circTADA2As suppress breast cancer progression and metastasis via targeting miR-203a-3p/SOCS3 axis

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作者
Jian-Zhen Xu
Chang-Chun Shao
Xiao-Jia Wang
Xing Zhao
Jun-Qing Chen
Yan-Xiu Ouyang
Jun Feng
Fan Zhang
Wen-He Huang
Qian Ying
Chun-Fa Chen
Xiao-Long Wei
Hong-Yan Dong
Guo-Jun Zhang
Min Chen
机构
[1] Shantou University Medical College (SUMC),Department of Bioinformatics
[2] Shantou University Medical College,ChangJiang Scholar’s Laboratory
[3] Zhejiang Cancer Hospital,Key Lab of Diagnosis & Treatment Technology on Thoracic Oncology
[4] Cancer Hospital of Shantou University Medical College,Guangdong Provincial Key Laboratory on Breast Cancer Diagnosis and Treatment
[5] Cancer Hospital of Shantou University Medical College,The Breast Center
[6] First Affiliated Hospital of Shantou University Medical College,Department of Thyroid and Breast Surgery
[7] Cancer Hospital of Shantou University Medical College,Department of Pathology
[8] Linyi People’s Hospital,Department of Pathology
[9] Xiang’an Hospital of Xiamen University,The Cancer Center
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摘要
More and more evidence indicates that circular RNAs (circRNAs) have important roles in several diseases, especially in cancers. However, their involvement remains to be investigated in breast cancer. Through screening circRNA profile, we identified 235 differentially expressed circRNAs in breast cancer. Subsequently, we explored the clinical significance of two circTADA2As in a large cohort of triple-negative breast cancer (TNBC), and performed functional analysis of circTADA2A-E6 in vitro and in vivo to support clinical findings. Finally, we evaluated the effect of circTADA2A-E6 on miR-203a-3p and its target gene SOCS3. We detected two circRNAs, circTADA2A-E6 and circTADA2A-E5/E6, which were among the top five differentially expressed circRNAs in breast cancer. They were consistently and significantly decreased in a large cohort of breast cancer patients, and their downregulation was associated with poor patient survival for TNBC. Especially, circTADA2A-E6 suppressed in vitro cell proliferation, migration, invasion, and clonogenicity and possessed tumor-suppressor capability. circTADA2A-E6 preferentially acted as a miR-203a-3p sponge to restore the expression of miRNA target gene SOCS3, resulting in a less aggressive oncogenic phenotype. circTADA2As as promising prognostic biomarkers in TNBC patients, and therapeutic targeting of circTADA2As/miRNA/mRNA network may be a potential strategy for the treatment of breast cancer.
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