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Poly(ethylene glycol)-containing hydrogels promote the release of primary granules from human blood-derived polymorphonuclear leukocytes

机译:含聚乙二醇的水凝胶促进人类血液来源的多形核白细胞释放初级颗粒

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摘要

Polymorphonuclear leukocytes (PMNs) are recruited to sites of injury and biomaterial implants. Once activated, PMNs can exocytose their granule subsets to recruit monocytes (MCs) and mediate MC/macrophage activation. We investigated the release of myeloperoxidase (MPO), a primary granule marker, and matrix metalloproteinase-9 (MMP-9), a tertiary granule marker, from human blood-derived PMNs cultured on poly(ethylene glycol) (PEG) hydrogels, polydimethylsiloxane (PDMS), tissue culture polystyrene (TCPS) and gelatin-PEG (GP) hydrogels, with and without the presence of the bacterial peptide formyl-Met-Leu-Phe. Supernatants from PMN cultures on PEG-containing hydrogels (i.e., PEG and GP hydrogels) had higher concentrations of MPO than those from PMN cultures on PDMS or TCPS at 2 hours. PMNs on all biomaterials released comparable levels of MMP-9 at 2 hours, indicating that PMNs cultured on PEG-containing hydrogels have different mechanisms of release for primary and tertiary granules. Src family kinases were involved in the release of MPO from PMNs cultured on PEG hydrogels, TCPS and GP hydrogels and in the release of MMP-9 from PMNs cultured on all four materials. The increased release of primary granules from PMNs on PEG-containing hydrogels did not significantly increase MC chemotaxis, indicating that additional co-effectors in the dynamic inflammatory milieu in vivo modulate PMN-mediated MC recruitment.
机译:多形核白细胞(PMN)被募集到受伤部位和生物材料植入物。激活后,PMN可以将其颗粒子集胞吞,以募集单核细胞(MC)并介导MC /巨噬细胞激活。我们研究了从人类血液来源的PMN上培养的聚乙二醇(PEG)水凝胶,聚二甲基硅氧烷中释放的主要颗粒标记物髓过氧化物酶(MPO)和第三级颗粒标记物基质金属蛋白酶9(MMP-9)的释放(PDMS),组织培养聚苯乙烯(TCPS)和明胶-PEG(GP)水凝胶,无论是否存在细菌肽甲酰-Met-Leu-Phe。在2小时内,来自含PEG的水凝胶(即PEG和GP水凝胶)上PMN培养物的上清液的MPO浓度高于来自PDMS或TCPS上PMN培养物的上清液。所有生物材料上的PMN在2小时内释放出可比较的MMP-9水平,这表明在含PEG的水凝胶上培养的PMN具有不同的释放初级和第三级颗粒的机制。 Src家族激酶参与从PEG水凝胶,TCPS和GP水凝胶上培养的PMN释放MPO,以及从在所有四种材料上培养的PMN释放MMP-9。在含PEG的水凝胶上从PMNs释放初级颗粒的增加并未显着增加MC趋化性,表明体内动态炎症环境中的其他协同效应因子可调节PMN介导的MC募集。

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