Up regulation in gene expression of chromatin remodelling factors in cervical intraepithelial neoplasia.

Up regulation in gene expression of chromatin remodelling factors in cervical intraepithelial neoplasia. Research Abstract Details 

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Up regulation in gene expression of chromatin remodelling factors in cervical intraepithelial neoplasia. Abstract Text:

Ashleen Shadeo,Raj Chari,Kim M Lonergan,Andrea Pusic,Dianne Miller,Tom Ehlen,Dirk Van Niekerk,Jasenka Matisic,Rebecca Richards-Kortum,Michele Follen,Martial Guillaud,Wan L Lam,Calum Macaulay,Ashleen Shadeo,Raj Chari,Kim M Lonergan,Andrea Pusic,Dianne Miller,Tom Ehlen,Dirk Van Niekerk,Jasenka Matisic,Rebecca Richards-Kortum,Michele Follen,Martial Guillaud,Wan L Lam,Calum MacAulay,

ABSTRACT: BACKGROUND: The highest rates of cervical cancer are found in developing countries. Frontline monitoring has reduced these rates in developed countries and present day screening programs primarily identify precancerous lesions termed cervical intraepithelial neoplasias (CIN). CIN lesions described as mild dysplasia (CIN I) are likely to spontaneously regress while CIN III lesions (severe dysplasia) are likely to progress if untreated. Thoughtful consideration of gene expression changes paralleling the progressive pre invasive neoplastic development will yield insight into the key casual events involved in cervical cancer development. RESULTS: In this study, we have identified gene expression changes across 16 cervical cases (CIN I, CIN II, CIN III and normal cervical epithelium) using the unbiased long serial analysis of gene expression (L-SAGE) method. The 16 L-SAGE libraries were sequenced to the level of 2,481,387 tags, creating the largest SAGE data collection for cervical tissue worldwide. We have identified 222 genes differentially expressed between normal cervical tissue and CIN III. Many of these genes influence biological functions characteristic of cancer, such as cell death, cell growth/proliferation and cellular movement. Evaluation of these genes through network interactions identified multiple candidates that influence regulation of cellular transcription through chromatin remodelling (SMARCC1, NCOR1, MRFAP1 and MORF4L2). Further, these expression events are focused at the critical junction in disease development of moderate dysplasia (CIN II) indicating a role for chromatin remodelling as part of cervical cancer development. CONCLUSION: We have created a valuable publically available resource for the study of gene expression in precancerous cervical lesions. Our results indicate deregulation of the chromatin remodelling complex components and its influencing factors occur in the development of CIN lesions. The increase in SWI/SNF stabilizing molecule SMARCC1 and other novel genes has not been previously illustrated as events in the early stages of dysplasia development and thus not only provides novel candidate markers for screening but a biological function for targeting treatment.

Up regulation in gene expression of chromatin remodelling factors in cervical intraepithelial neoplasia. Publishing Authors By Initials

A Shadeo,R Chari,KM Lonergan,A Pusic,D Miller,T Ehlen,D Van Niekerk,J Matisic,R Richards-Kortum,M Follen,M Guillaud,WL Lam,C Macaulay,A Shadeo,R Chari,KM Lonergan,A Pusic,D Miller,T Ehlen,D Van Niekerk,J Matisic,R Richards-Kortum,M Follen,M Guillaud,WL Lam,C MacAulay,

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Up regulation in gene expression of chromatin remodelling factors in cervical intraepithelial neoplasia. Journal Published:

PUBLICATION TYPE: Journal Article

Journal: BMC genomics

VOLUME: 9

Page Numbers: 64

Journal Abbreviation: BMC Genomics

ISSN: 1471-2164

DAY: 4

MONTH: 02

YEAR: 2008

Up regulation in gene expression of chromatin remodelling factors in cervical intraepithelial neoplasia. Information

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LANGUAGE: eng

NlmUniqueID: 100965258

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AFFILIATION: Cancer Genetics & Developmental Biology, British Columbia Cancer Research Centre, Vancouver, BC, Canada. ashadeo@bccrc.ca.

Country: England

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MEDLINETA: BMC Genomics

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