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首页> 外文期刊>Turkish journal of biology >Knockdown of SET Domain, Bifurcated 1 suppresses head and neck cancer cell viability and wound-healing ability in vitro
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Knockdown of SET Domain, Bifurcated 1 suppresses head and neck cancer cell viability and wound-healing ability in vitro

机译:设定域的敲低,分叉1抑制了头部和颈部癌细胞活力和伤口愈合能力

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摘要

Head and neck cancer (HNC) is the sixth most common cancer worldwide and therefore presents a global public health problem. There are no standard algorithms for the diagnosis and follow-up of the disease, and no effective current treatment approaches exist. Therefore, the discovery of new biomolecules and the design of new strategies to aid in early diagnosis is necessary, along with establishing prognostic factors of HNC. In several cancer studies, the upregulation of SET Domain, Bifurcated 1 (SETDB1) has been reported to be tumor-inducing and to indicate a cancer-invasive prognosis, leading to the modulation of genes associated with different signaling pathways; however, the literature is sparse regarding the relationship between SETDB1 and HNC.?In our study, three HNC primary cell lines and their corresponding metastatic cell lines were used. The quantitative reverse transcriptase-polymerase chain reaction and western blotting data indicated that the SETDB1 mRNA and protein expression levels were higher in all metastatic cell lines compared to their primary cell lines (P 0.05 for all). To investigate the role of SETDB1 in HNC biology, in vitro functional analyses were carried out using small interference RNA (siRNA) technology, cell viability, scratch wound-healing, and the caspase-3 activity assay of gene expression of SETDB1 to compare primary and metastatic cell lines of HNC. Metastatic cells were more susceptible to this suppression, which decreased the vitality of cells and their ability of wound-healing and induced level of caspase-3 activity?(P 0.05 for all). This functional study has shown that SETDB1 plays an important role in head and neck carcinogenesis. Therefore, SETDB1 may be an attractive therapeutic target molecule and also a potential diagnostic and prognostic biomarker in HNC.
机译:头部和颈部癌症(HNC)是全世界第六次常见的癌症,因此提出了全球公共卫生问题。疾病的诊断和随访没有标准算法,并且没有存在有效的电流处理方法。因此,有必要发现新的生物分子和新策略的设计,以及建立HNC的预后因素。在几种癌症研究中,据报道,套结构结构域的上调,分叉1(SetdB1)是肿瘤诱导和表明癌症侵入性预后,导致与不同信号通路相关的基因的调节;然而,文献对SetDB1和HNC之间的关系稀疏。我们的研究,使用了三种HNC主细胞系及其相应的转移细胞系。定量逆转录酶 - 聚合酶链反应和蛋白质印迹数据表明,与其主要细胞系(P <0.05)相比,所有转移性细胞系中的SETDB1 mRNA和蛋白表达水平较高。为了探讨SetDB1在HNC生物学中的作用,使用小的干扰RNA(siRNA)技术,细胞活力,划伤伤口愈合以及SetDB1的基因表达的Caspase-3活性测定来进行体外功能分析。 HNC的转移性细胞系。转移细胞更容易受到这种抑制的影响,这降低了细胞的活力及其伤口愈合能力和诱导的Caspase-3活性水平?(P <全部)。该功能研究表明,SetDB1在头部和颈部致癌物中起重要作用。因此,SetDB1可以是有吸引力的治疗靶分子,以及HNC中的潜在诊断和预后生物标志物。

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