长因子促进血管新生。封装在聚乙二醇二丙烯酸酯(PEGdA)和硫醇化明胶聚乙二醇(Gel-PEG-Cys)交联水凝胶中的MSC已导致伤口处的细胞呈现受控状态,并具有良好的伤口愈合效果。但是,负载MSC的水凝胶的治疗潜力可能受到非特异性蛋白质在输送基质上的吸附的限制,这可能会促进微生物的初始粘附以及随后形成有毒的生物膜。在水凝胶中与MSC同时加载的抗菌剂可以减少微生物的负担并促进愈合,但是对MSC伤口愈合能力的抗菌作用和水凝胶的抗菌功效尚不清楚。我们证明,米诺环素会特异性地诱导MSC迁移能力,增殖,基因表达,细胞外基质(ECM)附着,粘附分子和生长因子释放的有利变化,并随后增加血管生成。然后,我们证明了装有MSC,米诺环素,万古霉素和利奈唑胺的水凝胶可以显着减少细菌的生物负荷。我们的研究表明,米诺环素可以充当双重机制,提高MSC的再生能力并降低三重载有抗菌剂的水凝胶的生物负荷。

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