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替扎尼定。关于其在治疗与脑和脊髓疾病相关的痉挛方面的药理学、临床疗效及耐受性的综述。

Tizanidine. A review of its pharmacology, clinical efficacy and tolerability in the management of spasticity associated with cerebral and spinal disorders.

作者信息

Wagstaff A J, Bryson H M

机构信息

Adis International Limited, Auckland, New Zealand.

出版信息

Drugs. 1997 Mar;53(3):435-52. doi: 10.2165/00003495-199753030-00007.

DOI:10.2165/00003495-199753030-00007
PMID:9074844
Abstract

The central alpha 2 adrenoceptor agonist tizanidine is a myotonolytic agent used in the treatment of spasticity in patients with cerebral or spinal injury. Wide interpatient variability in the effective plasma concentrations of tizanidine means that the optimal dosage must be titrated over 2 to 4 weeks for each patient (dosages of 2 to 36 mg/day have been used in clinical trials). Maximum effects occur within 2 hours of administration. Antispastic efficacy has been demonstrated for tizanidine in placebo-controlled trials, with reduction in mean muscle tone scores of 21 to 37% versus 4 to 9% for patients receiving placebo. Improvement in muscle tone occurred in 60 to 82% of tizanidine recipients, compared with 60 to 65% of baclofen and 60 to 83% of diazepam recipients. Spasm frequency and clonus are also reduced by tizanidine. The most common adverse effects associated with tizanidine are dry mouth and somnolence/drowsiness. Muscle strength, as assessed by objective means, appears not to be adversely affected by tizanidine and subjective muscle weakness is reported less often by tizanidine recipients than by those receiving baclofen or diazepam. Global tolerability was assessed as good to excellent in 44 to 100% of patients receiving tizanidine, compared with 38 to 90% of baclofen and 20 to 54% of diazepam recipients. In conclusion, tizanidine is an antispastic agent with similar efficacy to that of baclofen and a more favourable tolerability profile. While drowsiness is a frequently reported adverse effect with both agents, subjective muscle weakness appears to be less of a problem with tizanidine than with baclofen. Tizanidine, therefore, appears to be an attractive therapeutic alternative for patients with spasticity associated with cerebral or spinal damage.

摘要

中枢性α2肾上腺素能受体激动剂替扎尼定是一种用于治疗脑损伤或脊髓损伤患者痉挛的肌松剂。替扎尼定有效血浆浓度在患者之间存在很大差异,这意味着必须为每位患者在2至4周内滴定最佳剂量(临床试验中使用的剂量为2至36毫克/天)。给药后2小时内出现最大效果。在安慰剂对照试验中已证明替扎尼定具有抗痉挛疗效,接受替扎尼定的患者平均肌张力评分降低21%至37%,而接受安慰剂的患者为4%至9%。60%至82%接受替扎尼定的患者肌张力得到改善,相比之下,接受巴氯芬的患者为60%至65%,接受地西泮的患者为60%至83%。替扎尼定还可降低痉挛频率和阵挛。与替扎尼定相关的最常见不良反应是口干和嗜睡/困倦。通过客观方法评估,肌肉力量似乎不受替扎尼定的不利影响,并且与接受巴氯芬或地西泮的患者相比,接受替扎尼定的患者较少报告主观肌肉无力。在接受替扎尼定的患者中,44%至100%的患者总体耐受性评估为良好至优秀,相比之下,接受巴氯芬的患者为38%至90%,接受地西泮的患者为20%至54%。总之,替扎尼定是一种抗痉挛药物,其疗效与巴氯芬相似,耐受性更好。虽然嗜睡是这两种药物经常报告的不良反应,但与巴氯芬相比,替扎尼定的主观肌肉无力问题似乎较小。因此,替扎尼定似乎是脑损伤或脊髓损伤相关痉挛患者有吸引力的治疗选择。

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本文引用的文献

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PRELIMINARY TRIAL OF CARISOPRODOL IN MULTIPLE SCLEROSIS.卡立普多治疗多发性硬化症的初步试验
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A comparison of the effects of two antispastic drugs, tizanidine and baclofen, on synaptic transmission from muscle spindle afferents to spinal interneurones in cats.两种抗痉挛药物替扎尼定和巴氯芬对猫从肌梭传入神经到脊髓中间神经元的突触传递影响的比较。
替扎尼定过量的应急处理:一例重症监护策略的病例报告
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Tizanidine-Induced Bradycardia Without Concomitant Medications: A Case Report.未合并使用其他药物情况下替扎尼定诱发的心动过缓:一例报告
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Case of tizanidine withdrawal showing hallucination, decorticate posture and tremor, with hypersympathetic vital signs.替扎尼定戒断致幻觉、去皮质强直姿势和震颤伴交感神经亢进生命体征 1 例
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Formulation of tizanidine hydrochloride-loaded provesicular system for improved oral delivery and therapeutic activity employing a 2 full factorial design.采用 2 因素完全设计,将盐酸替扎尼定载入前体囊泡系统以改善口服传递和治疗活性。
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Expert consensus on the diagnosis and treatment of myofascial pain syndrome.肌筋膜疼痛综合征诊断与治疗专家共识
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Irreversible profound symptomatic bradycardia requiring pacemaker after tizanidine/loxoprofen combination therapy: a case report.替扎尼定/洛索洛芬联合治疗后出现不可逆的严重症状性心动过缓,需植入起搏器:一例报告
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The sedative and sympatholytic effects of oral tizanidine in healthy volunteers.口服替扎尼定对健康志愿者的镇静和抗交感神经作用。
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A double-blind, placebo-controlled trial of tizanidine in the treatment of spasticity caused by multiple sclerosis. United Kingdom Tizanidine Trial Group.替扎尼定治疗多发性硬化所致痉挛的双盲、安慰剂对照试验。英国替扎尼定试验组。
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