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氯氮平所致胃肠道动力不足:临床表现与转归,英国药物警戒报告,1992 - 2017年

Clozapine-induced gastrointestinal hypomotility: presenting features and outcomes, UK pharmacovigilance reports, 1992-2017.

作者信息

Handley S A, Every-Palmer S, Ismail A, Flanagan R J

机构信息

Department of Pathology, Royal Hobart Hospital, Australia.

Department of Psychological Medicine, University of Otago, New Zealand.

出版信息

Br J Psychiatry. 2022 Feb 15:1-9. doi: 10.1192/bjp.2022.24.

Abstract

BACKGROUND

Clozapine-induced gastrointestinal hypomotility (CIGH) affects some 75% of patients treated with clozapine.

AIMS

To document the incidence of potentially harmful CIGH in the UK.

METHOD

We studied spontaneous UK pharmacovigilance reports recorded as clozapine-related gastrointestinal adverse drug reactions, 1992-2017.

RESULTS

There were 527 patients reported with potentially harmful CIGH; 33% (n = 172) died. Deaths averaged 1 per year 1992-1999, 5 per year 2000-2009 and 15 per year 2010-2017. Those who died were older (median 52 years v. 49 years) and had been prescribed clozapine for longer than those who recovered (median 11.3 years v. 4.8 years), but there was no difference in prescribed dose. Within the first 4 years of clozapine treatment, there were 169 reports of CIGH, of which 3% (n = 5) were fatal. At 10-14 years there were 63 reports of CIGH, of which 25% (n = 16) were fatal. Among the deaths, males were younger (median 51, range 22-89 v. median 57, range 24-89 years) with higher clozapine doses (median 450, range 100-900 v. median 300, range 12.5-800 mg/d) than females. In non-fatal CIGH, surgery was the most frequent outcome (n = 92). The procedures included appendectomy, ileostomy, total/partial colectomy, colostomy/stoma and proctosigmoidectomy. Clozapine dosage was reduced in 6 patients, stopped and restarted in 23, 'continued' in 6 and discontinued permanently in at least 76 patients.

CONCLUSIONS

The risk of serious morbidity/mortality from CIGH is substantial. The need to actively monitor bowel function and give laxatives to patients treated with clozapine is clear.

摘要

背景

氯氮平所致胃肠道动力不足(CIGH)影响约75%接受氯氮平治疗的患者。

目的

记录英国潜在有害CIGH的发生率。

方法

我们研究了1992年至2017年英国自发上报的记录为与氯氮平相关的胃肠道药物不良反应的药物警戒报告。

结果

报告有527例潜在有害CIGH患者;33%(n = 172)死亡。1992年至1999年平均每年死亡1例,2000年至2009年平均每年死亡5例,2010年至2017年平均每年死亡15例。死亡患者年龄更大(中位年龄52岁对49岁),且接受氯氮平治疗的时间比康复患者更长(中位时间11.3年对4.8年),但处方剂量无差异。在氯氮平治疗的前4年内,有169例CIGH报告,其中3%(n = 5)是致命的。在10至14年时有63例CIGH报告,其中25%(n = 16)是致命的。在死亡病例中,男性比女性更年轻(中位年龄51岁,范围22 - 89岁对中位年龄57岁,范围24 - 89岁),氯氮平剂量更高(中位剂量450,范围100 - 900对中位剂量300,范围12.5 - 800毫克/天)。在非致命性CIGH中,手术是最常见的结局(n = 92)。手术包括阑尾切除术、回肠造口术、全/部分结肠切除术、结肠造口术/造瘘术和直肠乙状结肠切除术。6例患者氯氮平剂量减少,23例停药后重新开始用药,6例“继续用药”,至少76例患者永久停药。

结论

CIGH导致严重发病/死亡的风险很大。显然有必要积极监测接受氯氮平治疗患者的肠道功能并给予泻药。

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