[Current status of multi-omics research on acute respiratory distress syndrome].

Ying Yang, Na Zang, Enmei Liu
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Abstract

Acute respiratory distress syndrome (ARDS) is a clinical syndrome characterized by diffuse alveolar and interstitial edema caused by damage to alveolar-capillary and epithelial cells, often induced by infection, sepsis, trauma, and other factors. It is marked by progressive hypoxemia and respiratory distress. Due to the diverse causes of ARDS, the unclear pathogenesis, and the absence of effective predictive markers or biomarkers, there are no effective treatment measures available, resulting in a high mortality rate. ARDS is increasingly recognized for its heterogeneity, biomarkers, and the emergence of new opportunities for the development of diagnostic tools and personalized treatment strategies provided by omics technologies. A single omics analysis cannot fully reveal the heterogeneity and complexity of ARDS, while multi-omics analysis can provide a more systematic and comprehensive understanding of ARDS. Using clinical samples is closer to the actual disease situation compared to animal models. Multi-omics studies based on clinical samples have achieved significant progress in elucidating the pathophysiology of ARDS, identifying ARDS subtypes, and identifying biomarkers related to ARDS. This review focuses on the current applications of genomics, transcriptomics, metabolomics, and proteomics analyses based on clinical samples in the ARDS field, with a focus on the application of these omics methods in ARDS heterogeneity, potential biomarkers, and pathogenesis. It also introduces the differences in the application of different clinical samples in ARDS omics research, in order to gain a deeper and more comprehensive understanding of the pathogenesis of ARDS and explore new strategies for its prevention and treatment.

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[急性呼吸窘迫综合征多组学研究现状]。
急性呼吸窘迫综合征(Acute respiratory distress syndrome, ARDS)是一种以肺泡毛细血管和上皮细胞损伤引起弥漫性肺泡和间质水肿为特征的临床综合征,常由感染、败血症、创伤等因素引起。其特点是进行性低氧血症和呼吸窘迫。由于ARDS病因多样,发病机制不明确,缺乏有效的预测标志物或生物标志物,没有有效的治疗措施,导致死亡率高。ARDS因其异质性、生物标志物以及组学技术提供的诊断工具和个性化治疗策略的发展新机会而日益得到认可。单一组学分析不能充分揭示ARDS的异质性和复杂性,而多组学分析可以更系统、更全面地了解ARDS。与动物模型相比,使用临床样本更接近实际疾病情况。基于临床样本的多组学研究在阐明ARDS病理生理、鉴定ARDS亚型、鉴定与ARDS相关的生物标志物等方面取得了重大进展。本文综述了基于临床样本的基因组学、转录组学、代谢组学和蛋白质组学分析在ARDS领域的应用现状,重点介绍了这些组学方法在ARDS异质性、潜在生物标志物和发病机制方面的应用。并介绍了不同临床样本在ARDS组学研究中的应用差异,以期更深入、更全面地了解ARDS的发病机制,探索其防治新策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Zhonghua wei zhong bing ji jiu yi xue
Zhonghua wei zhong bing ji jiu yi xue Medicine-Critical Care and Intensive Care Medicine
CiteScore
1.00
自引率
0.00%
发文量
42
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