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首页> 外文期刊>Molecular Therapy - Oncolytics >Upregulated CBX8 Promotes Cancer Metastasis via the WNK2/MMP2 Pathway
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Upregulated CBX8 Promotes Cancer Metastasis via the WNK2/MMP2 Pathway

机译:上调CBX8通过WNK2 / MMP2途径促进癌症转移

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Metastasis is associated with poor prognosis in cancer and is a multistep process that includes invasion and migration. Several epigenetic factors are involved in this process, including chromobox protein homolog 8 ( CBX8 ). Here, we show that CBX8 is overexpressed in many cancers compared with normal tissues. Functional analyses indicated that CBX8 promoted invasion and migration in glioblastoma, breast cancer, and lung cancer in?vitro and in?vivo . WNK2 was identified as a target gene of CBX8 , which interacted with the WNK2 promoter to suppress WNK2 expression and activity. WNK2 acted as an antioncogene, and decreased WNK2 levels resulted in high activity of matrix metalloprotease (MMP)-2 and RAC1 , which play a central role in invasion and migration, respectively. There was a positive relationship between MMP2 and RAC1 activity in CBX8 -modulated cell lines. In addition, WNK2 negatively regulated MMP2 and RAC1 activity. Collectively, the results indicated that CBX8 promoted invasion and migration by targeting WNK2 , which resulted in increased RAC1 and MMP2 expression and activity. Therefore, CBX8 may be a novel therapeutic target to treat metastatic cancers.
机译:转移与癌症预后差有关,是一个包括入侵和迁移的多步骤过程。在该过程中涉及多种表观遗传因素,包括ChromoBox蛋白质同源物8(CBX8)。在这里,与正常组织相比,我们表明CBX8在许多癌症中过表达。功能分析表明,CBX8促进了胶质母细胞瘤,乳腺癌和肺癌中的侵袭和迁移?体外,血液肿瘤。将WNK2鉴定为CBX8的靶基因,其与WNK2启动子相互作用以抑制WNK2表达和活性。 WNK2用作抗苏硫代硫基,并且降低的WNK2水平导致基质金属蛋白酶(MMP)-2和RAC1的高活性分别在侵袭和迁移中起着核心作用。在CBX8-剪发的细胞系中MMP2和RAC1活动之间存在正相关关系。此外,WNK2负调节MMP2和RAC1活动。总的来说,结果表明CBX8通过靶向WNK2促进侵袭和迁移,导致RAC1和MMP2表达和活性增加。因此,CBX8可以是治疗转移性癌症的新型治疗靶。

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