尿肌动蛋白作为脓毒症相关急性肾损伤的潜在标志物:一项初步研究。
Urinary actin, as a potential marker of sepsis-related acute kidney injury: A pilot study.
机构信息
Department of Laboratory Medicine, Medical School, University of Pécs, Pécs, Hungary.
Department of Anesthesiology and Intensive Therapy, Medical School, University of Pécs, Pécs, Hungary.
出版信息
PLoS One. 2021 Jul 26;16(7):e0255266. doi: 10.1371/journal.pone.0255266. eCollection 2021.
INTRODUCTION
A major complication of sepsis is the development of acute kidney injury (AKI). Recently, it was shown that intracellular actin released from damaged tissues appears in the urine of patients with multiple organ dysfunction syndrome. Our aims were to measure urinary actin (u-actin) concentrations of septic and control patients and to test if u-actin levels could predict AKI and mortality.
METHODS
Blood and urine samples were collected from septic and sepsis-related AKI patients at three time points (T1-3): T1: within 24 hours after admission; T2: second day morning; T3: third day morning of follow-up. Patients with malignancies needing palliative care, end-stage renal disease or kidney transplantation were excluded. Serum and u-actin levels were determined by quantitative Western blot. Patients were categorized by the Sepsis-3 and KDIGO AKI classifications.
RESULTS
In our study, 17 septic, 43 sepsis-induced AKI and 24 control patients were enrolled. U-actin levels were higher in septic patients compared with controls during follow-up (p<0.001). At T1, the septic and sepsis-related AKI groups also showed differences (p<0.001), yet this increase was not statistically significant at T2 and T3. We also detected significantly elevated u-actin concentrations in AKI-2 and AKI-3 septic patients compared with AKI-1 septic patients (p<0.05) at T1 and T3, along with a significant increase in AKI-2 septic patients compared with AKI-1 septic patients at T2 (p<0.01). This tendency remained the same when referring u-actin to urine creatinine. Parameters of first-day septic patient samples could discriminate AKI from non-AKI state (AUC ROC, p<0.001): u-actin: 0.876; se-creatinine: 0.875. Derived cut-off value for u-actin was 2.63 μg/L (sensitivity: 86.0%, specificity: 82.4%).
CONCLUSION
U-actin may be a complementary diagnostic biomarker to se-creatinine in sepsis-related AKI while higher u-actin levels also seem to reflect the severity of AKI. Further investigations may elucidate the importance of u-actin release in sepsis-related AKI.
介绍
脓毒症的一个主要并发症是急性肾损伤(AKI)的发生。最近,人们发现受损组织释放的细胞内肌动蛋白出现在多器官功能障碍综合征患者的尿液中。我们的目的是测量脓毒症和对照患者的尿肌动蛋白(u-actin)浓度,并检验 u-actin 水平是否可以预测 AKI 和死亡率。
方法
在三个时间点(T1-3)从脓毒症和脓毒症相关 AKI 患者采集血样和尿样:T1:入院后 24 小时内;T2:第二天早晨;T3:随访第三天早晨。排除患有姑息性治疗需要的恶性肿瘤、终末期肾病或肾移植的患者。通过定量 Western blot 测定血清和 u-actin 水平。根据 Sepsis-3 和 KDIGO AKI 分类对患者进行分类。
结果
在我们的研究中,纳入了 17 名脓毒症患者、43 名脓毒症诱导 AKI 患者和 24 名对照患者。与对照组相比,在随访期间脓毒症患者的 u-actin 水平更高(p<0.001)。在 T1,脓毒症和脓毒症相关 AKI 组之间也存在差异(p<0.001),但在 T2 和 T3 时这种增加没有统计学意义。我们还发现 AKI-2 和 AKI-3 脓毒症患者的 u-actin 浓度明显高于 AKI-1 脓毒症患者(p<0.05),在 T1 和 T3 时 AKI-2 脓毒症患者的 u-actin 浓度明显高于 AKI-1 脓毒症患者(p<0.01),而在 T2 时 AKI-2 脓毒症患者的 u-actin 浓度也明显高于 AKI-1 脓毒症患者(p<0.01)。当将 u-actin 与尿肌酐进行比较时,这种趋势仍然存在。第一天脓毒症患者样本的参数可以区分 AKI 与非 AKI 状态(AUC ROC,p<0.001):u-actin:0.876;血清肌酐:0.875。u-actin 的临界值为 2.63 μg/L(敏感性:86.0%,特异性:82.4%)。
结论
u-actin 可能是脓毒症相关 AKI 中血清肌酐的补充诊断生物标志物,而较高的 u-actin 水平似乎也反映了 AKI 的严重程度。进一步的研究可能阐明 u-actin 在脓毒症相关 AKI 中的重要性。
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