英夫利昔单抗 CT-P13 皮下注射在克罗恩病 14 天治疗周期内可使药物水平保持稳定。

Subcutaneous injection of infliximab CT-P13 results in stable drug levels within 14-day treatment cycle in Crohn's disease.

机构信息

Department of Gastroenterology, University Hospital of Saint-Etienne, Saint-Etienne, France.

CIRI (Centre International de Recherche en Infectiologie), Université Claude Bernard Lyon 1, INSERM U1111, CNRS, UMR5308, ENS Lyon, Université Jean Monnet de Saint-Etienne, France.

出版信息

Aliment Pharmacol Ther. 2022 Jul;56(1):77-83. doi: 10.1111/apt.16852. Epub 2022 Feb 28.

DOI:10.1111/apt.16852

PMID:35229331

Abstract

UNLABELLED

The new subcutaneous (sc) formulation of the infliximab (IFX) biosimilar CT-P13 results in homogeneous serum trough concentrations of IFX at steady state. The present study aimed to investigate in Crohn's disease (CD) patients the intra-individual variations of IFX drug levels at multiple time-points during 2 consecutive cycles of maintenance therapy with CT-P13 sc.

PATIENTS AND METHODS

CD patients in clinico-biological remission under maintenance therapy with intravenous (iv) IFX/CT-P13 were switched to CT-P13 sc 8 weeks (W) after the last infusion. They were treated with CT-P13 sc, 120 mg every 2 W. Assessments were performed from 8 W after starting CT-P13 sc and patients had to attend 6 visits on 2 consecutive cycles of treatment (cycles A and B). Visits were scheduled on days 4-6 (visit 1), days 7-9 (visit 2) and day 14 (visit 3) of each cycle, where days 1 and 14 were the days of sc injection of CT-P13. At each visit, peripheral blood was collected to measure serum IFX levels and anti-drug antibodies.

RESULTS

Twenty patients underwent 120 evaluations. Large intra-individual variations of serum drug levels of IFX were observed. When pooling the 120 evaluations, the mean drug level was 11.3 ± 4.9 μg/ml, and the median drug level was 10.9 μg/ml (IQR 7.5-15.5). During each cycle, the median drug levels were similar between visits 1 and 2 as well as between visits 1 and 3 and between visits 2 and 3. In cycle A, median drug levels were 11.1 μg/ml (7.8-14.5), 12.0 μg/ml (7.2-16.1) and 11.0 μg/ml (7.5-15.1) at V1, V2 and V3, respectively. Similar results were obtained in cycle B, where median drug levels were 11.6 μg/ml (7.9-14.9), 11.4 μg/ml (8.1-15.2) and 10.9 μg/ml (7.9-15.6) at V1, V2 and V3, respectively. In univariate analysis, we failed to identify factors predictive of low drug levels.

CONCLUSIONS

IFX drug levels are quite stable within 14-day treatment cycle, without trough levels in CD patients in remission during the maintenance therapy with CT-P13 sc. In patients with inactive CD under maintenance therapy with CT-P13 sc, therapeutic drug monitoring of IFX can be performed at any time between two CT-P13 sc injections.

摘要

目的

本研究旨在探讨接受 CT-P13 皮下（sc）治疗的克罗恩病（CD）患者在接受 CT-P13 sc 维持治疗的 2 个连续周期中，在药物水平的多个时间点上的个体内变异性。

方法

正在接受静脉（iv）IFX/CT-P13 维持治疗且临床和生物学缓解的 CD 患者在最后一次输注后 8 周（W）转换为 CT-P13 sc。他们接受 CT-P13 sc，每 2 W 给予 120mg。从开始 CT-P13 sc 后 8 W 开始进行评估，患者必须在 2 个连续治疗周期（周期 A 和 B）中接受 6 次就诊。就诊时间安排在每个周期的第 4-6 天（就诊 1）、第 7-9 天（就诊 2）和第 14 天（就诊 3），其中第 1 天和第 14 天是 sc 注射 CT-P13 的日子。每次就诊时，采集外周血以测量血清 IFX 水平和抗药物抗体。

结果

20 名患者接受了 120 次评估。IFX 血清药物水平的个体内变异性较大。当汇总 120 次评估时，平均药物水平为 11.3±4.9μg/ml，中位数药物水平为 10.9μg/ml（IQR 7.5-15.5）。在每个周期中，就诊 1 和 2 之间以及就诊 1 和 3 之间以及就诊 2 和 3 之间的中位数药物水平相似。在周期 A 中，就诊 1、就诊 2 和就诊 3 的中位数药物水平分别为 11.1μg/ml（7.8-14.5）、12.0μg/ml（7.2-16.1）和 11.0μg/ml（7.5-15.1）。在周期 B 中也得到了类似的结果，就诊 1、就诊 2 和就诊 3 的中位数药物水平分别为 11.6μg/ml（7.9-14.9）、11.4μg/ml（8.1-15.2）和 10.9μg/ml（7.9-15.6）。在单变量分析中，我们未能确定预测低药物水平的因素。