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Polygenic Risk Score for Schizophrenia and Treatment-Resistant Schizophrenia

机译:精神分裂症和难治性精神分裂症的多基因风险评分

摘要

Treatment-resistant schizophrenia (TRS) affects around one-third of individuals with schizophrenia. Although a number of sociodemographic and clinical predictors of TRS have been identified, data on the genetic risk of TRS are sparse. We aimed to investigate the association between a polygenic risk score for schizophrenia and treatment resistance in patients with schizophrenia. We conducted a nationwide, population-based follow-up study among all Danish individuals born after 1981 and with an incident diagnosis of schizophrenia between 1999 and 2007. Based on genome-wide data polygenic risk scores for schizophrenia were calculated in 862 individuals with schizophrenia. TRS was defined as either clozapine initiation or at least 2 periods of different antipsychotic monotherapies and still being hospitalized. We estimated hazard rate ratios (HRs) for TRS in relation to the polygenic risk score while adjusting for population stratification, age, sex, geographical area at birth, clinical treatment setting, psychiatric comorbidity, and calendar year. Among the 862 individuals with schizophrenia, 181 (21.0%) met criteria for TRS during 4674 person-years of follow-up. We found no significant association between the polygenic risk score and TRS, adjusted HR = 1.13 (95% CI: 0.95–1.35). Based on these results, the use of the polygenic risk score for schizophrenia to identify individuals with TRS is at present inadequate to be of clinical utility at the individual patient level. Future research should include larger genetic samples in combination with non-genetic markers. Moreover, a TRS-specific developed polygenic risk score would be of great interest towards early prediction of TRS.
机译:难治性精神分裂症(TRS)影响约三分之一的精神分裂症患者。尽管已经确定了TRS的许多社会人口统计学和临床​​预测指标,但有关TRS遗传风险的数据很少。我们旨在研究精神分裂症的多基因风险评分与精神分裂症患者的治疗抵抗之间的关系。我们对1981年以后出生并在1999年至2007年间被诊断为精神分裂症的所有丹麦个体进行了全国性的,基于人群的随访研究。基于全基因组数据,计算了862名精神分裂症个体的精神分裂症多基因风险评分。 TRS被定义为开始氯氮平或至少2个时期的不同抗精神病药物单一疗法并仍在住院。我们在调整人口分层,年龄,性别,出生时的地理区域,临床治疗设置,精神病合并症和日历年的同时,估算了与多基因风险评分相关的TRS危险率(HRs)。在862名精神分裂症患者中,有181名(21.0%)在4674人-年的随访期间达到了TRS标准。我们发现,多基因风险评分与TRS之间无显着相关性,校正后的HR = 1.13(95%CI:0.95-1.35)。基于这些结果,目前对于精神分裂症使用多基因风险评分来鉴定患有TRS的个体尚不足以在个体患者水平上发挥临床作用。未来的研究应包括更大的遗传样本和非遗传标记。此外,TRS特有的多基因风险评分将对TRS的早期预测非常感兴趣。

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