幼猪应用大剂量甲氨蝶呤治疗引起急性肾损伤的早期临床指标。

Frontiers in nephrology Pub Date : 2023-09-12 eCollection Date: 2023-01-01 DOI:10.3389/fneph.2023.1193494
Randal K Buddington, Thomas Wong, Karyl K Buddington, Torben S Mikkelsen, Xueyuan Cao, Scott C Howard
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摘要

引言:早期发现高剂量甲氨蝶呤(HDMTX)引起的肾清除率受损,对于及时采取干预措施,减少急性肾损伤和MTX诱导的全身毒性至关重要。方法:在不进行大容量碱化水合治疗的情况下,给42头幼猪输注4g/kg(80g/m2)MTX 4小时,诱导急性肾损伤(AKI)。在长达148小时的15个时间点测量血清肌酸酐和MTX的浓度,在HDMTX输注开始后的前24小时内收集10个样本。结果:在最初的28小时内,81%的猪在一个或多个样本中的血清肌酐浓度增加,表明AKI(即增加>0.3g/dL)。HDMTX输注后最初4小时内血浆MTX清除率低于90%,并且开始输注后6小时和8小时的总血清肌酐增加大于0.3 g/dL,可预测28小时的AKI(分别为p<0.05和p<0.001)。输注结束时,肌酸酐浓度高于基线0.3 g/dL或血清MTX高于5000μmol/L的猪患严重AKI的风险增加。结论:我们的研究结果表明,在输注HDMTX结束时和输注后不久采集的血清样本可用于预测即将发生的AKI。猪模型可用于确定HDMTX诱导的AKI的生物学、环境和医源性风险因素,并评估保护肾功能、最大限度地减少急性肾损伤和降低全身毒性的干预措施。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Early clinical indicators of acute kidney injury caused by administering high-dose methotrexate therapy to juvenile pigs.

Introduction: Early identification of compromised renal clearance caused by high-dose methotrexate (HDMTX) is essential for initiating timely interventions that can reduce acute kidney injury and MTX-induced systemic toxicity.

Methods: We induced acute kidney injury (AKI) by infusing 42 juvenile pigs with 4 g/kg (80 g/m2) of MTX over 4 hours without high-volume alkalinizing hydration therapy. Concentrations of serum creatinine and MTX were measured at 15 time points up to 148 hours, with 10 samples collected during the first 24 hours after the start of the HDMTX infusion.

Results: During the first 28 hours, 81% of the pigs had increases in the concentrations of serum creatinine in one or more samples indicative of AKI (i.e., > 0.3g/dL increase). A rate of plasma MTX clearance of less than 90% during the initial 4 hours after the HDMTX infusion and a total serum creatinine increase at 6 and 8 hours after starting the infusion greater than 0.3 g/dL were predictive of AKI at 28 hours (p < 0.05 and p < 0.001, respectively). At conclusion of the infusion, pigs with a creatinine concentration more than 0.3 g/dL higher than baseline or serum MTX greater than 5,000 μmol/L had an increased risk of severe AKI.

Conclusions: Our findings suggest that serum samples collected at conclusion and shortly after HDMTX infusion can be used to predict impending AKI. The pig model can be used to identify biological, environmental, and iatrogenic risk factors for HDMTX-induced AKI and to evaluate interventions to preserve renal functions, minimize acute kidney injury, and reduce systemic toxicity.

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