Neuroleptic malignant syndrome associated with atypical antipsychotics: A case report

Johana Patricia Mogollon Díaz , Linda Yurani Lizcano Toloza , Angie Yarlady Serrano García , Camilo Andrés Alquichire Luna , Diego Fernando García Bohorquez , María Fernanda Chaparro Durán , María Valentina Cáceres Valero
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Abstract

Introduction

Neuroleptic malignant syndrome (NMS) is uncommon, with an incidence of 0.01%–3.23%, and is associated with the use of drugs that intervene with dopamine, causing hyperthermia, muscular rigidity, confusion, autonomic instability and death.

Case report

A 35-year-old man with a history of catatonia, refractory epilepsy and functional impairment, required frequent changes in his anticonvulsant and antipsychotic treatment, due to adverse effects. During 2019, in the month of July, clozapine was changed to amisulpride, in September he developed fever, muscle stiffness, stupor, diaphoresis and tachypnea over a two-week period; paraclinical tests showed elevated creatine phosphokinase (CPK) and leukocytosis, so NMS was considered. The antipsychotic was withdrawn and he was treated with bromocriptine and biperiden, with a good response. Ten days after discharge, he began treatment with olanzapine, which generated a similar episode to the one described in December, with subsequent management and resolution.

Discussion

The diagnosis is based on the use of drugs that alter dopamine levels, plus altered state of consciousness, fever, autonomic instability and paraclinical tests showing leukocytosis and elevated CPK. Differential diagnoses must be ruled out. Early diagnosis generally leads to total remission, although some patients will suffer complications, long-term sequelae or recurrences. The recurrence in this case derived from the early reintroduction of the neuroleptic after the first episode. Treatment should be individualised according to severity to avoid mortality.

Conclusions

Atypical antipsychotics are rarely suspected of generating NMS. Moreover, the time to reintroduction after an episode must also be taken into account.

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与非典型抗精神病药物相关的抗精神病药恶性综合征1例报告
神经抑制药恶性综合征(NMS)并不常见,发病率为0.01%-3.23%,与使用干预多巴胺的药物有关,可引起高热、肌肉僵硬、意识不清、自主神经不稳定和死亡。病例报告:一名35岁男性,有紧张症、难治性癫痫和功能障碍病史,由于不良反应,需要频繁改变抗惊厥药和抗精神病药的治疗。2019年7月,氯氮平改为氨硫pride, 9月,他在两周内出现发烧、肌肉僵硬、昏迷、出汗和呼吸急促;临床试验显示肌酸磷酸激酶(CPK)升高,白细胞增多,考虑NMS。停用抗精神病药物,并给予溴隐亭和双哌啶治疗,效果良好。出院后10天,他开始使用奥氮平治疗,这引起了与12月描述的类似的发作,随后得到了管理和解决。诊断是基于使用改变多巴胺水平的药物,加上意识状态改变、发热、自主神经不稳定和临床旁检查显示白细胞增多和CPK升高。必须排除鉴别诊断。早期诊断通常会导致完全缓解,尽管有些患者会出现并发症、长期后遗症或复发。此例的复发源于首次发作后早期再次使用抗精神病药。应根据病情轻重进行个体化治疗,以避免死亡。结论典型抗精神病药物很少被怀疑产生NMS。此外,事件发生后重新引入的时间也必须考虑在内。
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