Institute of Psychiatry, University of Bologna, Italy.
Eur Neuropsychopharmacol. 2013 Aug;23(8):887-94. doi: 10.1016/j.euroneuro.2012.08.013. Epub 2012 Sep 11.
We previously investigated a sample of psychotic patients acutely ill and acutely treated with haloperidol in the search for genetic predictors of response at PANSS scores during the first month of treatment. In the present work we extend the analysis to a wider panel of genetic variations including SNPs harbored by genes whose products are involved in molecular pathways consistent with the latest results of genome-wide association studies (GWAS) of antipsychotic efficacy. 96 Patients were investigated. The results were replicated in an independent sample of bipolar manic patients treated with antipsychotics (n tot=470, the sample was retrieved from the STEP-BD). Outcomes were the PANSS variation through time in the first sample, and changes of mania symptomatology at any two consecutive observations in the public available STEP-BD replication sample. A list of variations harbored by AKAP13, CACNA1, GRIK4 and GRIA1 were found to be significantly associated with outcome in both samples (different set of variations for each sample). Results did not survived multiple testing in the original sample but were replicated in both samples. This finding stresses the relevance of the glutamatergic system and regulatory molecular cascades in antipsychotic response. Nonetheless, the level of significance and the indirect and incomplete replication mandate cautiousness and further replication.
我们之前对一组急性精神病患者进行了研究,这些患者在急性发作期间接受了氟哌啶醇治疗,以寻找治疗的第一个月期间 PANSS 评分的反应的遗传预测因子。在本研究中,我们将分析扩展到更广泛的遗传变异面板,包括 SNP,这些 SNP 存在于其产物参与与抗精神病药物疗效的全基因组关联研究(GWAS)一致的分子途径的基因中。对 96 名患者进行了研究。结果在使用抗精神病药物治疗的双相情感障碍躁狂患者的独立样本中得到了复制(n tot=470,该样本从 STEP-BD 中检索)。结果是第一个样本中 PANSS 随时间的变化,以及在公开的 STEP-BD 复制样本中任何两个连续观察点上的躁狂症状变化。发现 AKAP13、CACNA1、GRIK4 和 GRIA1 所携带的一系列变异与两个样本中的结果均显著相关(每个样本中都有不同的变异集)。原始样本中未通过多重检验的结果在两个样本中均得到了复制。这一发现强调了谷氨酸能系统和调节分子级联在抗精神病药物反应中的相关性。然而,显著水平以及间接和不完全的复制需要谨慎和进一步的复制。
