Down regulation of Cathepsin W is associated with poor prognosis in pancreatic cancer

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作者
Fatemeh Khojasteh-Leylakoohi
Reza Mohit
Nima Khalili-Tanha
Alireza Asadnia
Hamid Naderi
Ghazaleh Pourali
Zahra Yousefli
Ghazaleh Khalili-Tanha
Majid Khazaei
Mina Maftooh
Mohammadreza Nassiri
Seyed Mahdi Hassanian
Majid Ghayour-Mobarhan
Gordon A. Ferns
Soodabeh Shahidsales
Alfred King-yin Lam
Elisa Giovannetti
Elham Nazari
Jyotsna Batra
Amir Avan
机构
[1] Mashhad University of Medical Sciences,Metabolic Syndrome Research Center
[2] Mashhad University of Medical Sciences,Basic Sciences Research Institute
[3] Mashhad University of Medical Sciences,Medical Genetics Research Center
[4] Bushehr University of Medical Sciences,Department of Anesthesia
[5] Ferdowsi University of Mashhad,Recombinant Proteins Research Group, The Research Institute of Biotechnology
[6] Brighton and Sussex Medical School,Cancer Research Center
[7] Division of Medical Education,Pathology, School of Medicine and Dentistry
[8] Mashhad University of Medical Sciences,Department of Medical Oncology, Cancer Center Amsterdam
[9] Griffith University,Cancer Pharmacology Lab, AIRC Start up Unit
[10] Amsterdam U.M.C.,Department of Health Information, Technology and Management, School of Allied Medical Sciences
[11] VU. University Medical Center (VUMC),College of Medicine
[12] Fondazione Pisana Per La Scienza,Faculty of Health, School of Biomedical Sciences
[13] Shahid BeheshtiUniversity of Medical Science,Translational Research Institute
[14] University of Warith Al-Anbiyaa,undefined
[15] Queensland University of Technology (QUT),undefined
[16] Queensland University of Technology,undefined
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摘要
Pancreatic ductal adenocarcinoma (PDAC) is associated with a very poor prognosis. Therefore, there has been a focus on identifying new biomarkers for its early diagnosis and the prediction of patient survival. Genome-wide RNA and microRNA sequencing, bioinformatics and Machine Learning approaches to identify differentially expressed genes (DEGs), followed by validation in an additional cohort of PDAC patients has been undertaken. To identify DEGs, genome RNA sequencing and clinical data from pancreatic cancer patients were extracted from The Cancer Genome Atlas Database (TCGA). We used Kaplan–Meier analysis of survival curves was used to assess prognostic biomarkers. Ensemble learning, Random Forest (RF), Max Voting, Adaboost, Gradient boosting machines (GBM), and Extreme Gradient Boosting (XGB) techniques were used, and Gradient boosting machines (GBM) were selected with 100% accuracy for analysis. Moreover, protein–protein interaction (PPI), molecular pathways, concomitant expression of DEGs, and correlations between DEGs and clinical data were analyzed. We have evaluated candidate genes, miRNAs, and a combination of these obtained from machine learning algorithms and survival analysis. The results of Machine learning identified 23 genes with negative regulation, five genes with positive regulation, seven microRNAs with negative regulation, and 20 microRNAs with positive regulation in PDAC. Key genes BMF, FRMD4A, ADAP2, PPP1R17, and CACNG3 had the highest coefficient in the advanced stages of the disease. In addition, the survival analysis showed decreased expression of hsa.miR.642a, hsa.mir.363, CD22, BTNL9, and CTSW and overexpression of hsa.miR.153.1, hsa.miR.539, hsa.miR.412 reduced survival rate. CTSW was identified as a novel genetic marker and this was validated using RT-PCR. Machine learning algorithms may be used to Identify key dysregulated genes/miRNAs involved in the disease pathogenesis can be used to detect patients in earlier stages. Our data also demonstrated the prognostic and diagnostic value of CTSW in PDAC.
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