Defective Cyclin B1 Induction in Trastuzumab-emtansine (T-DM1) Acquired Resistance in HER2-positive Breast Cancer

被引:80
|
作者
Sabbaghi, Mohammad A. [1 ]
Gil-Gomez, Gabriel [1 ]
Guardia, Cristina [1 ]
Servitja, Sonia [1 ,2 ]
Arpi, Oriol [1 ]
Garcia-Alonso, Sara [3 ]
Menendez, Silvia [1 ]
Arumi-Uria, Montserrat [4 ]
Serrano, Laia [4 ]
Salido, Marta [1 ,4 ]
Muntasell, Aura [5 ]
Martinez-Garcia, Maria [1 ,2 ]
Zazo, Sandra [6 ]
Chamizo, Cristina [6 ]
Gonzalez-Alonso, Paula [6 ]
Madoz-Gurpide, Juan [6 ]
Eroles, Pilar [7 ]
Arribas, Joaquin [8 ,9 ,10 ]
Tusquets, Ignasi [1 ,2 ]
Lluch, Ana [11 ]
Pandiella, Atanasio [3 ]
Rojo, Federico [6 ]
Rovira, Ana [1 ,2 ]
Albanell, Joan [1 ,2 ,12 ]
机构
[1] IMIM Hosp Mar Res Inst, Canc Res Program, Barcelona, Spain
[2] Hosp Mar, Med Oncol Dept, CIBERONC, Barcelona, Spain
[3] Univ Salamanca, Ctr Invest Canc, CSIC, CIBERONC, Salamanca, Spain
[4] Hosp Mar, Pathol Dept, Barcelona, Spain
[5] IMIM Hosp Mar Res Inst, Immun & Infect Lab, Barcelona, Spain
[6] IIS, Pathol Dept, Fdn Jimenez Diaz, CIBERONC, Madrid, Spain
[7] INCLIVA Biomed Res Inst, Valencia, Spain
[8] VHIO, Preclin Res Program, CIBERONC, Barcelona, Spain
[9] Autonomous Univ Barcelona, Barcelona, Spain
[10] ICREA, Barcelona, Spain
[11] Hosp Clin Univ, Oncol & Hematol Dept, CIBERONC, Valencia, Spain
[12] Univ Pompeu Fabra, Barcelona, Spain
来源
CLINICAL CANCER RESEARCH | 2017年 / 23卷 / 22期
关键词
ANTIBODY-DRUG CONJUGATE; CELL-CYCLE; PHASE-III; TUMOR BIOMARKERS; EFFICACY; MECHANISMS; CHEMOTHERAPY; EXPRESSION; APOPTOSIS; PREDICT;
D O I
10.1158/1078-0432.CCR-17-0696
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Purpose: Trastuzumab-emtansine (T-DM1) is a standard treatment in advanced HER2-positive breast cancer. However, resistance inevitably occurs. We aimed to identify mechanisms of acquired T-DM1 resistance. Experimental Design: HER2-positive breast cancer cells (HCC1954, HCC1419, SKBR3, and BT474) were treated in a pulse-fashion with T-DM1 to induce a resistant phenotype. Cellular and molecular effects of T-DM1 in parental versus resistant cells were compared. CDK1 kinase activity and cyclin B1 expression were assayed under various conditions. Genetic modifications to up-or downregulate cyclin B1 were conducted. Effects of T-DM1 on cyclin B1 levels, proliferation, and apoptosis were assayed in human HER2-positive breast cancer explants. Results: We obtained three cell lines with different levels of acquired T-DM1 resistance (HCC1954/TDR, HCC1419/TDR, and SKBR3/TDR cells). HER2 remained amplified in the resistant cells. Binding to HER2 and intracellular uptake of T-DM1 were maintained in resistant cells. T-DM1 induced cyclin B1 accumulation in sensitive but not resistant cells. Cyclin B1 knockdown by siRNA in parental cells induced T-DM1 resistance, while increased levels of cyclin B1 by silencing cdc20 partially sensitized resistant cells. In a series of 18 HER2-positive breast cancer fresh explants, T-DM1 effects on proliferation and apoptosis paralleled cyclin B1 accumulation. Conclusions: Defective cyclin B1 induction by T-DM1 mediates acquired resistance in HER2-positive breast cancer cells. These results support the testing of cyclin B1 induction upon T-DM1 treatment as a pharmacodynamic predictor in HER2-positive breast cancer. (C) 2017 AACR.
引用
收藏
页码:7006 / 7019
页数:14
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