Prognostic value of 5-microRNA based signature in T2-T3N0 colon cancer

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作者
Maciej Bobowicz
Marcin Skrzypski
Piotr Czapiewski
Michał Marczyk
Agnieszka Maciejewska
Michał Jankowski
Anna Szulgo-Paczkowska
Wojciech Zegarski
Ryszard Pawłowski
Joanna Polańska
Wojciech Biernat
Janusz Jaśkiewicz
Jacek Jassem
机构
[1] Medical University of Gdansk,Department of Surgical Oncology
[2] Medical University of Gdansk,Department of Oncology and Radiotherapy
[3] Medical University of Gdansk,Department of Pathomorfology
[4] Silesian University of Technology,Institute of Automatic Control, Data Mining Group
[5] Medical University of Gdansk,Institute of Forensic Medicine
[6] Nicolaus Copernicus University,Department and Clinic of Oncologic Surgery, Collegium Medicum
[7] Centre of Oncology,Department of Clinical Oncology
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microRNA expression; colon cancer; metastasis; prognostic marker; miR-1300; miR-939;
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摘要
The role of adjuvant chemotherapy in stage T2-T3N0 colon cancer (CC) is controversial and there are currently no reliable factors allowing for individual selection of patients with high risk of relapse for such therapy. We searched for microRNA-based signature with prognostic significance in this group. We assessed by qRT-PCR expression of 754 microRNAs (miRNAs) in tumour samples from 85 stage pT2-3N0 CC patients treated with surgery alone. MiRNA expression was compared between two groups of patients: 40 and 45 patients who did and did not develop distant metastases after resection, respectively. Additionally, miRNA expression was compared between CC and normal colon mucosa samples and between the mismatch repair (MMR) competent and deficient tumours. Low expression of miR-1300 and miR-939 was significantly correlated with shorter distant metastasis-free survival (DMFS) in Cox univariate analysis (p.adjusted = 0.049). The expression signature of five miRNAs (miR-1296, miR-135b, miR-539, miR-572 and miR-185) was found to be prognostic [p = 1.28E−07, HR 8.4 (95 % CI: 3.81–18.52)] for DMFS and cross-validated in a leave-one-out analysis, with the sensitivity and specificity of 74 and 78 %, respectively. The expression of miR-592 was significantly associated with the MMR status (p.adjusted <0.01). The expression of several novel miRNAs were found to be tumour specific, e.g. miR-888, miR-523, miR-18b, miR-302a, miR-423-5p, miR-582-3p (p < 0.05). We developed a miRNA expression signature that may be predictive for the risk of distant relapse in early stage CC and confirmed previously reported association between miR-592 expression and MMR status.
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页码:765 / 773
页数:8
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