Litcius/Paper detail

Exosome‐mediated transfer of long noncoding RNA H19 induces doxorubicin resistance in breast cancer

Xinxing Wang, Xinhong Pei, Guangcheng Guo, Xueke Qian, Dongwei Dou, Zhe Zhang, Xiaodong Xu, Xin Duan

2020Journal of Cellular Physiology114 citationsDOI

Abstract

Development of the acquired resistance is one major obstacle during chemotherapy for cancer patients. Exosomes mediate intercellular communication and cause environmental changes in tumor progression by transmitting active molecules. In this study, the role of long noncoding RNA H19 within exosomes is elucidated in terms of regulating doxorubicin (DOX) resistance of breast cancer. As a result, increased H19 expression was observed in DOX-resistant breast cancer cells in comparison with the corresponding parental cells. Suppression of H19 significantly lowered DOX resistance by decreasing cell viability, lowering colony-forming ability, and inducing apoptosis. Moreover, extracellular H19 could be moved to sensitive cells via being incorporated into exosomes. Treating sensitive cells with exosomes from resistant cells increased the chemoresistance of DOX, while downregulation of H19 in sensitive cells abated this effect. Taken together, H19 could be delivered by exosomes to sensitive cells, leading to the dissemination of DOX resistance. Our finding highlights the potential of exosomal H19 as a molecular target to reduce DOX resistance.

Topics & Concepts

MicrovesiclesDoxorubicinDownregulation and upregulationExosomeCancer researchApoptosisIntracellularBiologyBreast cancerCancer cellCancerLong non-coding RNARNACell biologyChemotherapymicroRNAGeneBiochemistryGeneticsCancer-related molecular mechanisms researchExtracellular vesicles in diseaseCircular RNAs in diseases