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迟发性运动障碍

Tardive dyskinesia.

作者信息

Casey D E

机构信息

Psychiatry Service, Veterans Administration Medical Center, Portland, OR 97207.

出版信息

West J Med. 1990 Nov;153(5):535-41.

Abstract

Tardive dyskinesia is a potentially irreversible syndrome of involuntary hyperkinetic movements that occur in predisposed persons receiving extended neuroleptic (antipsychotic) drug therapy. It is usually characterized by choreoathetoid dyskinesias in the orofacial, limb, and truncal regions, but subtypes of this syndrome may include tardive dystonia and tardive akathisia. Although the mechanisms underlying the pathogenesis and pathophysiology of this disorder are unproven, altered dopaminergic functions will likely play a role in any explanation of it. Tardive dyskinesia develops in 20% of neuroleptic-treated patients, but high-risk groups such as the elderly have substantially higher rates. Risk factors include age, female sex, affective disorders, and probably those without psychotic diagnoses, including patients receiving drugs with antidopaminergic activity for nausea or gastrointestinal dysfunction for extended periods. Total drug exposure is positively correlated with tardive dyskinesia risk. Management strategies include a careful evaluation of both the psychiatric and neurologic states, a broad differential diagnosis, and adjustment of neuroleptic agents to the lowest effective dose that controls psychosis and minimizes motor side effects. No drug therapy is uniformly safe and effective for treating this disorder. A favorable long-term outcome of improvement or resolution correlates with younger age, early detection, lower drug exposure, and duration of follow-up.

摘要

迟发性运动障碍是一种潜在不可逆的综合征,表现为不自主的运动亢进,发生于接受长期抗精神病药物治疗的易感人群。其通常特征为口面部、肢体和躯干区域的舞蹈手足徐动样运动障碍,但该综合征的亚型可能包括迟发性肌张力障碍和迟发性静坐不能。尽管这种疾病发病机制和病理生理学的潜在机制尚未得到证实,但多巴胺能功能改变可能在任何相关解释中起作用。20%接受抗精神病药物治疗的患者会发生迟发性运动障碍,但老年人等高风险人群的发病率要高得多。风险因素包括年龄、女性、情感障碍,可能还包括那些没有精神病诊断的人群,包括长期接受具有抗多巴胺能活性药物治疗恶心或胃肠道功能障碍的患者。药物总暴露量与迟发性运动障碍风险呈正相关。管理策略包括仔细评估精神状态和神经状态、广泛的鉴别诊断,以及将抗精神病药物调整至控制精神病且使运动副作用最小化的最低有效剂量。没有哪种药物治疗对这种疾病是普遍安全有效的。改善或缓解的良好长期预后与年龄较小、早期发现、较低的药物暴露量以及随访时间有关。

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