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慢性精神分裂症患者持续性阳性症状的抗精神病药物反应与 xMHC 区域的精神分裂症风险基因座相关。

Schizophrenia risk loci from xMHC region were associated with antipsychotic response in chronic schizophrenic patients with persistent positive symptom.

机构信息

Department of Psychiatry and Behavioral Sciences, Northwestern University Feinberg School of Medicine, Chicago, IL, USA.

Department of Molecular and Functional Genomics, Weis Center for Research, Geisinger Health System, Danville, PA, USA.

出版信息

Transl Psychiatry. 2022 Mar 7;12(1):92. doi: 10.1038/s41398-022-01854-9.

Abstract

We examined whether common variants from the extended major histocompatibility complex (xMHC) region contribute to the response to antipsychotic drugs (APDs) in patients with schizophrenia with persistent psychosis. Subjects participated in a prospective longitudinal study of the effect of APDs on psychopathology were temporally split into discovery (n = 88) and replication (n = 42) cohorts. The primary endpoint was a change in Brief Psychiatric Rating Scale at 6-week or 6-month after treatment. rs204991 (β = 3.917, p = 3.72 × 10), the strongest signal associated with response at 6-week was located near C4A/C4B after a linear regression adjusted for covariates. xMHC SNP imputation disclosed much stronger signals (rs9268469, β = 5.140, p = 1.57 × 10) and other weaker signals (p < 1 × 10) spanning the entire xMHC region. All the variants were previously identified schizophrenia risk loci. Conditional fine-mapping revealed three subgroups of SNPs which were the eQTLs (p < 1 × 10) for C4A, HLA-C, and BTN3A2 in disease-relevant tissue. Epistasis between HLA-C and C4A was observed (p = 0.019). Minor allele (G) carriers of rs204991, eQTL for C4A, having decreased risk for schizophrenia and lower imputed expression of C4A, had a better response to APDs. Some imputed HLA alleles associated with a decreased risk for schizophrenia had a positive association with improvement in psychotic symptoms. An independent cohort validated the association of change in psychosis with C4A. We provide evidence that genetic risk factors for schizophrenia from the xMHC region are associated with response to APDs and those variants significantly alter the imputed expression of C4A, HLA-C, and BTN3A2. The minor alleles predicting higher C4A level are associated with diminished improvement in psychotic symptoms after APD treatment.

摘要

我们研究了扩展的主要组织相容性复合体(xMHC)区域中的常见变体是否会影响持续性精神病患者的抗精神病药物(APD)反应。研究对象参加了一项关于 APD 对精神病理学影响的前瞻性纵向研究,根据治疗后 6 周或 6 个月的简明精神病评定量表(Brief Psychiatric Rating Scale)的变化将患者分为发现(n=88)和复制(n=42)队列。主要终点是治疗后 6 周时简要精神病评定量表的变化。rs204991(β=3.917,p=3.72×10),与 6 周时反应相关的最强信号位于 C4A/C4B 附近,经过协变量调整后的线性回归。xMHC SNP 推断显示出更强的信号(rs9268469,β=5.140,p=1.57×10)和其他较弱的信号(p<1×10)跨越整个 xMHC 区域。所有变体均为先前确定的精神分裂症风险基因座。条件精细映射显示了三个亚组 SNP,它们是疾病相关组织中 C4A、HLA-C 和 BTN3A2 的 eQTL(p<1×10)。观察到 HLA-C 和 C4A 之间的上位性(p=0.019)。rs204991 的 C4A 效应等位基因(G)携带者,C4A 风险降低,C4A 表达降低,对 APD 反应更好。一些与精神分裂症风险降低相关的 HLA 等位基因与精神病症状改善呈正相关。独立队列验证了精神病变化与 C4A 的关联。我们提供了证据,表明 xMHC 区域的精神分裂症遗传风险因素与 APD 反应相关,这些变体显著改变了 C4A、HLA-C 和 BTN3A2 的推断表达。预测 C4A 水平较高的次要等位基因与 APD 治疗后精神病症状改善程度降低有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fe8a/8898944/6fcdc2ff278f/41398_2022_1854_Fig1_HTML.jpg

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