CXCL10 rs4256246、CXCR4 rs2228014、CCR2 rs1799864 和 CXCL16 rs2277680 与精神分裂症易感性的关系

IF 2.8 4区 医学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Hana Saoud, Hajer Foddha, Youssef Aflouk, Besma Bel Hadj Jrad
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引用次数: 0

摘要

与促炎和抗炎细胞因子相比,趋化因子配体及其受体在精神分裂症(SCZ)中受到的关注较少。因此,我们旨在研究趋化因子基因 CXCL10、CXCL16、CXCR4 和 CCR2 的功能多态性对 SCZ 发病的影响。通过 PCR-RFLP,我们在由 200 名 SCZ 患者和 200 名健康对照者组成的突尼斯队列中分析了所选的多态性。我们的初步数据表明,CXCL10 rs4256246的小等位基因A与SCZ的发病几率(PAdjusted = 0.00002)显著相关,更确切地说,与晚发SCZ的偏执狂患者(PAdjusted = 0.0007)相关。然而,CXCR4 rs2228014的突变等位基因T对SCZ有显著的保护作用(PAdjusted = 0.000007),特别是对男性(PAdjusted = 0.000003)。这种效应在早发 SCZ 的未分化患者中持续存在(PAdjusted = 0.002)。经过分层分析,CCR2 rs1799864 和 CXCL16 rs2277680 与精神紊乱患者的临床症状显著相关。至于单倍型分析,我们注意到 GATG 单倍型与 SCZ 的保护相关(PAdjusted = 0.0087),但 AGCG 单倍型与该病的易感性相关(PAdjusted = 0.014)。我们的初步研究结果表明,CXCL10 rs4256246增加了对SCZ的易感性,而CXCR4 rs2228014似乎是保护因素。此外,我们还发现 CCR2 rs1799864 和 CXCL16 rs2277680 与该疾病的临床表现密切相关。要验证这些结果并明确目标多态性在 SCZ 中的功能意义,还需要更多的独立研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Involvement of CXCL10 rs4256246, CXCR4 rs2228014, CCR2 rs1799864 and CXCL16 rs2277680 in the Predisposition to Schizophrenia

Involvement of CXCL10 rs4256246, CXCR4 rs2228014, CCR2 rs1799864 and CXCL16 rs2277680 in the Predisposition to Schizophrenia

Involvement of CXCL10 rs4256246, CXCR4 rs2228014, CCR2 rs1799864 and CXCL16 rs2277680 in the Predisposition to Schizophrenia

Chemokine ligands and their receptors have acquired less attention than pro- and anti-inflammatory cytokines in schizophrenia (SCZ). Thus, we aimed to examine the impact of functional polymorphisms of the chemokine genes CXCL10, CXCL16, CXCR4, and CCR2 in the development of SCZ. Using PCR–RFLP, we analyzed the selected polymorphisms in a Tunisian cohort composed of 200 patients with SCZ and 200 healthy controls. Our preliminary data suggest that the minor allele A of CXCL10 rs4256246 is significantly associated with likelihood of SCZ (PAdjusted = 0.00002) and more precisely to paranoid patients with late-onset SCZ (PAdjusted = 0.0007). However, the mutated allele T of CXCR4 rs2228014 showed a significant protective impact against SCZ (PAdjusted = 0.000007) and especially to male sex (PAdjusted = 0.000003). This effect persists among the undifferentiated patients with early-onset SCZ (PAdjusted = 0.002). Following the stratified analyses, CCR2 rs1799864 and CXCL16 rs2277680 were significantly correlated with the clinical symptoms among disorganized patients. As regards haplotype analysis, we noted that GATG haplotype was associated with protection against SCZ (PAdjusted = 0.0087) but the AGCG haplotype was correlated with susceptibility to this disease (PAdjusted = 0.014). Our preliminary results suggested that CXCL10 rs4256246 enhanced susceptibility to SCZ, while CXCR4 rs2228014 seemed to be protective factor. Furthermore, we identified a substantial correlation between CCR2 rs1799864 and CXCL16 rs2277680 with the clinical signs of the disorder. To validate these results and clarify the functional significance of the targeted polymorphisms in SCZ, more independent research is needed.

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来源期刊
Journal of Molecular Neuroscience
Journal of Molecular Neuroscience 医学-神经科学
CiteScore
6.60
自引率
3.20%
发文量
142
审稿时长
1 months
期刊介绍: The Journal of Molecular Neuroscience is committed to the rapid publication of original findings that increase our understanding of the molecular structure, function, and development of the nervous system. The criteria for acceptance of manuscripts will be scientific excellence, originality, and relevance to the field of molecular neuroscience. Manuscripts with clinical relevance are especially encouraged since the journal seeks to provide a means for accelerating the progression of basic research findings toward clinical utilization. All experiments described in the Journal of Molecular Neuroscience that involve the use of animal or human subjects must have been approved by the appropriate institutional review committee and conform to accepted ethical standards.
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