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Evaluating the associations between human circadian rhythms and dysregulated genes in liver cancer cells

机译:评估肝癌细胞中人昼夜节律和呼吸失调基因的关联

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Network analysis is a useful approach in cancer biology as it provides information regarding the genes and proteins. In our previous study, a network analysis was performed on dysregulated genes in HepG2 cells, a hepatoblastoma cell line that lacks the viral infection, compared with normal hepatocytes, identifying the presence of 26 HUB genes. The present study aimed to identify whether these previously identified HUB genes participate in the network that controls the human circadian rhythms. The results of the present study demonstrated that 20/26 HUB genes were associated with the metabolic processes that control human circadian rhythms, which supports the hypothesis that a number of cancer types are dependent from circadian cycles. In addition, it was revealed that the CLOCK circadian regulator gene was associated, via cytoskeleton associated protein 5 (CKAP5), with the HUB genes of the HepG2 network, and that CKAP5 was associated with three other circadian genes (casein kinase 1 epsilon, casein kinase 1 delta and histone deacetylase 4) and 10 HepG2 genes (SH2 domain containing, ZW10 interacting kinetochore protein, aurora kinase B, cell division cycle 20, centromere protein A, inner centromere protein, mitotic arrest deficient 2 like 1, baculoviral IAP repeat containing 5, SPC24 NDC80 kinetochore complex component and kinesin family member 2C). Furthermore, the genes that associate the circadian system with liver cancer were demonstrated to encode intrinsically disordered proteins. Finally, the results of the present study identified the microRNAs involved in the network formed by the overlapping of HepG2 and circadian genes.
机译:网络分析是癌症生物学中的有用方法,因为它提供了关于基因和蛋白质的信息。在我们以前的研究中,对HepG2细胞中的失调基因进行了网络分析,与常规肝细胞相比,缺乏病毒感染的肝脏细胞系,鉴定26个枢纽基因的存在。本研究旨在识别这些先前已识别的集线器基因是否参与控制人昼夜节律的网络。本研究的结果表明,20/26个枢纽基因与控制人昼夜节律的代谢过程相关,这支持许多癌症类型从昼夜循环取决于癌症的假设。此外,揭示了时钟昼夜节律调节剂基因通过细胞骨架相关蛋白5(CKAP5)与HepG2网络的中心基因相关联,并且CKAP5与其他三种昼夜昼夜基因有关(酪蛋白激酶1 epsilon,酪蛋白激酶1 delta和组蛋白脱乙酰酶4)和10 hepg2基因(含有zw10相互作用的kinetochore蛋白,极光激酶b,细胞分裂循环20,centromere蛋白A,内厘米蛋白,有丝分裂滞留缺乏2,如1,杆状病毒Iap重复含有5,SPC24 NDC80 Kinetochore复杂组件和Kinesin家族2C)。此外,证明将肝癌与肝癌相关联的基因以编码本质无序的蛋白质。最后,本研究的结果鉴定了通过HepG2和昼夜节律基因的重叠形成的网络中涉及的MicroRNA。

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