角蛋白6驱动的鸟氨酸脱羧酶在毛囊角质形成细胞中的表达通过负向调节Notch信号通路增强干性和肿瘤发生。
Keratin-6 driven ODC expression to hair follicle keratinocytes enhances stemness and tumorigenesis by negatively regulating Notch.
作者信息
Arumugam Aadithya, Weng Zhiping, Chaudhary Sandeep C, Afaq Farrukh, Elmets Craig A, Athar Mohammad
机构信息
Department of Dermatology, University of Alabama at Birmingham, Birmingham, AL 35294-0019, USA.
Department of Dermatology, University of Alabama at Birmingham, Birmingham, AL 35294-0019, USA; Skin Diseases Research Center, University of Alabama at Birmingham, Birmingham, AL 35294, USA.
出版信息
Biochem Biophys Res Commun. 2014 Aug 29;451(3):394-401. doi: 10.1016/j.bbrc.2014.07.129. Epub 2014 Aug 2.
Over-expression of ornithine decarboxylase (ODC) is known to be involved in the epidermal carcinogenesis. However, the mechanism by which it enhances skin carcinogenesis remains undefined. Recently, role of stem cells localized in various epidermal compartments has been shown in the pathogenesis of skin cancer. To direct ODC expression in distinct epidermal compartments, we have developed keratin 6 (K6)-ODC/SKH-1 and keratin 14 (K14)-ODC/SKH-1 mice and employed them to investigate the role of ODC directed to these epidermal compartments on UVB-induced carcinogenesis. K6-driven ODC over-expression directed to outer root sheath (ORS) of hair follicle was more effective in augmenting tumorigenesis as compared to mice where K14-driven ODC expression was directed to inter-follicular epidermal keratinocytes. Chronically UVB-irradiated K6-ODC/SKH-1 developed 15±2.5 tumors/mouse whereas K14-ODC/SKH-1 developed only 6.8±1.5 tumors/mouse. K6-ODC/SKH-1 showed augmented UVB-induced proliferation and much higher pro-inflammatory responses than K14-ODC/SKH-1 mice. Tumors induced in K6-ODC/SKH-1 were rapidly growing, invasive and ulcerative squamous cell carcinoma (SCC) showing decreased expression of epidermal polarity marker E-cadherin and enhanced mesenchymal marker, fibronectin. Interestingly, the number of CD34/CK15/p63 positive stem-like cells was significantly higher in chronically UVB-irradiated K6-ODC/SKH-1 as compared to K14-ODC/SKH-1 mice. Reduced Notch1 expression was correlated with the expansion of stem cell compartment in these animals. However, other signaling pathways such as DNA damage response or mTOR signaling pathways were not significantly different in tumors induced in these two murine models suggesting the specificity of Notch pathway in this regard. These data provide a novel role of ODC in augmenting tumorigenesis via negatively regulated Notch-mediated expansion of stem cell compartment.
已知鸟氨酸脱羧酶(ODC)的过表达与表皮癌发生有关。然而,其增强皮肤癌发生的机制仍不明确。最近,已表明定位于不同表皮区室的干细胞在皮肤癌发病机制中发挥作用。为了在不同的表皮区室中定向表达ODC,我们构建了角蛋白6(K6)-ODC/SKH-1和角蛋白14(K14)-ODC/SKH-1小鼠,并利用它们来研究定向到这些表皮区室的ODC在紫外线B(UVB)诱导的癌发生中的作用。与K14驱动的ODC表达定向到毛囊间表皮角质形成细胞的小鼠相比,K6驱动的ODC过表达定向到毛囊外根鞘(ORS)在增强肿瘤发生方面更有效。长期UVB照射的K6-ODC/SKH-1小鼠每只发生15±2.5个肿瘤,而K14-ODC/SKH-1小鼠每只仅发生6.8±1.5个肿瘤。与K14-ODC/SKH-1小鼠相比,K6-ODC/SKH-1表现出UVB诱导的增殖增强和更高的促炎反应。K6-ODC/SKH-1诱导的肿瘤是快速生长、侵袭性和溃疡性鳞状细胞癌(SCC),表现为表皮极性标志物E-钙黏蛋白表达降低和间充质标志物纤连蛋白表达增强。有趣的是,与K14-ODC/SKH-1小鼠相比,长期UVB照射的K6-ODC/SKH-1中CD34/CK15/p63阳性干细胞样细胞的数量显著更高。Notch1表达降低与这些动物中干细胞区室的扩张相关。然而,在这两种小鼠模型诱导的肿瘤中,其他信号通路如DNA损伤反应或mTOR信号通路没有显著差异,这表明Notch通路在这方面具有特异性。这些数据揭示了ODC在通过负调控Notch介导的干细胞区室扩张增强肿瘤发生中的新作用。
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