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RGS4 Polymorphisms Associated With Variability of Cognitive Performance in a Family-Based Schizophrenia Sample

机译:RGS4多态性与基于家庭的精神分裂症样本中认知表现的变异性相关。

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Polymorphisms of the gene encoding the regulator of G protein signaling, subtype 4 (RGS4), may be associated with schizophrenia. Among first-episode schizophrenia patients, they are also associated with dorsolateral prefrontal cortex (DLPFC) volume. The DLPFC is a key region that regulates heritable cognitive functions implicated in schizophrenia pathogenesis. To further understand the relationship of RGS4 variants to schizophrenia, we examined their associations with cognitive functions among schizophrenia patients and their relatives. We analyzed 31 multiplex, multigenerational Caucasian families with schizophrenia recruited on the basis of 2 affected first-degree relatives. All participants underwent a computerized neurocognitive battery that evaluates accuracy and speed (response time) of performance on abstraction/mental flexibility; attention; verbal, spatial, and face memory; and spatial ability. “Tag” single-nucleotide polymorphisms (SNPs) representing common polymorphisms were genotyped. Measured genotype analyses accounting for family relationships were performed using Sequential Oligogenic Linkage Analysis Routines. SNPs rs10917670 (“SNP1”) and rs951439 (“SNP7”) were associated with face memory speed (P = .0003) at a significance level that survived Bonferroni correction (P = .039). The same SNPs have earlier been reported to be associated with schizophrenia. There also were uncorrected associations with rs10917670 (“SNP1”) and rs951439 (“SNP7”) on face memory efficiency (P = .03) and verbal memory efficiency (P = 0.02), rs28757217 on abstraction/mental flexibility speed (P = .02) and verbal memory efficiency (P = .03), SNP18 (rs2661319) on spatial memory accuracy (P = 0.02) and face memory speed (P = .03). RGS4 polymorphisms are associated with variations in cognitive functions and contribute a small but statistically significant proportion of variance in a family-based sample.
机译:编码G蛋白信号传导调节子亚型4(RGS4)的基因多态性可能与精神分裂症有关。在首发型精神分裂症患者中,他们还与背外侧前额叶皮层(DLPFC)体积相关。 DLPFC是调节与精神分裂症发病机理有关的遗传性认知功能的关键区域。为了进一步了解RGS4变异与精神分裂症的关系,我们检查了精神分裂症患者及其亲属中它们与认知功能的关系。我们分析了基于2个受影响的一级亲属招募的31个多元,多代白种人精神分裂症家庭。所有参加者均接受了计算机化的神经认知电池,评估其对抽象/心理灵活性的准确性和表现速度(响应时间)。注意;语言,空间和面部记忆;和空间能力。对代表常见多态性的“标签”单核苷酸多态性(SNP)进行基因分型。使用顺序寡核苷酸连锁分析例行程序进行了解释家庭关系的基因型分析。 SNP rs10917670(“ SNP1”)和rs951439(“ SNP7”)与面部记忆速度(P = .0003)相关联,且其显着性水平在Bonferroni校正后仍然有效(P = .039)。早先有报道称相同的SNP与精神分裂症有关。面部记忆效率(P = .03)和言语记忆效率(P = 0.02)的rs10917670(“ SNP1”)和rs951439(“ SNP7”)的关联也没有得到纠正,抽象/心理柔韧性速度(P =。 02)和口头记忆效率(P = .03),SNP18(rs2661319)对空间记忆的准确性(P = 0.02)和面部记忆速度(P = .03)。 RGS4多态性与认知功能的变异有关,并且在基于家庭的样本中贡献了很小但统计上显着的方差。

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