A型肉毒毒素治疗脑卒中后下肢远端痉挛：一项随机试验。

OnabotulinumtoxinA for the Treatment of Poststroke Distal Lower Limb Spasticity: A Randomized Trial.

机构信息

McGill University, Department of Neurology and Neurosurgery, L7 312 Montreal General Hospital, 1650 Cedar Avenue Montreal, QC H3G 1A4 QC, Canada.

MossRehab Gait and Motion Analysis Laboratory, Elkins Park, PA.

出版信息

PM R. 2018 Jul;10(7):693-703. doi: 10.1016/j.pmrj.2017.12.006. Epub 2018 Jan 9.

DOI:10.1016/j.pmrj.2017.12.006

PMID:29330071

Abstract

BACKGROUND

Poststroke distal lower limb spasticity impairs mobility, limiting activities of daily living and requiring additional caregiver time.

OBJECTIVE

To evaluate the efficacy, safety, and sustained benefit of onabotulinumtoxinA in adults with poststroke lower limb spasticity (PSLLS).

DESIGN

A multicenter, randomized, double-blind, phase 3, placebo-controlled trial (NCT01575054).

SETTING

Sixty study centers across North America, Europe, Russia, the United Kingdom, and South Korea.

PATIENTS

Adult patients (18-65 years of age) with PSLLS (Modified Ashworth Scale [MAS] ≥3) of the ankle plantar flexors and the most recent stroke ≥3 months before study enrollment.

INTERVENTIONS

During the open-label phase, patients received ≤3 onabotulinumtoxinA treatments (≤400 U) or placebo at approximately 12-week intervals. Treatments were into the ankle plantar flexors (onabotulinumtoxinA 300 U into ankle plantar flexors; ≤100 U, optional lower limb muscles).

MAIN OUTCOME MEASUREMENTS

The double-blind primary endpoint was MAS change from baseline (average score at weeks 4 and 6). Secondary measures included physician-assessed Clinical Global Impression of Change (CGI), MAS change from baseline in optional muscles, Goal Attainment Scale (GAS), and pain scale.

RESULTS

Of 468 patients enrolled, 450 (96%) completed the double-blind phase and 413 (88%) completed the study. Small improvements in MAS observed with onabotulinumtoxinA during the double-blind phase (onabotulinumtoxinA, -0.8; placebo, -0.6, P = .01) were further enhanced with additional treatments through week 6 of the third open-label treatment cycle (onabotulinumtoxinA/onabotulinumtoxinA, -1.2; placebo/onabotulinumtoxinA, -1.4). Small improvements in CGI observed during the double-blind phase (onabotulinumtoxinA, 0.9; placebo, 0.7, P = .01) were also further enhanced through week 6 of the third open-label treatment cycle (onabotulinumtoxinA/onabotulinumtoxinA, 1.6; placebo/onabotulinumtoxinA, 1.6). Physician- and patient-assessed GAS scores improved with each subsequent treatment. No new safety signals emerged.

CONCLUSIONS

OnabotulinumtoxinA significantly improved ankle MAS, CGI, and GAS scores compared with placebo; improvements were consistent and increased with repeated treatments of onabotulinumtoxinA over 1 year in patients with PSLLS.

LEVEL OF EVIDENCE

摘要

背景

脑卒中后下肢远端痉挛会影响活动能力，限制日常生活活动，并需要额外的护理人员时间。

目的

评估利鲁唑在脑卒中后下肢痉挛（PSLLS）成人患者中的疗效、安全性和持续获益。

设计

一项多中心、随机、双盲、III 期、安慰剂对照试验（NCT01575054）。

地点

北美、欧洲、俄罗斯、英国和韩国的 60 个研究中心。

患者

脑卒中后下肢痉挛患者（踝跖屈肌改良 Ashworth 量表 [MAS] ≥3），最近一次脑卒中发生在研究入组前≥3 个月。

干预措施

在开放性试验阶段，患者接受≤3 次利鲁唑治疗（≤400 U）或安慰剂，间隔约 12 周。治疗药物为踝跖屈肌（利鲁唑 300 U 入踝跖屈肌；≤100 U，可选下肢肌肉）。

主要观察指标

双盲主要终点为基线时 MAS 的变化（第 4 周和第 6 周的平均评分）。次要观察指标包括医生评估的临床总体印象变化（CGI）、基线时可选肌肉的 MAS 变化、目标实现量表（GAS）和疼痛量表。

结果

468 例患者中，450 例（96%）完成了双盲阶段，413 例（88%）完成了研究。在双盲阶段，利鲁唑观察到 MAS 有较小的改善（利鲁唑组-0.8，安慰剂组-0.6，P=0.01），通过第三轮开放性治疗周期的第 6 周进一步增强（利鲁唑组/利鲁唑组-1.2，安慰剂组/利鲁唑组-1.4）。双盲阶段观察到的 CGI 较小的改善（利鲁唑组 0.9，安慰剂组 0.7，P=0.01）也通过第三轮开放性治疗周期的第 6 周进一步增强（利鲁唑组/利鲁唑组 1.6，安慰剂组/利鲁唑组 1.6）。经后续治疗，医生和患者评估的 GAS 评分均有所改善。未出现新的安全性信号。