αποθετήριο
Ασκληπιός
Ασκληπιός- Ιδρυματικό Αποθετήριο Επιστημών Υγείας Ασκληπιείου Βούλας
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http://hdl.handle.net/11642/86| Τίτλος: | New miRNA profiles accurately distinguish renal cell carcinomas and upper tract urothelial carcinomas from the normal kidney. |
| Δημιουργός: | Zaravinos, Apostolos Lambrou, G. I. Mourmouras, Nikos Katafygiotis, Patroklos Papagregoriou, Gregory Giannikou, Krinio Delakas, Dimitris Deltas, Constantinos |
| Χρονολογία: | 2014 |
| Γλώσσα: | Αγγλικά |
| Εξειδίκευση τύπου : | Άρθρο |
| Περιγραφή: | PLoS One. 2014 Mar 12;9(3):e91646. doi: 10.1371/journal.pone.0091646. eCollection 2014. |
| Περίληψη: | Background: Upper tract urothelial carcinomas (UT-UC) can invade the pelvicalyceal system making differential diagnosis of the various histologically distinct renal cell carcinoma (RCC) subtypes and UT-UC, difficult. Correct diagnosis is critical for determining appropriate surgery and post-surgical treatments. We aimed to identify microRNA (miRNA) signatures that can accurately distinguish the most prevalent RCC subtypes and UT-UC form the normal kidney. Methods and Findings: miRNA profiling was performed on FFPE tissue sections from RCC and UT-UC and normal kidney and 434 miRNAs were significantly deregulated in cancerous vs. the normal tissue. Hierarchical clustering distinguished UTUCs from RCCs and classified the various RCC subtypes among them. qRT-PCR validated the deregulated expression profile for the majority of the miRNAs and ROC analysis revealed their capability to discriminate between tumour and normal kidney. An independent cohort of freshly frozen RCC and UT-UC samples was used to validate the deregulated miRNAs with the best discriminatory ability (AUC.0.8, p,0.001). Many of them were located within cytogenetic regions that were previously reported to be significantly aberrated. miRNA targets were predicted using the miRWalk algorithm and ingenuity pathway analysis identified the canonical pathways and curated networks of the deregulated miRNAs. Using the miRWalk algorithm, we further identified the top anti-correlated mRNA/miRNA pairs, between the deregulated miRNAs from our study and the top co-deregulated mRNAs among 5 independent ccRCC GEO datasets. The AB8/13 undifferentiated podocyte cells were used for functional assays using luciferase reporter constructs and the developmental transcription factor TFCP2L1 was proved to be a true target of miR-489, which was the second most upregulated miRNA in ccRCC. Conclusions: We identified novel miRNAs specific for each RCC subtype and UT-UC, we investigated their putative targets, the networks and pathways in which they participate and we functionally verified the true targets of the top deregulated miRNAs. |
| Θέμα: | Carcinoma, Renal Cell Καρκίνωμα Νεφρικών Κυττάρων RNA RNA Biomarkers, Tumor |
| Εναλλακτικός δικτυακός τόπος: | http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3951427/ |
| Άδεια Χρήσης: | Αναφορά Παρόμοια Διανομή  |
| Διάθεση ψηφιακού τεκμηρίου: | Πλήρης |
| Εμφανίζεται στις Ομάδες Τεκμηρίων: | Ουρολογία |
Ψηφιακά Αρχεία
| Αρχείο | Μέγεθος | Μορφότυπος | |
|---|---|---|---|
| Delakas2.pdf | 5.44 MB | Adobe PDF | Δείτε/Ανοίξτε |