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Treatment of severe sepsis with nanoparticulate cell-free DNA scavengers

机译:用纳米颗粒无细胞DNA清除剂治疗严重脓毒症

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Severe sepsis represents a common, expensive, and deadly health care issue with limited therapeutic options. Gaining insights into the inflammatory dysregulation that causes sepsis would help develop new therapeutic strategies against severe sepsis. In this study, we identified the crucial role of cell-free DNA (cfDNA) in the regulation of the Toll-like receptor 9–mediated proinflammatory pathway in severe sepsis progression. Hypothesizing that removing cfDNA would be beneficial for sepsis treatment, we used polyethylenimine (PEI) and synthesized PEI-functionalized, biodegradable mesoporous silica nanoparticles with different charge densities as cfDNA scavengers. These nucleic acid–binding nanoparticles (NABNs) showed superior performance compared with their nucleic acid–binding polymer counterparts on inhibition of cfDNA-induced inflammation and subsequent multiple organ injury caused by severe sepsis. Furthermore, NABNs exhibited enhanced accumulation and retention in the inflamed cecum, along with a more desirable in vivo safety profile. Together, our results revealed a key contribution of cfDNA in severe sepsis and shed a light on the development of NABN-based therapeutics for sepsis therapy, which currently remains intractable.
机译:严重的败血症代表了普通,昂贵和致命的医疗保健问题,治疗有限。获得导致败血症的炎症性失调的见解将有助于为严重败血症产生新的治疗策略。在这项研究中,我们确定了无细胞DNA(CFDNA)在严重脓毒症进展中调节Toll样受体9介导的促炎途径中的关键作用。假设除去CFDNA将有利于败血症处理,我们使用聚乙基菊氨酸(PEI)和合成的PEI官能化的可生物降解的介孔二氧化硅纳米粒子,其具有不同的电荷密度作为CFDNA清除剂。与核酸结合聚合物对应物相比,这些核酸结合纳米颗粒(NABNS)与抑制CFDNA诱导的炎症和随后由严重败血症引起的多种器官损伤相比,表现出优异的性能。此外,NABNS在发炎的盲肠中表现出增强的积累和保留,以及更可取的体内安全性。我们的结果在一起揭示了CFDNA在严重败血症中的关键贡献,并阐明了败血症治疗基于NABN的治疗方法的光明,目前仍然是棘手的。

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