内质网应激介导的 JNK/c-Jun信号通路在雷公藤内酯醇诱导小鼠体内黑色素瘤A375细胞凋亡中的作用研究

doi:10.35541/cjd.20230415

Abstract

Abstract: 【Abstract】 Objective To explore the role of c-Jun N-terminal kinase （JNK）/c-Jun signaling pathway mediated by endoplasmic reticulum stress in triptolide-induced apoptosis of melanoma A375 cells. Methods Nude mice were subcutaneously inoculated with melanoma A375 cells on the back to establish the animal model of melanoma. Tumor formation could be observed at approximately 3 weeks after inoculation, and then the mice were divided into 4 groups （4 mice in each group）: control group （injected with sodium chloride physiological solution via the tail vein）, 0.1-, 0.2-, and 0.4-mg/kg triptolide groups （injected with 0.1, 0.2, and 0.4 mg/kg triptolide via the tail vein, respectively）. Injections were performed twice a week. After 3 weeks of injections, tumors were resected, and their size and weight were measured. The apoptosis levels of tumor xenografts were detected by the terminal deoxyribonucleotide transferase-mediated dUTP nick end labeling （TUNEL） assay. qPCR was conducted to determine the mRNA expression of inositol-requiring enzyme 1 （IRE1）, JNK, and c-Jun, and Western blot analysis to determine the protein expression of IRE1, JNK, c-Jun, phosphorylated-JNK （p-JNK）, and phosphorylated-c-Jun （p-c-Jun）. Comparisons among multiple groups were performed using one-way analysis of variance, and multiple comparisons were performed using Dunnett's test. Results Significant differences were observed in the tumor mass, volume and tumor suppression rate among the control group, 0.1-, 0.2-, and 0.4-mg/kg triptolide groups （all P < 0.05）; all the triptolide groups showed significantly decreased tumor masses and volumes （all P < 0.05）, but significantly increased tumor suppression rates compared with the control group （all P < 0.05）. The tumor apoptosis index significantly differed among the control group, 0.1-, 0.2-, and 0.4-mg/kg triptolide groups （7.67% ± 1.15%, 9.67% ± 3.21%, 62.00% ± 6.08%, and 85.67% ± 5.51%, respectively; F = 305.91, P < 0.01）, and the 0.2- and 0.4-mg/kg triptolide groups showed significantly increased tumor apoptosis indices compared with the control group （t = 17.56, 27.72, respectively, both P < 0.05）. qPCR and Western blot analysis revealed significant differences in the mRNA expression of IRE1, JNK, and c-Jun among the control group, 0.1-, 0.2-, and 0.4-mg/kg triptolide groups （F = 112.23, 27.51, 112.37, respectively, all P < 0.05）, as well as in the relative protein expression levels of IRE1, JNK, c-Jun, p-JNK, and p-c-Jun among the above 4 groups （all P < 0.05）. Additionally, the 0.4-mg/kg triptolide group showed significantly increased mRNA and protein expression of IRE1, JNK and c-Jun （including p-JNK, p-c-Jun） compared with the control group （all P < 0.05）. The mRNA and protein expression levels of IRE1, JNK, and c-Jun in the tumor tissues tended to increase with the rise in drug concentrations, and the protein expression levels of p-JNK and p-c-Jun showed the same trend. Conclusion Triptolide could activate the JNK/c-Jun signaling pathway mediated by the endoplasmic reticulum stress, and then induce apoptosis of melanoma A375 cells in mice.

Key words: Melanoma, Triptolide, Endoplasmic reticulum stress, Apoptosis, A375 cells, JNK/c-Jun signaling pathway

Zhang Yamei, Liu Guohao, Tao Yue, Bao Jun. Role of JNK/c-Jun signaling pathway mediated by endoplasmic reticulum stress in triptolide-induced apoptosis of melanoma A375 cells in mice[J]. Chinese Journal of Dermatology, 2024, 57(8): 709-714.doi:10.35541/cjd.20230415

References ［14］

［1］	陶玥, 马鹏程, 孙建方, 等. 雷公藤内酯醇对人黑素瘤M14细胞系增殖与凋亡的影响［J］. 中华皮肤科杂志, 2012,45（9）:641⁃643. doi: 10.3760/cma.j.issn.0412⁃4030.2012.09.010.
［2］	陶玥, 张孟丽, 马鹏程, 等. 丹皮酚对人黑素瘤A375细胞增殖和凋亡的影响［J］. 中华皮肤科杂志, 2014,47（6）:393⁃396. doi: 10.3760/cma.j.issn.0412⁃4030.2014.06.005.
［3］	张亚美, 孙悦鑫, 陶玥, 等. CHOP依赖内质网应激通路在雷公藤内酯醇诱导黑素瘤A375细胞凋亡中的作用机制［J］. 中华皮肤科杂志, 2018,51（4）:288⁃293. doi: 10.3760/cma.j.issn.0412⁃4030.2018.04.010.
［4］	吴欣怡, 刘长安, 龚建平, 等. 内质网应激介导细胞凋亡及免疫炎症反应的研究进展［J］. 国际免疫学杂志, 2022,45（1）:69⁃73. doi: 10.3760/cma.j.issn.1673⁃4394.2022.01.012.
［5］	曹丽婷, 马宝慧. JNK信号通路在细胞凋亡与自噬中作用的研究进展［J］. 包头医学院学报, 2022,38（1）:88⁃91. doi: 10. 16833/j.cnki.jbmc.2022.01.021.
［6］	Wang SY, Gao K, Deng DL, et al. TLE4 promotes colorectal cancer progression through activation of JNK/c⁃Jun signaling pathway［J］. Oncotarget, 2016,7（3）:2878⁃2888. doi: 10.18632/oncotarget.6694.
［7］	Lee J, Sohn EJ, Yoon S, et al. Activation of JNK and IRE1 is critically involved in tanshinone I⁃induced p62 dependent autophagy in malignant pleural mesothelioma cells: implication of p62 UBA domain［J］. Oncotarget, 2017,8（15）:25032⁃25045. doi: 10.18632/oncotarget.15336.
［8］	Chen S, Wang Y, Yang Y, et al. Psoralen inhibited apoptosis of osteoporotic osteoblasts by modulating IRE1⁃ASK1⁃JNK pathway［J］. Biomed Res Int, 2017,2017:3524307. doi: 10.1155/2017/3524307.
［9］	Janda E, Lascala A, Carresi C, et al. Parkinsonian toxin⁃induced oxidative stress inhibits basal autophagy in astrocytes via NQO2/quinone oxidoreductase 2: Implications for neuroprotection［J］. Autophagy, 2015,11（7）:1063⁃1080. doi: 10.1080/15548627.2015. 1058683.
［10］	Chen J, Ye C, Wan C, et al. The roles of c⁃Jun N⁃terminal kinase （JNK） in infectious diseases［J］. Int J Mol Sci, 2021,22（17）:9640. doi: 10.3390/ijms22179640.
［11］	Wang G, Zhao Z, Ren B, et al. Exenatide exerts a neuroprotective effect against diabetic cognitive impairment in rats by inhibiting apoptosis: Role of the JNK/c‑JUN signaling pathway［J］. Mol Med Rep, 2022,25（4）:111 ［pii］. doi: 10.3892/mmr.2022.12627.
［12］	雍熙, 王贤芝, 张富钊, 等. 基于JNK/c⁃Jun信号通路探讨孟鲁司特钠抑制小鼠腹主动脉瘤形成的机制［J］. 中国老年学杂志, 2021,41（13）:2828⁃2832. doi: 10.3969/j.issn.1005⁃9202. 2021.13.040.
［13］	Li GJ, Yang QH, Yang GK, et al. MiR⁃137 regulates low⁃intensity shear stress⁃induced human aortic endothelial cell apoptosis via JNK/AP⁃1 signaling［J］. J Physiol Biochem, 2021,77（3）:451⁃460. doi: 10.1007/s13105⁃021⁃00812⁃1.
［14］	李青青, 陆刚, 丁怿虹, 等. 脓毒症诱导小鼠淋巴器官JNK和CHOP凋亡途径及刺激炎性细胞因子的变化［J］. 中华危重病急救医学, 2020,32（10）:1194⁃1198. doi: 10.3760/cma.j.cn121430⁃ 20200422⁃00321.

[1]	Wang Guanyu, Sun Jiachen, Li Tingting, Wang Yimeng, Zhang Chunlei. Antitumor effects and mechanisms of action of chidamide combined with curcumin in the treatment of cutaneous T-cell lymphoma [J]. Chinese Journal of Dermatology, 2024, 57(8): 728-738.
[2]	Li Jing, Li Zhi, Yu Yin, Liu Sutao, Diao Qingchun, Wang Can. Role of antioncogenes ADCY2/4/5/8 in cutaneous melanoma [J]. Chinese Journal of Dermatology, 2024, 57(8): 698-708.
[3]	Chen Jiaxi, Yi Xiuli, Li Chunying, Li Shuli. Study on the protective effect of folic acid against oxidative stress-induced damage to melanocytes in vitro [J]. Chinese Journal of Dermatology, 2024, 57(6): 547-552.
[4]	Tian Cuicui, Shi Haoze, Chen Hao. Effect of the Na+/Ca2+ exchanger inhibitor bepridil on the proliferation, migration and apoptosis of melanoma cells [J]. Chinese Journal of Dermatology, 2024, 57(6): 530-538.
[5]	Liu Lyuye, Zhang Junling. Ferroptosis in common skin diseases [J]. Chinese Journal of Dermatology, 2024, 0(3): 20220783-e20220783.
[6]	Yan Kexin, Xu Xiulian. Nanomedicine: a new strategy for the diagnosis and treatment of melanoma [J]. Chinese Journal of Dermatology, 2024, 0(3): 20230109-e20230109.
[7]	Skin Cancer Research Group, Committee on Dermatology, Chinese Association of Integrative Medicine, Melanoma Society of China Anti-Cancer Association. Expert consensus on human interferon α1b for the treatment of melanoma （2024） [J]. Chinese Journal of Dermatology, 2024, 57(1): 1-7.
[8]	Dong Dong, Liu Tianyi. Cell metabolism and metastasis of cutaneous malignant melanoma [J]. Chinese Journal of Dermatology, 2023, 56(9): 878-881.
[9]	Chen Fangqi, Liang Yan, Wu Ting, Huang Changzheng. Associations between m6A RNA methylation and cutaneous melanoma [J]. Chinese Journal of Dermatology, 2023, 56(9): 889-892.
[10]	Yuan Xingang, Ni Sili, Zhang Jian, Luo Xiaoyan, Wang Hua. Improving diagnosis and treatment of melanocytic nevi in children: an urgent need [J]. Chinese Journal of Dermatology, 2023, 56(8): 782-786.
[11]	Tang Zhiming, Jing Mengqing, Lu Lu, Shan Xiao, Zhang Cuixia, Zhang Xiaoyu, Meng Sa. Effect of Xidi Liangxue recipe on the proliferation and apoptosis of HaCaT cells through the lncRNA NEAT1/miR-485-5p/STAT3 regulatory network [J]. Chinese Journal of Dermatology, 2023, 56(7): 642-650.
[12]	Li Jiaqi, Ye Feng, Ju Qiang. Symbiotic homeostasis of Staphylococcus epidermidis is associated with common skin disorders [J]. Chinese Journal of Dermatology, 2023, 56(5): 459-462.
[13]	Zhang Congcong, Chen Hao. Spitzoid melanocytic tumors [J]. Chinese Journal of Dermatology, 2023, 56(5): 463-467.
[14]	Chen Yi, Song Xiuzu. Role of transient receptor potential channels in melanocytes and their related diseases [J]. Chinese Journal of Dermatology, 2023, 56(4): 376-379.
[15]	Yang Kaiying, Gong Xue, Qiu Tong, Zhou Jiangyuan, Lan Yuru, Ji Yi. Effects of the key glycolytic enzyme PFKFB3 on the proliferation, migration and apoptosis of hemangioma-derived endothelial cells [J]. Chinese Journal of Dermatology, 2023, 56(4): 320-324.

Role of JNK/c-Jun signaling pathway mediated by endoplasmic reticulum stress in triptolide-induced apoptosis of melanoma A375 cells in mice

PDF

Knowledge

Abstract

Cite this article

share this article

References ［14］

Related Articles 15

Metrics

Comments

Recommended 10