精神分裂症的新疗法。

C. Correll, A. Abi-Dargham, O. Howes
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引用次数: 12

摘要

尽管抗精神病药物已经使用了近70年,并极大地改善了精神分裂症患者的预后,但目前所有可用的选择都是通过阻断多巴胺能受体来获得其疗效的。然而,这种作用机制留下了许多未解决的症状,并与显著的副作用负担相关。精神分裂症的潜在机制最初被认为与大脑特定区域突触前多巴胺过量有关,但现在被认为要复杂得多,涉及整个大脑回路的结构和分子变化。因此,药物发现工作已经在寻找新的靶点,以寻找更安全、更有效的药物来改善精神分裂症和精神病的症状,包括微量胺相关受体(TAARs)、毒蕈碱受体和血清素能受体。TAAR1激动剂ulotaront (ep -363856)和muscarinic M1/M4激动剂KarXT (xanomeline + trospium)对精神分裂症急性加重期患者的总、阳性和阴性症状的有效性和安全性,以及5-羟色胺5-HT2A激动剂/拮抗剂匹马万色林对精神分裂症患者的主要阴性症状和阴性症状控制的有效性和安全性令人鼓舞。综上所述,这些数据表明,在正在进行的3期试验项目的背景下,精神分裂症患者可能很快就能获得第一种非D2阻断药物,这可能会彻底改变治疗前景,改善许多精神分裂症患者的治疗效果,这些患者对目前可用的抗精神病药物没有完全反应或不能耐受,目前所有抗精神病药物都是通过突触后多巴胺D2受体阻断起作用的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Emerging Treatments in Schizophrenia.
Although antipsychotics have been available for almost 70 years and greatly improved outcomes for individuals with schizophrenia, all currently available options derive their efficacy from blockade of dopaminergic receptors. However, this mechanism of action leaves many symptoms unresolved and is associated with a significant side effect burden. The mechanisms underlying schizophrenia, which were initially thought to be related to excessive presynaptic dopamine in specific areas of the brain, are now understood to be much more complex and involve structural and molecular changes throughout brain circuits. Consequently, drug discovery efforts have sought new targets in the search for safer and more effective medications that can improve symptoms of schizophrenia and psychosis, including trace amine-associated receptors (TAARs), muscarinic receptors, and serotonergic receptors. Positive phase 2 trial results indicating efficacy and safety of the TAAR1 agonist ulotaront (SEP-363856) and of the muscarinic M1/M4 agonist KarXT (xanomeline plus trospium) for total, positive, and negative symptoms in patients with acute exacerbation of schizophrenia, and of the serotonin 5-HT2A agonist/antagonist pimavanserin in patients with schizophrenia and predominant negative symptoms for negative symptom control are encouraging. Taken together, these data indicate in the context of ongoing phase 3 trial programs that patients with schizophrenia may soon have access to the first non-D2 blocking medication, which could drastically change the treatment landscape and improve outcomes for many of the individuals with schizophrenia who do not fully respond to or cannot tolerate currently available antipsychotic agents that currently all act via postsynaptic dopamine D2 receptor blockade.
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