肥胖内科患者预防性使用依诺肝素的剂量及抗Xa水平
Prophylactic Enoxaparin Dosing and Anti-Xa Levels in Medicine Patients With Obesity.
作者信息
Phyo Wint War, Deodhar Karishma, Chang Amy, Blair Mary, Boyd Allison N, Geik Christopher
机构信息
Department of Pharmacy, Eskenazi Health, Indianapolis, IN, USA.
出版信息
J Pharm Technol. 2025 Mar 29:87551225251328255. doi: 10.1177/87551225251328255.
Previous studies have shown that the manufacturer's standard fixed dosing of enoxaparin for venous thromboembolism (VTE) prophylaxis leads to sub-prophylactic anti-Xa levels in medicine patients with obesity. Yet, there is limited literature describing higher dosing strategies in this patient population, and an optimal dosing regimen has not been well-established. The primary objective was to evaluate mean doses (mg/kg/d) of prophylactic enoxaparin that are associated with goal anti-Xa levels in medicine patients with obesity across 3 body mass index (BMI) groups (40-49 kg/m, 50-59 kg/m, ≥60 kg/m). This is a single-center, retrospective cohort study of adult patients (age ≥18 years) with BMI ≥40 kg/m admitted to a medicine team with at least 1 appropriately drawn anti-Xa level between January 2018 and July 2023. The institution's goal anti-Xa level for VTE prophylaxis was 0.2 to 0.4 units/mL. The primary outcome was the comparison of mean dose between those within anti-Xa at goal and not at goal. Secondary outcomes included the percentages of initial anti-Xa levels below, within, or above goal range and the incidence of new VTE and major bleeding events during hospitalization while on enoxaparin. All outcomes were stratified into 3 BMI groups: 40-49 kg/m, 50-59 kg/m, and ≥60 kg/m. Median dose of those with final anti-Xa level at goal was significantly higher than that of those not in goal anti-Xa range across all 3 BMI groups (0.57 vs 0.50 mg/kg/d; < 0.05). The majority of the initial anti-Xa levels were subprophylactic, with only 35.7% of patients (or 75 of 210 patients) had initial anti-Xa within the goal range. There were no statistically significant differences in the number of blood transfusions or VTE events between the groups. Findings suggest that medicine patients with BMI ≥40 kg/m may require enoxaparin doses higher than 0.5 mg/kg/d to reach goal prophylactic anti-Xa level. However, more robust data are necessary to further validate these results and the clinical implications.
先前的研究表明,制造商用于静脉血栓栓塞(VTE)预防的依诺肝素标准固定剂量,在肥胖的内科患者中会导致抗Xa水平低于预防剂量。然而,描述该患者群体更高剂量策略的文献有限,且尚未确立最佳给药方案。主要目的是评估在3个体重指数(BMI)组(40 - 49kg/m²、50 - 59kg/m²、≥60kg/m²)的肥胖内科患者中,与目标抗Xa水平相关的预防性依诺肝素平均剂量(mg/kg/天)。这是一项单中心回顾性队列研究,研究对象为2018年1月至2023年7月期间入住内科团队、BMI≥40kg/m²且至少有1次抗Xa水平检测结果合适的成年患者(年龄≥18岁)。该机构预防VTE的目标抗Xa水平为0.2至0.4单位/毫升。主要结局是比较抗Xa水平达到目标和未达到目标的患者之间的平均剂量。次要结局包括初始抗Xa水平低于、处于或高于目标范围的百分比,以及住院期间使用依诺肝素时新发生VTE和大出血事件的发生率。所有结局均分为3个BMI组:40 - 49kg/m²、50 - 59kg/m²和≥60kg/m²。在所有3个BMI组中,最终抗Xa水平达到目标的患者的中位剂量显著高于抗Xa水平未达到目标范围的患者(0.57 vs 0.50mg/kg/天;P<0.05)。大多数初始抗Xa水平低于预防剂量,只有(210名患者中的)35.7%(即75名患者)的初始抗Xa水平在目标范围内。两组之间输血次数或VTE事件数量无统计学显著差异。研究结果表明,BMI≥40kg/m²的内科患者可能需要高于0.5mg/kg/天的依诺肝素剂量才能达到预防性抗Xa目标水平。然而,需要更有力的数据来进一步验证这些结果及其临床意义。
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