在 IL-32γ 过表达条件下,通过抑制 NF-κB 依赖性 ITGAV 和 TIMP-1 表达抑制皮肤癌发生。
Inhibition of skin carcinogenesis by suppression of NF-κB dependent ITGAV and TIMP-1 expression in IL-32γ overexpressed condition.
机构信息
College of Pharmacy and Medical Research Center, Chungbuk National University, Osongsaengmyeong 1-ro, Osong-eup, Heungdeok-gu, Cheongju, Chungbuk, 28160, Republic of Korea.
Hanbul Co, Ltd. R&D center, 634 Eon Ju-Ro, Gangnam-gu, Seoul, Republic of Korea.
出版信息
J Exp Clin Cancer Res. 2018 Nov 28;37(1):293. doi: 10.1186/s13046-018-0943-8.
BACKGROUND
Interleukin-32 (IL-32) has been associated with various diseases. Previous studies have shown that IL-32 inhibited the development of several tumors. However, the role of IL-32γ, an isotype of IL-32, in skin carcinogenesis remains unknown.
METHODS
We compared 7,12-Dimethylbenz[a]anthracene/12-O-Tetradecanoylphorbol-13-acetate (DMBA/TPA)-induced skin carcinogenesis in wild type (WT) and IL-32γ-overexpressing mice to evaluate the role of IL-32γ. We also analyzed cancer stemness and NF-κB signaling in skin cancer cell lines with or without IL-32γ expression by western blotting, quantitative real-time PCR and immunohistochemistry analysis.
RESULTS
Carcinogen-induced tumor incidence in IL-32γ mice was significantly reduced in comparison to that in WT mice. Infiltration of inflammatory cells and the expression levels of pro-inflammatory mediators were decreased in the skin tumor tissues of IL-32γ mice compared with WT mice. Using a genome-wide association study analysis, we found that IL-32 was associated with integrin αV (ITGAV) and tissue inhibitor of metalloproteinase-1 (TIMP-1), which are critical factor for skin carcinogenesis. Reduced expression of ITGAV and TIMP-1 were identified in DMBA/TPA-induced skin tissues of IL-32γ mice compared to that in WT mice. NF-κB activity was also reduced in DMBA/TPA-induced skin tissues of IL-32γ mice. IL-32γ decreased cancer cell sphere formation and expression of stem cell markers, and increased chemotherapy-induced cancer cell death. IL-32γ also downregulated expression of ITGAV and TIMP-1, accompanied with the inhibition of NF-κB activity. In addition, IL-32γ expression with NF-κB inhibitor treatment further reduced skin inflammation, epidermal hyperplasia, and cancer cell sphere formation and downregulated expression levels of ITGAV and TIMP-1.
CONCLUSIONS
These findings indicated that IL-32γ suppressed skin carcinogenesis through the inhibition of both stemness and the inflammatory tumor microenvironment by the downregulation of TIMP-1 and ITGAV via inactivation of NF-κB signaling.
背景
白细胞介素-32(IL-32)与多种疾病相关。先前的研究表明,IL-32 抑制了几种肿瘤的发展。然而,白细胞介素-32γ(IL-32 的一种同工型)在皮肤癌变中的作用尚不清楚。
方法
我们比较了野生型(WT)和 IL-32γ过表达小鼠中 7,12-二甲基苯并[a]蒽/12-O-十四烷酰佛波醇-13-乙酸酯(DMBA/TPA)诱导的皮肤癌变,以评估 IL-32γ 的作用。我们还通过 Western blot、定量实时 PCR 和免疫组织化学分析,分析了具有或不具有 IL-32γ 表达的皮肤癌细胞系中的癌症干性和 NF-κB 信号。
结果
与 WT 小鼠相比,IL-32γ 小鼠中致癌物诱导的肿瘤发生率明显降低。与 WT 小鼠相比,IL-32γ 小鼠皮肤肿瘤组织中炎症细胞的浸润和促炎介质的表达水平降低。通过全基因组关联研究分析,我们发现 IL-32 与整合素 αV(ITGAV)和金属蛋白酶组织抑制剂-1(TIMP-1)相关,它们是皮肤癌变的关键因素。与 WT 小鼠相比,DMBA/TPA 诱导的 IL-32γ 小鼠皮肤组织中 ITGAV 和 TIMP-1 的表达减少。DMBA/TPA 诱导的 IL-32γ 小鼠皮肤组织中的 NF-κB 活性也降低。IL-32γ 减少了癌细胞球的形成和干细胞标志物的表达,并增加了化疗诱导的癌细胞死亡。IL-32γ 还下调了 ITGAV 和 TIMP-1 的表达,同时抑制了 NF-κB 活性。此外,用 NF-κB 抑制剂处理 IL-32γ 表达进一步减少了皮肤炎症、表皮过度增生、癌细胞球形成,并下调了 ITGAV 和 TIMP-1 的表达水平。
结论
这些发现表明,IL-32γ 通过下调 TIMP-1 和 ITGAV 抑制 NF-κB 信号转导,抑制干性和炎症性肿瘤微环境,从而抑制皮肤癌变。
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