Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNAS

Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNAS

Oral Squamous Cell Carcinoma (OSCC) is the sixth most frequent malignant tumour. There is some evidence that tongue cancer has a higher local failure rate and poorer prognosis than other anatomical sites in the oral cavity. We used tongue squamous cell carcinoma cell lines harbouring mutated p53/p16...

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Main Authors: A. Guida, G. Pannone, A. Lucchese, R. Serpico, D. Pasquali, A. Santoro, G. Russo, L. Lo Muzio, P. Bufo, C. Sbordone, G. Donnarumma, S. Papagerakis
Format: Article
Language:English
Published: SAGE Publishing 2012-09-01
Series:European Journal of Inflammation
Online Access:https://doi.org/10.1177/1721727X1201000320
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spelling doaj-73ba6d992ca14f4785c5e774f2d782532020-11-25T04:02:41ZengSAGE PublishingEuropean Journal of Inflammation1721-727X2012-09-011010.1177/1721727X1201000320Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNASA. Guida0G. Pannone1A. Lucchese2R. Serpico3D. Pasquali4A. Santoro5G. Russo6L. Lo Muzio7P. Bufo8C. Sbordone9G. Donnarumma10S. Papagerakis11 Department of Odontostomatological, Orthodontics and Surgical Disciplines, Second University of Naples SUN, Naples, Italy Department of Clinical and Experimental Medicine, Section of Anatomic Pathology, University of Foggia, Foggia, Italy Department of Odontostomatological, Orthodontics and Surgical Disciplines, Second University of Naples SUN, Naples, Italy Department of Odontostomatological, Orthodontics and Surgical Disciplines, Second University of Naples SUN, Naples, Italy Department of Clinical and Experimental Medicine and Surgery, Endocrine Unit, Second University of Naples SUN, Naples, Italy Department of Clinical and Experimental Medicine, Section of Anatomic Pathology, University of Foggia, Foggia, Italy Department of Clinical and Experimental Medicine, University of Foggia, Foggia, Italy Department of Clinical and Experimental Medicine, Section of Oral Pathology, University of Foggia, Foggia, Italy Department of Clinical and Experimental Medicine, Section of Anatomic Pathology, University of Foggia, Foggia, Italy Chair of Maxillo-Facial Surgery, School of Medicine, University of Naples Federico II, Naples, Italy Second University of Naples, Department of Experimental Medicine, Microbiology and Clinical Microbiology, Naples, Italy Department of Otolaryngology, Head and Neck Surgery Laboratory of Oral, Head and Neck Cancer Invasion and Metastasis, Medical School, University of Michigan Ann Arbor, Ann Arbor, MI, USAOral Squamous Cell Carcinoma (OSCC) is the sixth most frequent malignant tumour. There is some evidence that tongue cancer has a higher local failure rate and poorer prognosis than other anatomical sites in the oral cavity. We used tongue squamous cell carcinoma cell lines harbouring mutated p53/p16 as tongue cancer models to study the influences exerted by p53 and p16 genes on the expression of micro RNAs (miRNAs). The study was performed on microarray chips harbouring 298 miRNA sequences. OSCC cell lines used in this study were SCC-4, SCC-15 and SCC-25, all three carrying mutated/hypermethylated p53/p16. The expression values normalized to healthy control of 298 miRNAs were obtained for each cell line. MiRNA 196b was found hyperexpressed in the three cell lines. MiRNAs 19b-1, 21, 27a, 30d, 134, 339, 379 and 465 were found altered in two out of three cell lines. miRNAs found altered in one cell line out of three were: 7b, 23a, 25, 30c, 30e-3p, 107,125b, 124a, 214, 216, 325 and 384. A literature review for each miRNA found significant was undertaken. Some miRNAs have a well-known role in oral cancer, some have been put in correlation with other cancers/diseases, others are found significant for the first time. These early results in tongue cancer cell lines harbouring mutation of p16/p53 need further analyses to understand whether this variation of miRNA levels are directly influenced by the malfunction of these proteins or if, vice-versa, altered miRNA levels influence the function of p16 and p53.https://doi.org/10.1177/1721727X1201000320
collection DOAJ
language English
format Article
sources DOAJ
author A. Guida
G. Pannone
A. Lucchese
R. Serpico
D. Pasquali
A. Santoro
G. Russo
L. Lo Muzio
P. Bufo
C. Sbordone
G. Donnarumma
S. Papagerakis
spellingShingle A. Guida
G. Pannone
A. Lucchese
R. Serpico
D. Pasquali
A. Santoro
G. Russo
L. Lo Muzio
P. Bufo
C. Sbordone
G. Donnarumma
S. Papagerakis
Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNAS
European Journal of Inflammation
author_facet A. Guida
G. Pannone
A. Lucchese
R. Serpico
D. Pasquali
A. Santoro
G. Russo
L. Lo Muzio
P. Bufo
C. Sbordone
G. Donnarumma
S. Papagerakis
author_sort A. Guida
title Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNAS
title_short Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNAS
title_full Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNAS
title_fullStr Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNAS
title_full_unstemmed Tongue Cancer and Epigenetic Factors: An Study on 298 Micro-RNAS
title_sort tongue cancer and epigenetic factors: an study on 298 micro-rnas
publisher SAGE Publishing
series European Journal of Inflammation
issn 1721-727X
publishDate 2012-09-01
description Oral Squamous Cell Carcinoma (OSCC) is the sixth most frequent malignant tumour. There is some evidence that tongue cancer has a higher local failure rate and poorer prognosis than other anatomical sites in the oral cavity. We used tongue squamous cell carcinoma cell lines harbouring mutated p53/p16 as tongue cancer models to study the influences exerted by p53 and p16 genes on the expression of micro RNAs (miRNAs). The study was performed on microarray chips harbouring 298 miRNA sequences. OSCC cell lines used in this study were SCC-4, SCC-15 and SCC-25, all three carrying mutated/hypermethylated p53/p16. The expression values normalized to healthy control of 298 miRNAs were obtained for each cell line. MiRNA 196b was found hyperexpressed in the three cell lines. MiRNAs 19b-1, 21, 27a, 30d, 134, 339, 379 and 465 were found altered in two out of three cell lines. miRNAs found altered in one cell line out of three were: 7b, 23a, 25, 30c, 30e-3p, 107,125b, 124a, 214, 216, 325 and 384. A literature review for each miRNA found significant was undertaken. Some miRNAs have a well-known role in oral cancer, some have been put in correlation with other cancers/diseases, others are found significant for the first time. These early results in tongue cancer cell lines harbouring mutation of p16/p53 need further analyses to understand whether this variation of miRNA levels are directly influenced by the malfunction of these proteins or if, vice-versa, altered miRNA levels influence the function of p16 and p53.
url https://doi.org/10.1177/1721727X1201000320
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