MicroRNA let-7g acts as tumor suppressor and predictive biomarker for chemoresistance in human epithelial ovarian cancer

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作者
Flavia Biamonte
Gianluca Santamaria
Alessandro Sacco
Francesca Marta Perrone
Annalisa Di Cello
Anna Martina Battaglia
Alessandro Salatino
Anna Di Vito
Ilenia Aversa
Roberta Venturella
Fulvio Zullo
Francesco Costanzo
机构
[1] “Magna Græcia” University of Catanzaro,Research Center of Biochemistry and Advanced Molecular Biology, Department of Experimental and Clinical Medicine
[2] Campus Salvatore Venuta -Viale Europa,Department of Experimental and Clinical Medicine
[3] University Magna Graecia of Catanzaro,Department of Neuroscience, Reproductive Sciences and Dentistry, School of Medicine
[4] Campus Salvatore Venuta -Viale Europa,Interdepartmental Center of Services (CIS)
[5] Klinikum rechts der Isar,undefined
[6] Department of Regenerative Medicine in Cardiovascular Disease,undefined
[7] Ismaningerstr 22,undefined
[8] Unit of Obstetrics and Gynaecology,undefined
[9] “Magna Graecia” University of Catanzaro,undefined
[10] University of Naples “Federico II”,undefined
[11] University Magna Graecia of Catanzaro,undefined
[12] Campus Salvatore Venuta -Viale Europa,undefined
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Scientific Reports | / 9卷
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摘要
Remarkable deregulation of microRNAs has been demonstrated in epithelial ovarian cancer (EOC). In particular, some of the let-7 miRNA family members have been proposed as tumor suppressors. Here, we explored the functional roles of let-7g in EOC. The ectopic overexpression of let-7g in OVCAR3 and HEY-A8 EOC cells induced i) a down-regulation of c-Myc and cyclin-D2 thus promoting cell cycle arrest, ii) a reduction of Vimentin, Snail and Slug thus counteracting the progression of epithelial to mesenchymal transition, iii) a chemosensitization to cis-platinum treatment. Next, analysis of human EOC tissues revealed that let-7g expression was significantly reduced in tumor tissue specimens of patients with EOC compared to their non-tumor counterparts (p = 0.0002). Notably, low let-7g tissue levels were significantly associated with acquired chemoresistance of patients with late-stage of EOC (n = 17, p = 0.03194). This finding was further validated in the serum samples collected from the same cohort of patients (n = 17, p = 0.003). To conclude, we demonstrate that let-7g acts as tumor suppressor and might be used to disable EOC tumor progression and chemoresistance to cis-platinum-based chemotherapy. Furthermore, we propose that decreased expression of let-7g could serve as a tissue and serum biomarker able to predict the chemo-resistant features of EOC patients.
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