MT4-MMP and EGFR expression levels are key biomarkers for breast cancer patient response to chemotherapy and erlotinib

被引:15
|
作者
Yip, Cassandre [1 ]
Foidart, Pierre [1 ,2 ,3 ]
Somja, Joan [4 ]
Truong, Alice [1 ]
Lienard, Mehdi [1 ]
Feyereisen, Emilie [1 ]
Schroeder, Helene [2 ]
Gofflot, Stephanie [5 ]
Donneau, Anne-Francoise [6 ]
Collignon, Joelle [2 ]
Delvenne, Philippe [4 ]
Sounni, Nor Eddine [1 ]
Jerusalem, Guy [2 ,3 ]
Noel, Agnes [1 ]
机构
[1] Univ Liege, Lab Tumor & Dev Biol, GIGA Canc, B-4000 Liege, Belgium
[2] Univ Hosp Liege CHU, Dept Med Oncol, B-4000 Liege, Belgium
[3] Univ Liege, Fac Med, B-4000 Liege, Belgium
[4] Univ Liege, GIGA Canc, Lab Expt Pathol, B-4000 Liege, Belgium
[5] Univ Liege, Biotheque Univ Liege, Biobank, B-4000 Liege, Belgium
[6] Univ Liege, Dept Biostat, B-4000 Liege, Belgium
关键词
triple-negative breast cancer; MT4-MMP; EGFR; chemotherapy; erlotinib; biomarker; MATRIX-METALLOPROTEINASE MT4-MMP; TRIPLE-NEGATIVE PHENOTYPE; RANDOMIZED PHASE-II; CARCINOMA; METASTASIS; MORPHOLOGY; CETUXIMAB; GROWTH; BASAL;
D O I
10.1038/bjc.2017.23
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background: Triple-negative breast cancers (TNBC) are heterogeneous cancers with poor prognosis. We aimed to determine the clinical relevance of membrane type-4 matrix metalloproteinase (MT4-MMP), a membrane type matrix metalloproteinase that interacts with epidermal growth factor receptor (EGFR) overexpressed in >50% of TNBC. Methods: We conducted a retrospective immunohistochemical analysis on human TNBC samples (n = 81) and validated our findings in in vitro and in vivo assays. Results: Membrane type-4 matrix metalloproteinase and EGFR are produced in 72.5% of TNBC samples, whereas those proteins are faintly produced by healthy tissues. Unexpectedly, tumour relapse after chemotherapy was reduced in samples highly positive for MT4-MMP. Mechanistically, this is ascribed to a higher sensitivity of MT4-MMP-producing cells to alkylating or intercalating chemotherapeutic agents, as assessed in vitro. In sharp contrast, MT4-MMP expression did not affect tumour cell sensitivity to paclitaxel that interferes with protease trafficking. Importantly, MT4-MMP expression sensitised cancer cells to erlotinib, a tyrosine kinase EGFR inhibitor. In a pre-clinical model, the growth of MT4-MMP overexpressing xenografts, but not of control ones, was reduced by epirubicin or erlotinib. The combination of suboptimal drug doses blocked drastically the growth of MT4-MMP-producing tumours. Conclusions: We demonstrate that MT4-MMP defines a sub-population of TNBC sensitive to a combination of DNA-targeting chemotherapeutic agents and anti-EGFR drugs.
引用
收藏
页码:742 / 751
页数:10
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