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Transcriptomic metaanalyses of autistic brains reveals shared gene expression and biological pathway abnormalities with cancer

机译:自闭虫大脑的转录组metaanyses揭示了与癌症的共同基因表达和生物途径异常

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Epidemiological and clinical evidence points to cancer as a comorbidity in people with autism spectrum disorders (ASD). A significant overlap of genes and biological processes between both diseases has also been reported. Here, for the first time, we compared the gene expression profiles of ASD frontal cortex tissues and 22 cancer types obtained by differential expression meta-analysis and report gene, pathway, and drug set-based overlaps between them. Four cancer types (brain, thyroid, kidney, and pancreatic cancers) presented a significant overlap in gene expression deregulations in the same direction as ASD whereas two cancer types (lung and prostate cancers) showed differential expression profiles significantly deregulated in the opposite direction from ASD. Functional enrichment and LINCS L1000 based drug set enrichment analyses revealed the implication of several biological processes and pathways that were affected jointly in both diseases, including impairments of the immune system, and impairments in oxidative phosphorylation and ATP synthesis among others. Our data also suggest that brain and kidney cancer have patterns of transcriptomic dysregulation in the PI3K/AKT/MTOR axis that are similar to those found in ASD. Comparisons of ASD and cancer differential gene expression meta-analysis results suggest that brain, kidney, thyroid, and pancreatic cancers are candidates for direct comorbid associations with ASD. On the other hand, lung and prostate cancers are candidates for inverse comorbid associations with ASD. Joint perturbations in a set of specific biological processes underlie these associations which include several pathways previously implicated in both cancer and ASD encompassing immune system alterations, impairments of energy metabolism, cell cycle, and signaling through PI3K and G protein-coupled receptors among others. These findings could help to explain epidemiological observations pointing towards direct and inverse comorbid associations between ASD and specific cancer types and depict a complex scenario regarding the molecular patterns of association between ASD and cancer.
机译:流行病学和临床证据指向癌症作为自闭症谱系疾病(ASD)的人的合并症。还报道了两种疾病之间基因和生物过程的显着重叠。在此,我们首次进行了通过差异表达或报告基因,途径和预示基因,途径基因所获得的ASD型前皮质组织和22种癌症类型的基因表达谱。四种癌症类型(脑,甲状腺,肾脏和胰腺癌)在基因表达放管中呈现出显着重叠,与ASD相同,而两种癌症类型(肺和前列腺癌)显示差异表达谱在亚梁的相反方向上显着定化。功能性富集和LINCS L1000的药物型富集分析揭示了在两种疾病中共同影响的若干生物过程和途径的含义,包括免疫系统的损伤,以及氧化磷酸化和ATP合成中的损伤。我们的数据还表明,脑和肾癌在PI3K / AKT / MTOR轴上具有类似于ASD中的PI3K / AKT / MTOR轴的转录组体失衡模式。 ASD和癌症差异基因表达的比较META分析结果表明,脑,肾,甲状腺和胰腺癌是与ASD直接共用关联的候选者。另一方面,肺和前列腺癌是与ASD反向同血合作症的候选者。在一组特定的生物学过程中联合扰动提出了这些关联,其包括先前涉及癌症和ASD的几种途径,包括免疫系统改变,能量代谢,细胞周期和通过PI3K和G蛋白偶联的受体中的信号传导。这些发现可以有助于解释指向ASD和特异性癌症类型之间直接和逆同化性缔合的流行病学观察,并描绘了关于ASD和癌症之间关联的分子模式的复杂情景。

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