Abstract

Clozapine is an atypical antipsychotic used for treatment-resistant schizophrenia. Venous thromboembolism (VTE) is a rare side effect of clozapine which can be fatal. This article summarizes current evidence regarding the risk of VTE associated with the use of clozapine. We performed a PubMed (MeSH) and Google Scholar search for the last two decades. Studies or case reports performed in humans were included in the review, of which 42 case reports of patients taking clozapine at VTE onset were included in the analysis of this review. According to the articles reviewed, the mean age was 42.9 years, with more males (71.43%) than females (28.57%). The average clozapine dose was 285.62 mg/day. VTE onset occurred within the first six months in 71.8% of the cases. Overall, 70.37% of the patients had comorbidities, and 87.5% had risk factors for VTE. In total, 68.57% were prescribed other medications at VTE onset, and 60% were being treated with another antipsychotic concomitantly. Finally, 32.5% of the patients died, while 67.5% survived. In 60% of the cases, clozapine was discontinued after VTE. In our literature review, we observed that among clozapine users, VTE occurred at a wide dose range, and most of the events occurred within the first six months. As many patients who are prescribed clozapine have risk factors for VTE, the risk should be considered at the time of prescribing. Further research should be conducted to elucidate the risk of VTE in clozapine users and the benefits of thromboprophylaxis.

Highlights

  • BackgroundSchizophrenia is a mental disorder that affects approximately 20 million people worldwide [1]

  • This study aims to perform a literature review of the latest evidence and case reports intending to unearth the relationship between clozapine and thrombotic events

  • Clozapine has proven to be highly effective in the treatment of resistant schizophrenia

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Summary

Introduction

Schizophrenia is a mental disorder that affects approximately 20 million people worldwide [1]. Schizophrenia is a severe mental illness that may profoundly impact the individual [1]. It is a disease with complex genetics and not well-elucidated pathophysiology where environmental factors may play an important role [2]. Pharmacological and nonpharmacological therapies are available and can be beneficial. Antipsychotics, both typical and atypical, have been widely used for the treatment of this disorder [2]. The choice of long-term therapy depends upon the prior history of response and the avoidance of side effects [2]

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