mTORC1/autophagy-regulated MerTK in mutant BRAFV600 melanoma with acquired resistance to BRAF inhibition

被引:21
|
作者
Xue, Gongda [1 ]
Kohler, Reto [1 ]
Tang, Fengyuan [1 ,2 ]
Hynx, Debby [1 ]
Wang, Yuhua [1 ]
Orso, Francesca [3 ,4 ]
Pretre, Vincent [2 ]
Ritschard, Reto [2 ]
Hirschmann, Petra [5 ]
Cron, Peter [1 ]
Roloff, Tim [1 ]
Dummer, Reinhard [6 ]
Mandala, Mario [7 ]
Bichet, Sandrine [1 ]
Genoud, Christel [1 ]
Meyer, Alexandra G. [1 ]
Muraro, Manuele G. [2 ]
Spagnoli, Giulio C. [2 ]
Taverna, Daniela [3 ,4 ]
Ruegg, Curzio [8 ]
Merghoub, Taha [9 ]
Massi, Daniela [10 ]
Tang, Huifang [11 ]
Levesque, Mitchell P. [6 ]
Dirnhofer, Stephan [4 ,5 ]
Zippelius, Alfred [2 ]
Hemmings, Brian A. [1 ]
Wicki, Andreas [2 ]
机构
[1] Friedrich Miescher Inst Biomed Res, Dept Mech Canc, Basel, Switzerland
[2] Univ Hosp Basel, Dept Biomed, Basel, Switzerland
[3] Univ Turin, Mol Biotechnol Ctr, Turin, Italy
[4] Univ Turin, Dept Mol Biotechnol & Hlth Sci, Turin, Italy
[5] Univ Basel, Inst Pathol, Basel, Switzerland
[6] Univ Hosp Zurich, Dept Dermatol, Zurich, Switzerland
[7] Papa Giovanni XXIII Hosp, Dept Oncol & Hematol, Unit Clin & Translat Res, Bergamo, Italy
[8] Univ Fribourg, Dept Med, Fribourg, Switzerland
[9] Mem Sloan Kettering Canc Ctr, Ludwig Ctr Canc Immunotherapy, 1275 York Ave, New York, NY 10021 USA
[10] Univ Florence, Div Pathol Anat, Dept Surg & Translat Med, Florence, Italy
[11] Zhejiang Univ, Sch Basic Med Sci, Dept Pharmacol, Hangzhou, Zhejiang, Peoples R China
来源
ONCOTARGET | 2017年 / 8卷 / 41期
基金
瑞士国家科学基金会;
关键词
Mer tyrosine kinase; drug resistance; BRAF mutation; Zeb2; autophagy; RECEPTOR TYROSINE KINASE; AUTOPHAGY MODULATION; THERAPEUTIC TARGET; TUMOR PROGRESSION; DRUG-RESISTANCE; MICE LACKING; DOUBLE-BLIND; CANCER; EMT; CELLS;
D O I
10.18632/oncotarget.18213
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
BRAF inhibitors (BRAFi) and the combination therapy of BRAF and MEK inhibitors (MEKi) were recently approved for therapy of metastatic melanomas harbouring the oncogenic BRAFV600 mutation. Although these therapies have shown pronounced therapeutic efficacy, the limited durability of the response indicates an acquired drug resistance that still remains mechanistically poorly understood at the molecular level. We conducted transcriptome gene profiling in BRAFi-treated melanoma cells and identified that Mer tyrosine kinase (MerTK) is specifically upregulated. MerTK overexpression was demonstrated not only in melanomas resistant to BRAFi monotherapy (5 out of 10 samples from melanoma patients) but also in melanoma resistant to BRAFi+MEKi (1 out of 3), although MEKi alone does not affect MerTK. Mechanistically, BRAFi-induced activation of Zeb2 stimulates MerTK in BRAFV600 melanoma through mTORC1-triggered activation of autophagy. Co-targeting MerTK and BRAFV600 significantly reduced tumour burden in xenografted mice, which was pheno-copied by co-inhibition of autophagy and mutant BRAFV600.
引用
收藏
页码:69204 / 69218
页数:15
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