Centre for Addiction and Mental Health (CAMH), Toronto, ON, Canada; Institute of Medical Sciences, University of Toronto, Toronto, ON, Canada.
Centre for Addiction and Mental Health (CAMH), Toronto, ON, Canada; Department of Neuropsychiatry, Keio University, Minato, Tokyo, Japan.
Schizophr Res. 2024 Aug;270:152-161. doi: 10.1016/j.schres.2024.06.020. Epub 2024 Jun 22.
Clozapine is the only antipsychotic approved for treating treatment-resistant schizophrenia (TRS), characterized by persistent positive symptoms despite adequate antipsychotic treatment. Unfortunately, clozapine demonstrates clinical efficacy in only ~30-60 % of patients with TRS (clozapine-responders; ClzR+), while the remaining ~40-70 % are left with no pharmacological recourse for improvement (clozapine-resistant; ClzR-). Mechanism(s) underlying clozapine's superior efficacy remain unclear. However, in vitro evidence suggests clozapine may mitigate glutamatergic dysregulations observed in TRS, by modulating astrocyte activity in ClzR+, but not ClzR-. A factor that if proven correct, may help the assessment of treatment response and development of more effective antipsychotics. To explore the presence of clozapine-astrocyte interaction and clinical improvement, we used 3 T proton-magnetic resonance spectroscopy to quantify levels of myo-Inositol, surrogate biomarker of astrocyte activity, in regions related to schizophrenia neurobiology: Dorsal-anterior-cingulate-cortex (dACC), left-dorsolateral-prefrontal-cortex (left-DLPFC), and left-striatum (left-striatum) of 157 participants (ClzR- = 30; ClzR+ = 37; responders = 38; controls = 52). Clozapine treatment was assessed using clozapine to norclozapine plasma levels, 11-12 h after last clozapine dose. Measures for symptom severity (i.e., Positive and Negative Symptoms Scale) and cognition (i.e., Mini-Mental State Examination) were also recorded. Higher levels of myo-Inositol were observed in TRS groups versus responders and controls (dACC (p < 0.001); left-striatum (p = 0.036); left-DLPFC (p = 0.023)). In ClzR+, but not ClzR-, clozapine to norclozapine ratios were positively associated with myo-Inositol levels (dACC (p = 0.004); left-DLPFC (p < 0.001)), and lower positive symptom severity (p < 0.001). Our results support growing in vitro evidence of clozapine-astrocyte interaction in clozapine-responders. Further research may determine the viability of clozapine-astrocyte interactions as an early marker of clozapine response.
氯氮平是唯一一种被批准用于治疗治疗抵抗性精神分裂症(TRS)的抗精神病药物,其特征是尽管进行了充分的抗精神病治疗,但仍存在持续的阳性症状。不幸的是,氯氮平在 TRS 患者中的临床疗效仅约为 30-60%(氯氮平反应者;ClzR+),而其余约 40-70%的患者则没有改善的药物治疗方法(氯氮平抵抗者;ClzR-)。氯氮平疗效优越的机制尚不清楚。然而,体外证据表明,氯氮平通过调节 ClzR+中的星形胶质细胞活性,可以减轻 TRS 中观察到的谷氨酸能失调,但不能调节 ClzR-中的星形胶质细胞活性。如果这一假设被证明是正确的,它可能有助于评估治疗反应和开发更有效的抗精神病药物。为了探索氯氮平与星形胶质细胞相互作用和临床改善的关系,我们使用 3T 质子磁共振波谱(MRS)技术来定量测定与精神分裂症神经生物学相关的三个区域(背侧前扣带皮层(dACC)、左侧背外侧前额叶皮层(left-DLPFC)和左侧纹状体(left-striatum))中肌醇的水平,该物质是星形胶质细胞活性的替代生物标志物:157 名参与者(ClzR-=30;ClzR+=37;反应者=38;对照组=52)。使用氯氮平到去甲氯氮平的血浆水平来评估氯氮平治疗,在最后一次氯氮平剂量后 11-12 小时。还记录了症状严重程度(即阳性和阴性症状量表)和认知(即简易精神状态检查)的测量值。TRS 组与反应者和对照组相比,肌醇水平更高(dACC(p<0.001);左侧纹状体(p=0.036);左侧背外侧前额叶皮层(p=0.023))。在 ClzR+中,但不在 ClzR-中,氯氮平到去甲氯氮平的比值与肌醇水平呈正相关(dACC(p=0.004);左侧背外侧前额叶皮层(p<0.001)),且阳性症状严重程度较低(p<0.001)。我们的研究结果支持氯氮平与星形胶质细胞相互作用的体外证据不断增加。进一步的研究可能会确定氯氮平与星形胶质细胞相互作用作为氯氮平反应的早期标志物的可行性。
