A New Dosing Frontier: Retrospective Assessment of Effluent Flow Rates and Residual Renal Function Among Critically Ill Patients Receiving Continuous Renal Replacement Therapy

Critical Care Explorations Pub Date : 2024-03-22 DOI:10.1097/cce.0000000000001065

Damini Lakshmipathy, Xiaoyi Ye, J. Kuti, David P. Nicolau, Tomefa E. Asempa

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Abstract

In 2020, cefiderocol became the first Food and Drug Administration-approved medication with continuous renal replacement therapy (CRRT) dosing recommendations based on effluent flow rates (Q E). We aimed to evaluate the magnitude and frequency of factors that may influence these recommendations, that is, Q E intrapatient variability and residual renal function. Retrospective observational cohort study. ICUs within Hartford Hospital (890-bed, acute-care hospital) in Connecticut from 2017 to 2023. Adult ICU patients receiving CRRT for greater than 72 hours. CRRT settings including Q E and urine output (UOP) were extracted from the time of CRRT initiation (0 hr) and trends were assessed. To assess the impact on antibiotic dosing, cefiderocol doses were assigned to 0 hour, 24 hours, 48 hours, and 72 hours Q E values per product label, and the proportion of antibiotic dose changes required as a result of changes in inpatient’s Q E was evaluated. Among the 380 ICU patients receiving CRRT for greater than 72 hours, the median (interquartile range) 0 hour Q E was 2.96 (2.35–3.29) L/hr. Approximately 9 Q E values were documented per patient per 24-hour window. Q E changes of greater than 0.75 L/hr were observed in 21.6% of patients over the first 24 hours and in 7.9% (24–48 hr) and 5.8% (48–72 hr) of patients. Approximately 40% of patients had UOP greater than 500 mL at 24 hours post-CRRT initiation. Due to Q E changes within 24 hours of CRRT initiation, a potential cefiderocol dose adjustment would have been warranted in 38% of patients (increase of 21.3%; decrease of 16.6%). Q E changes were less common after 24 hours, warranting cefiderocol dose adjustments in less than 15% of patients. Results highlight the temporal and variable dynamics of Q E and prevalence of residual renal function. Data also demonstrate a risk of antibiotic under-dosing in the first 24 hours of CRRT initiation due to increases in Q E. For antibiotics with Q E-based dosing recommendations, empiric dose escalation may be warranted in the first 24 hours of CRRT initiation.

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剂量新领域：对接受持续肾脏替代疗法的重症患者的出血流量和残余肾功能进行回顾性评估

2020 年，头孢羟氨苄成为美国食品和药物管理局批准的首个根据出血流量（Q E）推荐连续性肾脏替代疗法（CRRT）剂量的药物。我们旨在评估可能影响这些建议的因素（即 Q E 在患者内部的变化和残余肾功能）的程度和频率。回顾性观察队列研究。 2017年至2023年康涅狄格州哈特福德医院（拥有890张病床的急症护理医院）内的重症监护病房。接受 CRRT 超过 72 小时的成人 ICU 患者。从 CRRT 启动时间（0 小时）开始提取 CRRT 设置，包括 Q E 和尿量（UOP），并评估其趋势。为了评估对抗生素剂量的影响，根据产品标签上的 Q E 值对 0 小时、24 小时、48 小时和 72 小时的头孢羟氨苄剂量进行了分配，并评估了因住院患者 Q E 值变化而需要改变抗生素剂量的比例。在接受 CRRT 超过 72 小时的 380 名重症监护病房患者中，0 小时 Q E 的中位数（四分位数间距）为 2.96 (2.35-3.29) 升/小时。每名患者在每个 24 小时窗口期记录了约 9 个 Q E 值。在头 24 小时内，21.6% 的患者观察到 Q E 变化超过 0.75 升/小时，7.9% 的患者（24-48 小时）和 5.8% 的患者（48-72 小时）观察到 Q E 变化超过 0.75 升/小时。大约 40% 的患者在 CRRT 启动后 24 小时内的尿量超过 500 毫升。由于 Q E 在 CRRT 启动后 24 小时内发生变化，38% 的患者可能需要调整头孢哌酮的剂量（增加 21.3%；减少 16.6%）。24 小时后 Q E 发生变化的情况较少，需要调整头孢羟氨苄剂量的患者不到 15%。结果凸显了 Q E 的时间性和可变动态以及残余肾功能的普遍性。数据还表明，在开始使用 CRRT 的前 24 小时内，由于 Q E 的增加，存在抗生素剂量不足的风险。

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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Critical Care Explorations

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