DAMPs, PAMPs和PRRs在创伤性炎症中的转化和临床意义。

Archives of clinical and biomedical research Pub Date : 2022-01-01 Epub Date: 2022-08-26 DOI:10.26502/acbr.50170279
Vikrant Rai, Gillian Mathews, Devendra K Agrawal
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引用次数: 6

摘要

多器官功能衰竭(MOF)引起的多发创伤后发病率和死亡率的增加是临床医生关注的主要问题。全身性炎症反应综合征(SIRS)和败血症是主要的潜在原因。多发损伤后释放的损伤相关分子蛋白(DAMPs)诱导炎症免疫反应修复组织,然而,持续的炎症最终导致免疫抑制和MOF。在免疫抑制期间,创伤组织暴露于模式相关分子模式(PAMPs)进一步增加了引起败血症的炎症级联反应的连续性。这两种打击加重了病人的病情,增加了发病率和死亡率。因此,根据创伤严重程度和炎症生物标志物水平对患者进行分层并相应地设计治疗以获得更好的临床结果是至关重要的。虽然已经报道了多创伤后SIRS和MOF的一些分子机制,但与DAMPs和PAMPs研究相关的关键因素的信息有限,包括采样时间(创伤后经过的时间)、采样来源(血液、尿液、唾液)、蛋白质组学和代谢组学、多重血浆测定、各种来源结果的比较解释和诊断价值。并对翻译和临床意义进行了解释。此外,关于热休克蛋白、线粒体DNA、中性粒细胞胞外陷阱等DAMPs及其在SIRS和MOF中的作用的文献有限。此外,在一定的时间范围内区分SIRS和败血症的生物标志物对于获得更好的临床结果也很重要。这篇重要的综述集中在这些方面,以提供全面的信息和发人深省的讨论,以设计未来的调查和临床试验。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Translational and Clinical Significance of DAMPs, PAMPs, and PRRs in Trauma-induced Inflammation.

Translational and Clinical Significance of DAMPs, PAMPs, and PRRs in Trauma-induced Inflammation.

Increased morbidity and mortality after polytrauma due to multiple organ failure (MOF) is a major concern for clinicians. Systemic inflammatory response syndrome (SIRS) and sepsis are the major underlying causes. Damage-associated molecular proteins (DAMPs) released after polytrauma induce an inflammatory immune response to repair the tissue, however, persistent inflammation finally results in immunosuppression and MOF. During immunosuppression, additional exposure of the traumatized tissue to pattern-associated molecular patterns (PAMPs) further adds to the continuum of inflammatory cascade causing sepsis. These two hits worsen the condition of the patient and increase morbidity and mortality. Thus, it is critical to stratify the patient based on trauma severity and inflammatory biomarkers levels and design treatment accordingly for a better clinical outcome. Although some of the molecular mechanisms involved in SIRS and MOF after polytrauma have been reported, there is limited information on the critical factors related to the study of DAMPs and PAMPs, including the timing of sampling (time elapsed after trauma), source of sampling (blood, urine, saliva), proteomics and metabolomics, multiplex plasma assay, comparative interpretation of the results from various sources and diagnostic value, and interpretation on the translational and clinical significance. Additionally, there is limited literature on DAMPs like heat shock proteins, mitochondrial DNA, neutrophil extracellular traps, and their role in SIRS and MOF. Further, it is also important to distinguish between the biomarkers of SIRS and sepsis in a time-bound window to have a better clinical outcome. This critical review focuses on these aspects to provide comprehensive information and thought-provoking discussion to design future investigation and clinical trials.

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