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The use of cell cycle arrest biomarkers in the early detection of acute kidney injury. Is this the new renal troponin?

机译:在早期检测急性肾损伤中使用细胞周期阻滞生物标志物。这是新的肾肌钙蛋白吗?

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Acute kidney injury (AKI) has a high prevalence in critical care patients. Early detection might prevent patients from developing chronic kidney disease and requirement for renal replacement therapy. If we compare AKI with acute coronary syndrome, in which an increase in cardiac troponin may trigger early diagnosis and therapeutic intervention, we could extrapolate a similar technique in patients with early AKI without changes in urinary frequency or serum creatinine. The objective is to identify biomarker-positive, creatinine-negative patients that would allow therapeutic interventions to be initiated before finding changes in serum creatinine, preventing kidney damage. Tissue inhibitor of metalloproteinase 2 and insulin-like growth factor binding protein 7 are cell cycle arrest biomarkers that have demonstrated, in recent clinical trials, to have good sensitivity and specificity for early detection of AKI. Other recent studies have shown that the joint use of these biomarkers with serum creatinine and urine production could improve the prognosis of AKI in critical patients. The application of these biomarkers in clinical practice would enable the early identification of patients at risk of AKI, establishing interventions that would improve the survival of renal function.
机译:重症监护患者的急性肾损伤(AKI)患病率很高。早期发现可能会阻止患者发展为慢性肾脏疾病,并需要进行肾脏替代治疗。如果将AKI与急性冠状动脉综合征(其中心肌肌钙蛋白升高可能触发早期诊断和治疗干预)进行比较,我们可以推断出早期AKI患者的类似技术,而尿频或血清肌酐没有变化。目的是确定生物标志物阳性,肌酐阴性的患者,这些患者可以在发现血清肌酐变化之前启动治疗干预措施,以防止肾脏损害。金属蛋白酶2和胰岛素样生长因子结合蛋白7的组织抑制剂是细胞周期阻滞生物标志物,在最近的临床试验中已证明对AKI的早期检测具有良好的敏感性和特异性。最近的其他研究表明,将这些生物标志物与血清肌酐和尿液一起使用可以改善危重患者的AKI预后。这些生物标志物在临床实践中的应用将能够及早发现有AKI风险的患者,并建立可改善肾功能存活率的干预措施。

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