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c-myc regulates the sensitivity of breast cancer cells to palbociclib via c-myc/miR-29b-3p/CDK6 axis

Wenfei Ji, Wenwen Zhang, Xin Wang, Yaqin Shi, Fang Yang, Hui Xie, Wenbin Zhou, Shui Wang, Xiaoxiang Guan

2020Cell Death and Disease92 citationsDOIOpen Access PDF

Abstract

Abstract Palbociclib, a CDK4/6 inhibitor, has been granted accelerated approval by US FDA for hormone receptor-positive HER2-negative metastatic breast cancer. To determine potential biomarkers of palbociclib sensitivity to assist in patient selection and clinical development, we investigated the effects of palbociclib in a panel of molecularly characterized breast cancer cell lines. We quantified palbociclib sensitivity and c-myc expression in 11 breast cancer cell lines, 124 breast cancer samples, and The Cancer Genome Atlas database. We found non-TNBC subtypes were more sensitive to palbociclib than TNBC. Activation of c-myc led to differential palbociclib sensitivities, and further inhibition of c-myc enhanced palbociclib sensitivity. Moreover, we identified for the first time a c-myc/miR-29b-3p/CDK6 axis in breast cancer that could be responsible for c-myc-induced palbociclib insensitivity, in which c-myc activation resulted in downregulation of miR-29b-3p, further activated CDK6 and inhibited cell-cycle arrest at G 1 phase. Moreover, downregulated (inactived) c-myc-induced oncogenic addiction could increase palbociclib efficacy, using both Xenograft model and patient-derived tumor xenograft (PDTX) model. Our finding extends the concept of combined blockade of the CDK4/6 and c-myc signaling pathways to increase palbociclib sensitivity, making c-myc a promising biomarker for palbociclib sensitivity in breast cancer.

Topics & Concepts

PalbociclibCyclin-dependent kinase 6Breast cancerCancer researchMedicineCancerCyclin-dependent kinase 4Cell cycleOncologyInternal medicineMetastatic breast cancerCyclin-dependent kinase 2Advanced Breast Cancer TherapiesCancer-related Molecular PathwaysCancer Mechanisms and Therapy