Litcius/Paper detail

miR‐221 confers lapatinib resistance by negatively regulating p27<sup>kip1</sup> in HER2‐positive breast cancer

Thanh Kieu Huynh, Chih‐Hao Huang, Jhen‐Yu Chen, J. Yao, Yi‐Shiang Yang, Ya‐Ling Wei, Hsiao‐Fan Chen, Chia‐Hung Chen, Chih‐Yen Tu, Yuan‐Man Hsu, Liang‐Chih Liu, Wei‐Chien Huang

2021Cancer Science19 citationsDOIOpen Access PDF

Abstract

Abstract Development of acquired resistance to lapatinib, a dual epidermal growth factor receptor (EGFR)/human epidermal growth factor receptor 2 (HER2) tyrosine kinase inhibitor, severely limits the duration of clinical response in advanced HER2‐driven breast cancer patients. Although the compensatory activation of the PI3K/Akt survival signal has been proposed to cause acquired lapatinib resistance, comprehensive molecular mechanisms remain required to develop more efficient strategies to circumvent this therapeutic difficulty. In this study, we found that suppression of HER2 by lapatinib still led to Akt inactivation and elevation of FOX3a protein levels, but failed to induce the expression of their downstream pro‐apoptotic effector p27 kip1 , a cyclin‐dependent kinase inhibitor. Elevation of miR‐221 was found to contribute to the development of acquired lapatinib resistance by targeting p27 kip1 expression. Furthermore, upregulation of miR‐221 was mediated by the lapatinib‐induced Src family tyrosine kinase and subsequent NF‐κB activation. The reversal of miR‐221 upregulation and p27 kip1 downregulation by a Src inhibitor, dasatinib, can overcome lapatinib resistance. Our study not only identified miRNA‐221 as a pivotal factor conferring the acquired resistance of HER2‐positive breast cancer cells to lapatinib through negatively regulating p27 kip1 expression, but also suggested Src inhibition as a potential strategy to overcome lapatinib resistance.

Topics & Concepts

LapatinibTyrosine-kinase inhibitorDownregulation and upregulationCancer researchEpidermal growth factor receptorTyrosine kinaseDasatinibProto-oncogene tyrosine-protein kinase SrcBreast cancerProtein kinase BCancerMedicineInternal medicineTrastuzumabBiologySignal transductionReceptorCell biologyBiochemistryGeneCancer-related Molecular PathwaysCancer Mechanisms and TherapyCell death mechanisms and regulation