Abstract

Drug resistance is a major challenge in breast cancer (BC) treatment at present. Accumulating studies indicate that breast cancer stem cells (BCSCs) are responsible for the BC drugs resistance, causing relapse and metastasis in BC patients. Thus, BCSCs elimination could reverse drug resistance and improve drug efficacy to benefit BC patients. Consequently, mastering the knowledge on the proliferation, resistance mechanisms, and separation of BCSCs in BC therapy is extremely helpful for BCSCs-targeted therapeutic strategies. Herein, we summarize the principal BCSCs surface markers and signaling pathways, and list the BCSCs-related drug resistance mechanisms in chemotherapy (CT), endocrine therapy (ET), and targeted therapy (TT), and display therapeutic strategies for targeting BCSCs to reverse drug resistance in BC. Even more importantly, more attention should be paid to studies on BCSC-targeted strategies to overcome the drug resistant dilemma of clinical therapies in the future.

Highlights

  • Breast cancer (BC) is one of the most common cancers diagnosed among women and ranked as the second cause of cancer-related death among women, after lung cancer (DeSantis et al, 2019; Siegel et al, 2019)

  • For improvement of chemotherapeutic effects in metastatic cancer (Lv et al, 2018b). These results demonstrate the important role of CD44 in BC stemness, invasion, metastasis, and drug resistance

  • CXC chemokine receptor 4 (CXCR4)+ breast cancer stem cells (BCSCs) displayed decreased vimentin and increased E-cadherin, indicating the occurrence of epithelialmesenchymal transitions (EMT). These findings demonstrate that CXCR4+ BCSC triggered EMT-related metastasis

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Summary

Introduction

Breast cancer (BC) is one of the most common cancers diagnosed among women and ranked as the second cause of cancer-related death among women, after lung cancer (DeSantis et al, 2019; Siegel et al, 2019).

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