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针对迟发性运动障碍的治疗策略。二十年的经验。

Therapeutic strategies against tardive dyskinesia. Two decades of experience.

作者信息

Jeste D V, Wyatt R J

出版信息

Arch Gen Psychiatry. 1982 Jul;39(7):803-16. doi: 10.1001/archpsyc.1982.04290070037008.

Abstract

We reviewed 285 treatment studies involving more than 3,000 patients with neuroleptic-induced tardive dyskinesia (TD). Neuroleptic withdrawal is found to reverse dyskinesia in about 37% of patients. There is no satisfactory treatment for persistent TD. Although neuroleptics are significantly superior to most other methods of treatment in suppressing signs of dyskinesia, the safety of their long-term use in dyskinetic patients remains to be demonstrated. Putative gamma-aminobutyric acid (GABA)-ergic drugs and noradrenergic blockers deserve careful study. A strategy for determining biochemical and pharmacologic subtypes of TD appears promising. The value of the available cholinergic agents in the treatment of TD is uncertain. Caution is warranted in interpreting "positive" results with a number of other drugs, which might act as placebos or as nonspecific sedatives. Anticholinergic drugs are generally not recommended for treating dyskinetic patients. Current theories of the pathophysiology of TD may need revision. Drug-free periods do not seem to prevent TD. Antipsychotic drugs without neuroleptic side effects should be developed.

摘要

我们回顾了285项治疗研究,涉及3000多名患有抗精神病药所致迟发性运动障碍(TD)的患者。发现停用抗精神病药可使约37%的患者的运动障碍得到缓解。对于持续性TD尚无令人满意的治疗方法。虽然抗精神病药在抑制运动障碍体征方面明显优于大多数其他治疗方法,但其在运动障碍患者中长期使用的安全性仍有待证实。假定的γ-氨基丁酸(GABA)能药物和去甲肾上腺素能阻滞剂值得仔细研究。确定TD生化和药理学亚型的策略似乎很有前景。现有胆碱能药物在TD治疗中的价值尚不确定。在解释许多其他药物的“阳性”结果时应谨慎,这些药物可能起安慰剂作用或作为非特异性镇静剂。一般不建议用抗胆碱能药物治疗运动障碍患者。目前关于TD病理生理学的理论可能需要修正。无药期似乎不能预防TD。应研发无抗精神病药副作用的抗精神病药物。

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