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肉毒毒素在脑瘫儿童管理中的应用。

Botulinum Toxin in the Management of Children with Cerebral Palsy.

机构信息

Royal Children's Hospital, 50 Flemington Road, Parkville, VIC, 3052, Australia.

Orthopaedic Department, Royal Children's Hospital, 50 Flemington Road, Parkville, VIC, 3052, Australia.

出版信息

Paediatr Drugs. 2019 Aug;21(4):261-281. doi: 10.1007/s40272-019-00344-8.

Abstract

During the past 25 years, botulinum toxin type A (BoNT-A) has become the most widely used medical intervention in children with cerebral palsy. In this review we consider the gaps in our knowledge in the use of BoNT-A and reasons why muscle morphology and function in children with cerebral palsy are impaired. We review limitations in our knowledge regarding the mechanisms underlying the development of contractures and the difficulty in preventing them. It is clear from this review that injection of BoNT-A in the large muscles of both the upper and lower limbs of children with cerebral palsy will result in a predictable decrease in muscle activity, which is usually reported as a reduction in spasticity, for between 3 and 6 months. These changes are noted by the use of clinical tools such as the Modified Ashworth Scale and the Modified Tardieu Scale. Decreased muscle over-activity usually results in improved range of motion in distal joints. Injection of the gastrocnemius muscle for toe-walking in a child with hemiplegia or diplegia usually has the effect of increasing the passive range of dorsiflexion at the ankle. In our review, we found that this may result in a measurable improvement in gait by the use of observational gait scales or gait analysis, in some children. However, improvements in gait function are not always achieved and are small in magnitude and short lived. We found that some of the differences in outcomes in clinical trials may relate to the use of adjunctive interventions such as serial casting, orthoses, night splints and intensive therapy. We note that the majority of clinical trials of the use of BoNT-A in children with cerebral palsy have focussed on a single injection cycle and this is insufficient to understand the balance between benefit and harm. Most outcomes were reported in terms of changes in muscle tone and there were fewer studies with robust methodology that reported improvements in function. Changes in the domains of activities and participation have rarely been reported in studies to date. There were no clinical reviews to date that consider the findings of studies in human volunteers and in experimental animals and their relevance to clinical protocols. In this review we found that studies in human volunteers and in experimental animals show muscle atrophy after an injection of BoNT-A for at least 12 months. Muscle atrophy was accompanied by loss of contractile elements in muscle and replacement with fat and connective tissue. It is not currently known if these changes, mediated at a molecular level, are reversible. We conclude that there is a need to revise clinical protocols by using BoNT-A more thoughtfully, less frequently and with greatly enhanced monitoring of the effects on injected muscle for both short-term and long-term benefits and harms.

摘要

在过去的 25 年中,A型肉毒毒素(BoNT-A)已成为脑瘫患儿最广泛使用的医学干预手段。在这篇综述中,我们考虑了我们在 BoNT-A 使用方面的知识空白,以及脑瘫患儿肌肉形态和功能受损的原因。我们回顾了关于挛缩发展机制的知识局限性,以及预防挛缩的困难。从这篇综述中可以清楚地看出,在脑瘫患儿的上下肢大肌肉中注射 BoNT-A,将导致肌肉活动的可预测下降,通常表现为痉挛的减少,持续 3 至 6 个月。这些变化可以通过使用改良 Ashworth 量表和改良 Tardieu 量表等临床工具来观察到。肌肉过度活动的减少通常会导致远端关节活动范围的改善。在偏瘫或四肢瘫患儿中,注射腓肠肌以治疗足下垂,通常会增加踝关节背屈的被动活动范围。在我们的综述中,我们发现,在一些儿童中,使用观察性步态量表或步态分析可以测量到步态的改善。然而,步态功能的改善并不总是能够实现,而且幅度较小,持续时间较短。我们发现,临床试验结果的一些差异可能与辅助干预的使用有关,例如连续石膏固定、矫形器、夜间夹板和强化治疗。我们注意到,大多数关于脑瘫患儿使用 BoNT-A 的临床试验都集中在一个注射周期,这不足以了解利弊之间的平衡。大多数结果都是以肌肉张力的变化来报告的,而使用稳健方法报告功能改善的研究较少。迄今为止,在研究中很少有报告活动和参与领域的变化。迄今为止,还没有临床综述考虑人类志愿者和实验动物研究的结果及其与临床方案的相关性。在这篇综述中,我们发现,在人类志愿者和实验动物中进行的研究表明,BoNT-A 注射后至少 12 个月肌肉会发生萎缩。肌肉萎缩伴随着肌肉收缩成分的丢失,并被脂肪和结缔组织取代。目前尚不清楚这些在分子水平上介导的变化是否可以逆转。我们得出的结论是,有必要通过更周到地使用 BoNT-A、更频繁地使用以及更加强化监测注射肌肉的短期和长期效果,来修改临床方案。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c6bc/6682585/a540018c8d92/40272_2019_344_Fig1_HTML.jpg

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