首页> 外文期刊>Journal of Cell Communication and Signaling >Stable expression of α1-antitrypsin Portland in MDA-MB-231 cells increased MT1-MMP and MMP-9 levels, but reduced tumour progression.
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Stable expression of α1-antitrypsin Portland in MDA-MB-231 cells increased MT1-MMP and MMP-9 levels, but reduced tumour progression.

机译:MDA-MB-231细胞中α1抗抗果皮波特兰的稳定表达增加了MT1-MMP和MMP-9水平,但减少了肿瘤进展。

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The membrane bound matrix metalloproteinase MT1-MMP plays roles in modulating cell movement, independent of its abilities to remodel the extracellular matrix. Unlike many MMPs, MT1-MMP is activated in the Golgi prior to secretion by a pro-protein convertase, primarily furin. Regulation of the activation of pro-MT1-MMP has been methodically investigated, as altering the level of the active protein has broad implications in both activating other pro-MMPs, including pro-MMP-2, and many subsequent remodelling events. Our previous work in MCF-7 cells has demonstrated that modest, and not extremely high, levels of active MT1-MMP manifests into altered cell morphology and movement. At this low but optimal amount of MT1-MMP protein, changes to MT1-MMP levels are always mirrored by MMP-9 and pERK levels, and always opposite to MMP-2 levels. In this study, stable expression of the furin inhibitor α1-antitrypsin Portland (α1-PDX) in MDA-MB-231 cells increased overall MT1-MMP levels, but cells maintained a 21% proportion of pro-MT1-MMP. The increase in MT1-MMP was mirrored by increases in MMP-9 and pERK, but a decrease in MMP-2. These changes were associated with increased NF-κB transcription. In vitro analysis showed that α1-PDX decreased cell protrusions and migration, and this manifested as decreased tumourigenesis when examined in vivo using a chick CAM assay.
机译:膜结合的基质金属蛋白酶MT1-MMP在调节细胞运动中起作用,与其改造细胞外基质的能力无关。与许多MMP不同,在通过Pro-蛋白转化酶分泌之前,在Golgi中激活MT1-MMP,主要是Furin。已经有条理地研究了Pro-MT1-MMP活化的调节,随着活性蛋白质的改变在激活其他Pro-MMP(包括Pro-MMP-2和许多后续重塑事件)中具有广泛意义。我们以前的MCF-7细胞的工作表明,适度,而不是极高,活性MT1-MMP的水平显现为改变的细胞形态和运动。在这种低但最佳的MT1-MMP蛋白质中,MT1-MMP水平的变化始终由MMP-9和PERK水平镜像,并且始终与MMP-2级相反。在该研究中,MDA-MB-231细胞中Furin抑制剂α1-抗酸酯素(α1-P​​DX)的稳定表达增加了总MT1-MMP水平,但细胞保持了21%的PRO-MT1-MMP比例。 MT1-MMP的增加通过MMP-9和PERK增加而镜像,但MMP-2的降低。这些变化与增加的NF-κB转录有关。体外分析表明,α1-PDX减少细胞突起和迁移,并且当使用小鸡凸轮测定在体内检查时,这种情况表现为下降的肿瘤内血。

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