Department of Translational Medical Sciences, University of Campania "Luigi Vanvitelli" - Monaldi Hospital, Via Leonardo Bianchi, Naples, Italy.
Unit of Clinical Pharmacology, Fatebenefratelli-Sacco University Hospital, Milano, Italy.
Clin Ther. 2021 Sep;43(9):e255-e263. doi: 10.1016/j.clinthera.2021.07.003. Epub 2021 Aug 6.
Direct oral anticoagulants (DOACs) are recommended in preference to vitamin K antagonists (VKAs) for stroke prevention in patients with atrial fibrillation (AF) eligible for oral anticoagulation therapy; however, data and clinical experiences supporting the use of DOACs in patients with a body mass index ≥40 kg/m or weight >120 kg remain limited. The aim of this study was to evaluate the pharmacokinetic properties of DOACs in patients with AF and extreme obesity.
We enrolled all consecutive patients with AF and extreme obesity undergoing treatment with DOACs followed up at Monaldi Hospital, Naples, Italy. To determine peak plasma and trough levels of DOACs, plasma samples were collected at 2nd, 4th, 6th, and 12th hours from the last dose intake in patients receiving apixaban and dabigatran and at the 2nd, 4th, 6th, and 24th hours in those receiving edoxaban and rivaroxaban. The DOACs' peak and trough plasma levels obtained from our study population were compared with those sourced from pharmacokinetic studies among patients without obesity, defined as a normal reference range in the literature. If at least 1 peak or trough plasma level was found below or above the normal reference ranges, the patients were classified as having out-of-range DOAC plasma levels. Study population was then divided into in-range and out-of-range groups. Baseline characteristics, including DOAC treatment, were compared between the 2 groups. Univariate and multivariate logistic regression analysis were performed to identify baseline variables associated with DOACs' plasma concentration out of the expected range.
A total of 58 patients (mean [SD] age, 70.93 [8.73] years; 40% female) with extreme obesity (mean [SD] body mass index. 44.43 [3.54] kg/m) and AF while undergoing DOAC treatment were included in the present study. In 9 patients (15.5 %), the DOAC plasma concentrations were out of the expected ranges (out-of-range group);, indicating a greater likelihood of edoxaban 30 mg treatment (33% vs 2%; P < 0.01) and inappropriate DOAC underdosing (56% vs 4%; P < 0.005) compared with the in-range group. According to the multivariate logistic analysis (P = 0.0011), the inappropriate DOAC underdosing (hazard ratio = 29.37; P = 0.0002) was an independent predictor of DOAC plasma levels out of the expected ranges.
Patients with extreme obesity and AF who were receiving DOAC therapy had DOAC plasma concentrations in the expected range. The inappropriate DOAC underdosing seems to be the only independent clinical factor associated with a plasma concentration of the drug out of the expected range.
对于有口服抗凝治疗适应证的心房颤动(AF)患者,推荐直接口服抗凝剂(DOACs)而非维生素 K 拮抗剂(VKAs)用于卒中预防;然而,支持 DOAC 在体重指数≥40kg/m2 或体重>120kg 的患者中应用的数据和临床经验仍然有限。本研究旨在评估 DOAC 在极度肥胖的 AF 患者中的药代动力学特征。
我们纳入了在意大利那不勒斯 Monaldi 医院接受 DOAC 治疗并随访的所有连续的极度肥胖 AF 患者。为了确定 DOAC 的峰值和谷值血浆浓度,在服用阿哌沙班和达比加群的患者中,在末次剂量后第 2、4、6 和 12 小时,以及服用依度沙班和利伐沙班的患者中,在末次剂量后第 2、4、6 和 24 小时采集血浆样本。我们的研究人群中的 DOAC 峰值和谷值血浆浓度与无肥胖患者(文献中定义的正常参考范围)的药代动力学研究中的浓度进行了比较。如果至少有 1 个峰值或谷值血浆水平低于或高于正常参考范围,则将患者分类为 DOAC 血浆水平超出范围。然后,将研究人群分为在范围内和超出范围两组。比较两组之间的基线特征,包括 DOAC 治疗。使用单变量和多变量逻辑回归分析确定与 DOAC 血浆浓度超出预期范围相关的基线变量。
本研究共纳入 58 例(平均[标准差]年龄,70.93[8.73]岁;40%为女性)极度肥胖(平均[标准差]体重指数,44.43[3.54]kg/m2)且正在接受 DOAC 治疗的 AF 患者。在 9 例患者(15.5%)中,DOAC 血浆浓度超出预期范围(超出范围组);与在范围内组相比,EDOX 30mg 治疗的可能性更大(33% vs 2%;P<0.01),且 DOAC 剂量不足的可能性更大(56% vs 4%;P<0.005)。根据多变量逻辑分析(P=0.0011),DOAC 剂量不足(风险比=29.37;P=0.0002)是 DOAC 血浆水平超出预期范围的独立预测因素。
接受 DOAC 治疗的极度肥胖 AF 患者的 DOAC 血浆浓度在预期范围内。DOAC 剂量不足似乎是与药物血浆浓度超出预期范围唯一相关的独立临床因素。
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