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克来夫定诱发的线粒体肌病

Clevudine Induced Mitochondrial Myopathy.

作者信息

Park Soo Hyun, Park Kyung Seok, Kim Nam Hee, Cho Joong Yang, Koh Moon Soo, Lee Jin Ho

机构信息

Department of Neurology, Dongguk University Ilsan Hospital, Goyang, Korea.

Department of Neurology, Seoul National University College of Medicine, Seoul, Korea.

出版信息

J Korean Med Sci. 2017 Nov;32(11):1857-1860. doi: 10.3346/jkms.2017.32.11.1857.

Abstract

Clevudine was approved as an antiviral agent for hepatitis B virus, which showed marked, rapid inhibition of virus replication without significant toxicity. However, several studies have reported myopathy associated with clevudine therapy. Also, we experienced seven patients who suffered from myopathy during clevudine therapy. To characterize clevudine-induced myopathy, we collected previously reported cases of clevudine myopathy and analyzed all the cases including our cases. We searched electronic databases that were published in English or Korean using PubMed and KoreaMed. Ninety-five cases with clevudine myopathy, including our seven cases, were selected and analyzed for the demographic data, clinical features, and pathologic findings. The 95 patients with clevudine-induced myopathy comprised 52 women and 43 men aged 48.9 years (27-76 years). The patients received clevudine therapy for about 14.2 months (5-24 months) before the development of symptoms. Weakness mainly involved proximal extremities, especially in the lower extremities, and bulbar and neck weakness were observed in some cases (13.7%). Creatine kinase was elevated in the majority of patients (97.9%). Myopathic patterns on electromyography were observed in most patients examined (98.1%). Muscle biopsy presented patterns compatible with mitochondrial myopathy in the majority (90.2%). The weakness usually improved within about 3 months after the discontinuation of clevudine. Though clevudine has been known to be safe in a 6-month clinical trial, longer clevudine therapy for about 14 months may cause reversible mitochondrial myopathy. Careful clinical attention should be paid to patients with long-term clevudine therapy.

摘要

克来夫定被批准作为一种抗乙型肝炎病毒的抗病毒药物,它能显著、快速地抑制病毒复制且无明显毒性。然而,多项研究报告了与克来夫定治疗相关的肌病。此外,我们也遇到了7例在克来夫定治疗期间出现肌病的患者。为了明确克来夫定所致肌病的特征,我们收集了先前报道的克来夫定肌病病例,并对包括我们的病例在内的所有病例进行了分析。我们使用PubMed和KoreaMed搜索了以英文或韩文发表的电子数据库。选取了95例克来夫定肌病病例,包括我们的7例,对其人口统计学数据、临床特征和病理结果进行分析。95例克来夫定所致肌病患者中,女性52例,男性43例,年龄48.9岁(27 - 76岁)。患者在出现症状前接受克来夫定治疗约14.2个月(5 - 24个月)。肌无力主要累及四肢近端,尤其是下肢,部分病例(13.7%)出现延髓和颈部肌无力。大多数患者(97.9%)肌酸激酶升高。大多数接受检查的患者(98.1%)肌电图显示为肌病模式。大多数肌肉活检结果(90.2%)符合线粒体肌病模式。停用克来夫定后,肌无力通常在约3个月内改善。尽管克来夫定在6个月的临床试验中被认为是安全的,但约14个月的更长时间克来夫定治疗可能会导致可逆性线粒体肌病。对于长期接受克来夫定治疗的患者应给予密切的临床关注。

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