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首页> 外文期刊>Seminars in Nephrology >Precision Medicine for Acute Kidney Injury (AKI): Redefining AKI by Agnostic Kidney Tissue Interrogation and Genetics
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Precision Medicine for Acute Kidney Injury (AKI): Redefining AKI by Agnostic Kidney Tissue Interrogation and Genetics

机译:急性肾损伤的精密药物(AKI):通过不良肾组织询问和遗传重新定义AKI

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Summary: Acute kidney injury (AKI) currently is diagnosed by a temporal trend of a single blood analyte: serum creatinine. This measurement is neither sensitive nor specific to kidney injury or its protean forms. Newer biomarkers, neutrophil gelatinase-associated lipocalin (NGAL, Lipocalin 2, Siderocalin), or kidney injury molecule-1 (KIM-1, Hepatitis A Virus Cellular Receptor 1), accelerate the diagnosis of AKI as well as prospectively distinguish rapidly reversible from prolonged causes of serum creatinine increase. Nonetheless, these biomarkers lack the capacity to subfractionate AKI further (eg, sepsis versus ischemia versus nephrotoxicity from medications, enzymes, or metals) or inform us about the primary and secondary sites of injury. It also is unknown whether all nephrons are injured in AKI, whether all cells in a nephron are affected, and whether injury responses can be stimulus-specific or cell type-specific or both. In this review, we summarize fully agnostic tissue interrogation approaches that may help to redefine AKI in cellular and molecular terms, including single-cell and single-nuclei RNA sequencing technology. These approaches will empower a shift in the current paradigm of AKI diagnosis, classification, and staging, and provide the renal community with a significant advance toward precision medicine in the analysis AKI.
机译:发明内容:急性肾损伤(AKI)目前被单血分析物的时间趋势诊断出:血清肌酐。该测量既不敏感,也不是肾损伤或其抗议形式。较新的生物标志物,中性粒细胞凝胶酶相关的脂素(Ngal,Lipocalin 2,Siderocalin)或肾损伤分子-1(Kim-1,甲型肝炎病毒受体1),加速AKI的诊断,并从长时间迅速地相反血清肌酐的原因增加。尽管如此,这些生物标志物缺乏进一步的次分析症的能力(例如,Sepsis与缺血与药物,酶或金属的肾毒性相比)或通知我们关于损伤的主要和次要部位。它还未知是否在AKI中损伤所有肾脏,无论是肾上腺中的所有细胞是否受到影响,是否损伤反应是刺激特异性或细胞类型特异性或两者。在本综述中,我们总结了完全不可知的组织询问方法,这可能有助于重新定义炎症和分子术语,包括单细胞和单细胞核RNA测序技术。这些方法将赋予目前AKI诊断,分类和分期范式的转变,并为肾社区提供了对分析AKI的精确药物的重大进步。

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