Daniel Patschan, Susann Patschan, Igor Matyukhin, Meike Hoffmeister, Martin Lauxmann, Oliver Ritter, Werner Dammermann
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The following databases were searched for references: PubMed, Web of Science, Cochrane Library, Scopus. The period lasted from 1940 until 2022. The following terms were utilized: \"acute kidney injury\" OR \"acute renal failure\" OR \"AKI\" AND \"metabolomics\" OR \"metabolic profiling\" OR \"omics\" AND \"ischemic\" OR \"toxic\" OR \"drug-induced\" OR \"sepsis\" OR \"LPS\" OR \"cisplatin\" OR \"cardiorenal\" OR \"CRS\" AND \"mouse\" OR \"mice\" OR \"murine\" OR \"rats\" OR \"rat\". Additional search terms were \"cardiac surgery\", \"cardiopulmonary bypass\", \"pig\", \"dog\", and \"swine\". In total, 13 studies were identified. Five studies were related to ischemic, seven studies to toxic (lipopolysaccharide (LPS), cisplatin), and one study to heat shock-associated AKI. Only one study, related to cisplatin-induced AKI, was performed as a targeted analysis. 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引用次数: 2
摘要
急性肾损伤(AKI)影响越来越多的住院患者在中欧和美国,预后仍然很差。尽管在确定诱发和延续AKI的分子/细胞过程方面取得了实质性进展,但缺乏更综合的病理生理观点。代谢组学能够从生物标本(如某些类型的液体或组织)中识别低分子量(< 1.5 kD)物质。本文的目的是回顾关于实验性AKI代谢谱的文献,并回答代谢组学是否允许在缺血性和中毒性AKI中整合不同的病理生理事件,如小管病变和微血管病变。检索了以下数据库:PubMed, Web of Science, Cochrane Library, Scopus。这一时期从1940年持续到2022年。使用了以下术语:“急性肾损伤”或“急性肾功能衰竭”或“AKI”和“代谢组学”或“代谢谱”或“组学”和“缺血”或“毒性”或“药物诱导”或“败血症”或“LPS”或“顺铂”或“心肾”或“CRS”和“小鼠”或“小鼠”或“大鼠”或“大鼠”。其他搜索词包括“心脏手术”、“体外循环”、“猪”、“狗”和“猪”。总共确定了13项研究。五项研究与缺血性有关,七项研究与毒性(脂多糖(LPS),顺铂)有关,一项研究与热休克相关的AKI有关。只有一项与顺铂诱导的AKI相关的研究被作为靶向分析进行。大多数研究发现缺血/给药LPS或顺铂后多种代谢恶化(如氨基酸、葡萄糖、脂质代谢)。特别是,在几乎所有的实验条件下,脂质稳态都表现出异常。lps诱导的AKI很可能与色氨酸代谢的改变有关。代谢组学研究为缺血性、中毒性或其他类型AKI中导致功能损伤/结构损伤的不同过程之间的病理生理联系提供了更深入的了解。
Metabolomics in Acute Kidney Injury: The Experimental Perspective.
Acute kidney injury (AKI) affects increasing numbers of in-hospital patients in Central Europe and the USA, the prognosis remains poor. Although substantial progress has been achieved in the identification of molecular/cellular processes that induce and perpetuate AKI, more integrated pathophysiological perspectives are missing. Metabolomics enables the identification of low-molecular-weight (< 1.5 kD) substances from biological specimens such as certain types of fluid or tissue. The aim of the article was to review the literature on metabolic profiling in experimental AKI and to answer the question if metabolomics allows the integration of distinct pathophysiological events such as tubulopathy and microvasculopathy in ischemic and toxic AKI. The following databases were searched for references: PubMed, Web of Science, Cochrane Library, Scopus. The period lasted from 1940 until 2022. The following terms were utilized: "acute kidney injury" OR "acute renal failure" OR "AKI" AND "metabolomics" OR "metabolic profiling" OR "omics" AND "ischemic" OR "toxic" OR "drug-induced" OR "sepsis" OR "LPS" OR "cisplatin" OR "cardiorenal" OR "CRS" AND "mouse" OR "mice" OR "murine" OR "rats" OR "rat". Additional search terms were "cardiac surgery", "cardiopulmonary bypass", "pig", "dog", and "swine". In total, 13 studies were identified. Five studies were related to ischemic, seven studies to toxic (lipopolysaccharide (LPS), cisplatin), and one study to heat shock-associated AKI. Only one study, related to cisplatin-induced AKI, was performed as a targeted analysis. The majority of the studies identified multiple metabolic deteriorations upon ischemia/the administration of LPS or cisplatin (e.g., amino acid, glucose, lipid metabolism). Particularly, abnormalities in the lipid homeostasis were shown under almost all experimental conditions. LPS-induced AKI most likely depends on the alterations in the tryptophan metabolism. Metabolomics studies provide a deeper understanding of pathophysiological links between distinct processes that are responsible for functional impairment/structural damage in ischemic or toxic or other types of AKI.
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