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一项针对非洲裔个体的全基因组关联研究表明,在评估氯氮平相关中性粒细胞减少症时,达菲缺失基因型具有重要意义。

A genome-wide association study in individuals of African ancestry reveals the importance of the Duffy-null genotype in the assessment of clozapine-related neutropenia.

机构信息

MRC Centre for Neuropsychiatric Genetics and Genomics, Division of Psychological Medicine and Clinical Neurosciences, School of Medicine, Cardiff University, Cardiff, UK.

Leyden Delta B.V., Nijmegen, The Netherlands.

出版信息

Mol Psychiatry. 2019 Mar;24(3):328-337. doi: 10.1038/s41380-018-0335-7. Epub 2019 Jan 15.

DOI:10.1038/s41380-018-0335-7
PMID:30647433
Abstract

Individuals of African ancestry in the United States and Europe are at increased risk of developing schizophrenia and have poorer clinical outcomes. The antipsychotic clozapine, the only licensed medication for treatment-resistant schizophrenia, is under-prescribed and has high rates of discontinuation in individuals of African ancestry, due in part to increased rates of neutropenia. The genetic basis of lower neutrophil levels in those of African ancestry has not previously been investigated in the context of clozapine treatment. We sought to identify risk alleles in the first genome-wide association study of neutrophil levels during clozapine treatment, in 552 individuals with treatment-resistant schizophrenia and robustly inferred African genetic ancestry. Two genome-wide significant loci were associated with low neutrophil counts during clozapine treatment. The most significantly associated locus was driven by rs2814778 (β = -0.9, P = 4.21 × 10), a known regulatory variant in the atypical chemokine receptor 1 (ACKR1) gene. Individuals homozygous for the C allele at rs2814778 were significantly more likely to develop neutropenia and have to stop clozapine treatment (OR = 20.4, P = 3.44 × 10). This genotype, also termed "Duffy-null", has previously been shown to be associated with lower neutrophil levels in those of African ancestry. Our results indicate the relevance of the rs2814778 genotype for those taking clozapine and its potential as a pharmacogenetic test, dependent on the outcome of additional safety studies, to assist decision making in the initiation and on-going management of clozapine treatment.

摘要

美国和欧洲的非裔个体罹患精神分裂症的风险增加,且临床结局较差。氯氮平是唯一获准用于治疗难治性精神分裂症的抗精神病药物,但在非裔个体中的应用不足,停药率较高,部分原因是中性粒细胞减少症的发生率增加。此前,尚未在氯氮平治疗的背景下研究非裔个体中性粒细胞水平较低的遗传基础。我们试图在接受氯氮平治疗的 552 例难治性精神分裂症和具有强大推断的非洲遗传背景的个体中,进行首次针对氯氮平治疗期间中性粒细胞水平的全基因组关联研究,以确定风险等位基因。在氯氮平治疗期间,有两个全基因组显著位点与中性粒细胞计数低相关。最显著相关的位点是由 rs2814778 驱动的(β=-0.9,P=4.21×10),这是趋化因子受体 1(ACKR1)基因中的一个已知调节变体。rs2814778 纯合子 C 等位基因的个体发生中性粒细胞减少症和不得不停止氯氮平治疗的可能性显著更高(OR=20.4,P=3.44×10)。这种基因型也称为“Duffy-缺失”,先前已被证明与非裔个体中的中性粒细胞水平较低相关。我们的研究结果表明,rs2814778 基因型与服用氯氮平的个体相关,并且在依赖于安全性研究的额外结果的情况下,其具有作为药物遗传学检测的潜力,以协助氯氮平治疗的启动和持续管理中的决策制定。

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A genome-wide association study of neutrophil count in individuals associated to an African continental ancestry group facilitates studies of malaria pathogenesis.一项针对与非洲大陆祖先群体相关的个体中性粒细胞计数的全基因组关联研究,促进了疟疾发病机制的研究。
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