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Expression profiling in monozygotic twins discordant for bipolar disorder reveals dysregulation of the WNT signalling pathway

机译:与双相情感障碍不一致的单卵双胞胎中的表达谱揭示了WNT信号通路的失调

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To identify genes dysregulated in bipolar disorder (BD1), we carried out global gene expression profiling using whole-genome microarrays. To minimize genetic variation in gene expression levels between cases and controls, we compared expression profiles in lymphoblastoid cell lines from monozygotic twin pairs discordant for the disease. We identified 82 genes that were differentially expressed by 1.3-fold in three BD1 cases compared to their co-twins, and which were statistically (P0.05) differentially expressed between the groups of BD1 cases and controls. Using quantitative reverse transcriptase-polymerase chain reaction, we confirmed the differential expression of some of these genes, including: KCNK1, MAL, PFN2, TCF7, PGK1 and PI4KCB, in at least two of the twin pairs. In contrast to the findings of a previous study by Kakiuchi and colleagues with similar discordant BD1 twin design, our data do not support the dysregulation of XBP1 and HSPA5. From pathway and gene ontology analysis, we identified upregulation of the WNT signalling pathway and the biological process of apoptosis. The differentially regulated genes and pathways identified in this study may provide insights into the biology of BD1.
机译:为了鉴定双相情感障碍(BD1)中失调的基因,我们使用全基因组微阵列进行了全球基因表达谱分析。为了最小化病例与对照之间基因表达水平的遗传差异,我们比较了与疾病不一致的单卵双生子对的淋巴母细胞样细胞系中的表达谱。我们确定了82个基因,在3个BD1病例中与其同卵双胞胎差异表达1.3倍,并且在BD1病例组和对照组之间差异表达(P0.05)。使用定量逆转录酶-聚合酶链反应,我们确认了其中至少两个双胞胎中某些基因的差异表达,包括:KCNK1,MAL,PFN2,TCF7,PGK1和PI4KCB。与Kakiuchi及其同事先前的研究相似,其BD1双胞胎的设计相似,与此相反,我们的数据不支持XBP1和HSPA5的失调。通过通路和基因本体分析,我们确定了WNT信号通路的上调和细胞凋亡的生物学过程。在这项研究中鉴定的差异调节基因和途径可能为BD1生物学提供见解。

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