Post-Stroke Spastic Movement Disorder and Botulinum Toxin A Therapy: Early Detection And Early Injection.

IF 2.9 Q1 REHABILITATION Annals of Rehabilitation Medicine-ARM Pub Date : 2023-10-01 Epub Date: 2023-10-23 DOI:10.5535/arm.23108
Jörg Wissel, Anatol Kivi
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Abstract

Post-stroke spastic movement disorder (PS-SMD) develops in up to 40% of stroke survivors after a first ever stroke within the first year. Chronic PS-SMD is often associated with severe disabilities and complications, emphasizing the importance of its early recognition and early adequate management. Extensive research has aimed to accurately predict and sensitively detect a PS-SMD. Symptomatic therapies include conventional rehabilitation and local intramuscular injections of botulinum toxin A (BoNT-A). The latter is widely used, but primarily in the chronic phase of stroke. However, recent studies have shown the safety and efficacy of BoNT-A therapy even in the acute phase and early sub-acute phase after stroke, i.e., within three months post-stroke, leading to an improved long-term outcome in stroke rehabilitation. Local BoNT-A injections evolve as the primary approach in focal, multifocal, and segmental chronic or acute/subacute PS-SMD. Patients at high risk for or manifest PS-SMD should be identified by an early spasticity risk assessment. By doing so, PS-SMD can be integral part of the patient-centered goal-setting process of a multiprofessional spasticity-experienced team. The benefit of an early PS-SMD treatment by BoNT-A should predominate putative degenerative muscle changes due to long-term BoNT-A therapy by far. This, as early treatment effectively avoids complications typically associated with a PS-SMD, i.e., contractures, pain, skin lesions. The management of PS-SMD requires a comprehensive and multidisciplinary approach. Early assessment, patient-centered goal setting, early intervention, and early use of BoNT-A therapy prevents from PS-SMD complications and may improve rehabilitation outcome after stroke.

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中风后痉挛性运动障碍和肉毒杆菌毒素A治疗:早期发现和早期注射。
在第一年内首次中风后,高达40%的中风幸存者会出现中风后痉挛性运动障碍(PS-SMD)。慢性PS-SMD通常与严重残疾和并发症有关,强调了早期识别和早期充分管理的重要性。广泛的研究旨在准确预测和灵敏地检测PS-SMD。症状治疗包括常规康复和局部肌肉注射肉毒杆菌毒素A(BoNT-A)。后者被广泛使用,但主要用于中风的慢性期。然而,最近的研究表明,即使在中风后的急性期和早期亚急性期,即中风后三个月内,BoNT-A治疗也具有安全性和有效性,从而改善了中风康复的长期结果。局部BoNT-A注射逐渐成为局灶性、多灶性和节段性慢性或急性/亚急性PS-SMD的主要方法。应通过早期痉挛风险评估确定PS-SMD高危或表现为PS-SMD的患者。通过这样做,PS-SMD可以成为多专业痉挛经验团队以患者为中心的目标设定过程中不可或缺的一部分。到目前为止,BoNT-A早期PS-SMD治疗的益处应该主要是由于长期BoNT-A治疗引起的假定的退行性肌肉变化。这是因为早期治疗有效地避免了通常与PS-SMD相关的并发症,即挛缩、疼痛和皮肤损伤。PS-SMD的管理需要一种全面和多学科的方法。早期评估、以患者为中心的目标设定、早期干预和早期使用BoNT-A治疗可以预防PS-SMD并发症,并可能改善中风后的康复结果。
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来源期刊
CiteScore
2.50
自引率
7.70%
发文量
32
审稿时长
30 weeks
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