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The role of hyaluronic acid in SEB-induced acute lung inflammation

机译:透明质酸在SEB诱导的急性肺炎中的作用

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We investigated the role of the extracellular matrix component, hyaluronic acid (HA) in SEB-induced ALI/ARDS. Intranasal exposure of mice to SEB led to a significant increase in the level of soluble hyaluronic acid in the lungs. Similarly, in an endothelial cell/spleen cell co-culture, SEB exposure led to significant increases in soluble levels of hyaluronic acid, cellular proliferation, and cytokine production compared with SEB-exposed spleen cells or endothelial cells alone. Exposure of SEB-activated spleen cells to hyaluronic acid led to increased cellular proliferation and increased cytokine production. SEB-induced cytokine production and proliferation in vitro were significantly reduced by the hyaluronic acid blocking peptide, Pep-1. Finally, treatment of SEB-exposed mice with Pep-1 significantly reduced SEB-induced ALI/ARDS, through reduction of cytokine production and numbers of lung inflammatory cells, compared to mice treated with a control peptide. Together, these results suggest the possibility of targeting HA for the treatment of SEB-induced ALI/ARDS.
机译:我们研究了SEB诱导的Ali / ARDS中细胞外基质组分,透明质酸(HA)的作用。小鼠鼻内暴露于SEB导致肺中可溶性透明质酸水平的显着增加。类似地,在内皮细胞/脾细胞共培养中,SEB暴露导致可溶性水平的透明质酸,细胞增殖和细胞因子产生的显着增加,与单独的SEB暴露的脾细胞或内皮细胞相比。将SEB活化的脾细胞暴露于透明质酸导致细胞增殖增加和细胞因子产生增加。透明质酸阻断肽,PEP-1,SEB诱​​导的细胞因子产生和增殖显着降低。最后,与用对照肽处理的小鼠的细胞因子产生和数量的细胞因子产生和数量,通过减少细胞因子产生和数量,通过减少细胞因子产生和数量的细胞因子产生和数量,治疗SEB暴露的小鼠。这些结果表明,靶向HA的可能性用于治疗SEB诱导的ALI / ARDS。

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