Division of Nephrology, Johns Hopkins University School of Medicine, Baltimore, MD, USA.
Crit Rev Clin Lab Sci. 2021 Aug;58(5):354-368. doi: 10.1080/10408363.2021.1879000. Epub 2021 Feb 8.
Despite advancements in standardizing the criteria for acute kidney injury (AKI), its definition remains based on changes in serum creatinine and urinary output that do not specifically represent tubular function or injury and that have significant limitations in the acute hospital setting. Much effort in nephrology has centered on identifying biomarkers of AKI to address these limitations. This review summarizes recent advances in our knowledge of biomarkers involved in pathophysiological processes during AKI and describes their potential clinical implications. Blood and urine biomarkers are released various mechanisms during renal tubular injury. Urinary kidney injury molecule-1 (KIM-1), liver-type fatty acid binding protein (L-FABP), insulin-like growth factor-binding protein-7 (IGFBP-7), and tissue inhibitor of metalloprotease-2 (TIMP-2) are released from the proximal tubule while uromodulin (UMOD) is secreted from the loop of Henle and neutrophil gelatinase-associated lipocalin (NGAL) is released from the distal tubule. These biomarkers could therefore be used to localize specific segments of injured tubules. Biomarkers also have diverse roles in pathophysiological processes in AKI, including inflammation, repair, and fibrosis. Current evidence suggests that these biomarkers could be used to predict the transition to chronic kidney disease (CKD), decrease discard of AKI kidneys, differentiate between kidney dysfunction and injury, guide AKI management, and improve diagnosis of diseases such as acute interstitial nephritis (AIN). They could differentiate between disease phenotypes, facilitate the inclusion of a homogenous patient population in future trials of AKI, and shed light on therapeutic pathways to prevent the transition from AKI to CKD. However, a major limitation of current biomarker research in AKI is the lack of tissue correlation. The Kidney Precision Medicine Project, a large-scale national effort, is currently underway to construct a kidney tissue atlas and expand the use of biomarkers to assess nephron health. Numerous biomarkers are involved in distinct pathophysiological processes after kidney injury and have demonstrated potential to improve diagnosis and risk stratification as well as provide a prognosis for patients with AKI. Some biomarkers are ready for use in clinical trials of AKI and could guide management in various clinical settings. Further investigation of these biomarkers will provide insight that can be applied to develop novel therapeutic agents for AKI.
尽管在急性肾损伤 (AKI) 的标准制定方面取得了进展,但它的定义仍然基于血清肌酐和尿排量的变化,这些变化并不能专门代表肾小管功能或损伤,并且在急性医院环境中存在很大的局限性。肾脏病学领域的大量努力都集中在确定 AKI 的生物标志物上,以解决这些局限性。这篇综述总结了我们在 AKI 病理生理过程中涉及的生物标志物的最新进展,并描述了它们的潜在临床意义。血液和尿液生物标志物是通过各种机制在肾小管损伤时释放的。尿肾损伤分子-1 (KIM-1)、肝型脂肪酸结合蛋白 (L-FABP)、胰岛素样生长因子结合蛋白-7 (IGFBP-7) 和组织金属蛋白酶抑制剂-2 (TIMP-2) 从近端肾小管释放,而尿调蛋白 (UMOD) 从 Henle 袢分泌,中性粒细胞明胶酶相关脂质运载蛋白 (NGAL) 从远端肾小管释放。因此,这些生物标志物可用于定位特定的损伤肾小管段。生物标志物在 AKI 的病理生理过程中也具有多种作用,包括炎症、修复和纤维化。目前的证据表明,这些生物标志物可用于预测向慢性肾脏病 (CKD) 的转变,减少 AKI 肾脏的丢弃,区分肾功能障碍和损伤,指导 AKI 管理,并改善急性间质性肾炎 (AIN) 等疾病的诊断。它们可以区分疾病表型,使同质患者人群能够纳入未来 AKI 的试验,并阐明预防从 AKI 到 CKD 转变的治疗途径。然而,目前 AKI 生物标志物研究的一个主要局限性是缺乏组织相关性。肾脏精准医学项目是一项大型的全国性努力,目前正在进行中,以构建肾脏组织图谱并扩大生物标志物的使用范围,以评估肾单位的健康状况。许多生物标志物参与了肾脏损伤后的不同病理生理过程,并已证明具有改善诊断和风险分层的潜力,并为 AKI 患者提供预后。一些生物标志物已经准备好用于 AKI 的临床试验,并可以指导各种临床环境中的管理。对这些生物标志物的进一步研究将提供可用于开发 AKI 新型治疗药物的见解。
