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使用卡立普多治疗精神分裂症:从临床研究到临床实践。国际专家小组的真实世界经验与建议。

Treating schizophrenia with cariprazine: from clinical research to clinical practice. Real world experiences and recommendations from an International Panel.

作者信息

Fagiolini Andrea, Alcalá José Ángel, Aubel Thomas, Bienkiewicz Wojciech, Bogren Mats Magnus Knut, Gago Joaquim, Cerveri Giancarlo, Colla Michael, Sanchez Francisco Collazos, Cuomo Alessandro, Helge Frieling, Iacoponi Eduardo, Karlsson Per-Axel, Peddu Pradeep, Pettorruso Mauro, Pereira Henrique Jorge Ramos, Schölin Johan Sahlsten, Vernaleken Ingo Bernd

机构信息

School of Medicine, Department of Molecular Medicine, University of Siena, Siena, Italy.

Clinical Unit of Mental Health, Reina Sofia University Hospital, Cordoba, Spain.

出版信息

Ann Gen Psychiatry. 2020 Sep 26;19:55. doi: 10.1186/s12991-020-00305-3. eCollection 2020.

Abstract

BACKGROUND

Management of schizophrenia is sub-optimal in many patients. Targeting negative symptoms, among the most debilitating aspects of schizophrenia, together with positive symptoms, can result in significant functional benefits and dramatically improve quality of life for patients and their carers. Cariprazine, a partial agonist of the dopamine receptors D2/D3 has demonstrated effectiveness across symptom domains in clinical trials, particularly on negative symptoms.

OBJECTIVE

To obtain a broader insight from clinicians with specific experience with cariprazine, on how it affects patient populations outside the clinical trial setting.

METHODS

The panel addressed a series of psychopharmacologic topics not comprehensively addressed by the evidence-based literature, including characteristics of patients treated, dosing and switching strategies, duration of therapy, role of concomitant medications and tolerability as well as recommendations on how to individualize cariprazine treatment for patients with schizophrenia.

RESULTS

Patients recommended for cariprazine treatment are those with first episodes of psychosis, predominant negative symptoms (maintenance/acute phase) and significant side effects (metabolic side effects, hyperprolactinemia, sedation) with other antipsychotics. When the long-term treatment of a lifetime illness is adequately weighted, cariprazine becomes one of the first-line medications, not only for patients with predominant negative symptoms but also for those with relatively severe positive symptoms, especially if they are at the first episodes and if a specific medication is added for symptoms such as agitation or insomnia. For instance, patients with agitation may also benefit from the combination of cariprazine and a benzodiazepine or another sedating agent. Cariprazine may be prescribed as add-on to medications such as clozapine, when that medication alone is ineffective for negative symptoms, and sometimes the first may be discontinued or its dose lowered, after a period of stability, leaving the patient on a better tolerated antipsychotic regimen.

CONCLUSIONS

Based on real-world clinical experience, the panel considered that cariprazine, with its distinct advantages including pharmacokinetics/pharmacodynamics, good efficacy and tolerability, represents a drug of choice in the long-term management of schizophrenia not only for patients with predominant negative symptoms but also for those with positive symptoms.

摘要

背景

许多精神分裂症患者的治疗效果欠佳。针对精神分裂症最使人衰弱的方面之一的阴性症状以及阳性症状进行治疗,可带来显著的功能改善,并极大地提高患者及其照料者的生活质量。卡立普嗪是多巴胺D2/D3受体的部分激动剂,在临床试验中已证明其在各个症状领域均有效,尤其是对阴性症状。

目的

从有卡立普嗪使用经验的临床医生那里获得更广泛的见解,了解其在临床试验环境之外如何影响患者群体。

方法

该小组讨论了一系列循证文献未全面涉及的精神药理学主题,包括接受治疗患者的特征、给药和换药策略、治疗持续时间、合并用药的作用和耐受性,以及关于如何为精神分裂症患者个体化使用卡立普嗪治疗的建议。

结果

推荐使用卡立普嗪治疗的患者包括首次发作精神病、以阴性症状为主(维持期/急性期)以及使用其他抗精神病药物有显著副作用(代谢副作用、高泌乳素血症、镇静作用)的患者。当充分权衡终身疾病的长期治疗时,卡立普嗪成为一线药物之一,不仅适用于以阴性症状为主的患者,也适用于阳性症状相对严重的患者,特别是如果他们处于首次发作且针对激越或失眠等症状添加了特定药物时。例如,激越患者可能也会从卡立普嗪与苯二氮䓬类药物或其他镇静剂的联合使用中获益。当单独使用氯氮平对阴性症状无效时,卡立普嗪可作为其附加用药,有时在病情稳定一段时间后,可停用氯氮平或降低其剂量,使患者采用耐受性更好的抗精神病治疗方案。

结论

基于实际临床经验,该小组认为卡立普嗪具有独特优势,包括药代动力学/药效学、良好的疗效和耐受性,不仅是阴性症状为主患者,也是阳性症状患者长期治疗精神分裂症的首选药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7cce/7520022/88ea440a61af/12991_2020_305_Fig1_HTML.jpg

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