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同时抑制 C5 和 CD14 可限制猪创伤后多器官功能障碍中的炎症反应。

Simultaneous C5 and CD14 inhibition limits inflammation and organ dysfunction in pig polytrauma.

机构信息

Institute of Clinical and Experimental Trauma Immunology, University Hospital Ulm, Ulm, Germany.

Department of Orthopedics, Trauma and Reconstructive Surgery, Rheinisch-Westfalische Technische Hochschule (RWTH) Aachen University, Aachen, Germany.

出版信息

Front Immunol. 2022 Aug 18;13:952267. doi: 10.3389/fimmu.2022.952267. eCollection 2022.

Abstract

Dysfunctional complement activation and Toll-like receptor signaling immediately after trauma are associated with development of trauma-induced coagulopathy and multiple organ dysfunction syndrome. We assessed the efficacy of the combined inhibition therapy of complement factor C5 and the TLR co-receptor CD14 on thrombo-inflammation and organ damage in an exploratory 72-h polytrauma porcine model, conducted under standard surgical and intensive care management procedures. Twelve male pigs were subjected to polytrauma, followed by resuscitation (ATLS guidelines) and operation of the femur fracture (intramedullary nailing technique). The pigs were allocated to combined C5 and CD14 inhibition therapy group (n=4) and control group (n=8). The therapy group received intravenously C5 inhibitor (RA101295) and anti-CD14 antibody (rMil2) 30 min post-trauma. Controls received saline. Combined C5 and CD14 inhibition reduced the blood levels of the terminal complement complex (TCC) by 70% (p=0.004), CRP by 28% (p=0.004), and IL-6 by 52% (p=0.048). The inhibition therapy prevented the platelet consumption by 18% and TAT formation by 77% (p=0.008). Moreover, the norepinephrine requirements in the treated group were reduced by 88%. The inhibition therapy limited the organ damage, thereby reducing the blood lipase values by 50% (p=0.028), LDH by 30% (p=0.004), AST by 33%, and NGAL by 30%. Immunofluorescent analysis of the lung tissue revealed C5b-9 deposition on blood vessels in five from the untreated, and in none of the treated animals. In kidney and liver, the C5b-9 deposition was similarly detected mainly the untreated as compared to the treated animals. Combined C5 and CD14 inhibition limited the inflammatory response, the organ damage, and reduced the catecholamine requirements after experimental polytrauma and might be a promising therapeutic approach.

摘要

功能失调的补体激活和 Toll 样受体信号在创伤后立即与创伤诱导的凝血功能障碍和多器官功能障碍综合征的发展相关。我们评估了补体因子 C5 和 TLR 共受体 CD14 的联合抑制疗法对标准手术和强化护理管理程序下探索性 72 小时多发伤猪模型中血栓炎症和器官损伤的疗效。12 只雄性猪经历多发伤,随后进行复苏(ATLS 指南)和股骨骨折手术(髓内钉技术)。猪被分配到联合 C5 和 CD14 抑制治疗组(n=4)和对照组(n=8)。治疗组在创伤后 30 分钟内静脉给予 C5 抑制剂(RA101295)和抗-CD14 抗体(rMil2)。对照组给予生理盐水。联合 C5 和 CD14 抑制使终末补体复合物(TCC)的血液水平降低了 70%(p=0.004),C 反应蛋白降低了 28%(p=0.004),白细胞介素-6 降低了 52%(p=0.048)。抑制疗法使血小板消耗减少了 18%,TAT 形成减少了 77%(p=0.008)。此外,治疗组的去甲肾上腺素需求减少了 88%。抑制疗法限制了器官损伤,从而使血液脂肪酶值降低了 50%(p=0.028),LDH 降低了 30%(p=0.004),AST 降低了 33%,NGAL 降低了 30%。肺组织的免疫荧光分析显示,在未治疗的 5 只动物的血管上有 C5b-9 沉积,而在治疗的动物中没有。在肾脏和肝脏中,C5b-9 沉积主要在未治疗的动物中被检测到,而在治疗的动物中则没有。联合 C5 和 CD14 抑制限制了炎症反应、器官损伤,并减少了实验性多发伤后的儿茶酚胺需求,可能是一种有前途的治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0505/9433645/631ec9fbbdef/fimmu-13-952267-g001.jpg

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