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Progressive 3q amplification consistently targets SOX2 in preinvasive squamous lung cancer.

Authors :
McCaughan F
Pole JC
Bankier AT
Konfortov BA
Carroll B
Falzon M
Rabbitts TH
George PJ
Dear PH
Rabbitts PH
McCaughan, Frank
Pole, Jessica C M
Bankier, Alan T
Konfortov, Bernard A
Carroll, Bernadette
Falzon, Mary
Rabbitts, Terence H
George, P Jeremy
Dear, Paul H
Rabbitts, Pamela H
Source :
American Journal of Respiratory & Critical Care Medicine; 7/1/2010, Vol. 182 Issue 1, p83-91, 9p
Publication Year :
2010

Abstract

<bold>Rationale: </bold>Amplification of distal 3q is the most common genomic aberration in squamous lung cancer (SQC). SQC develops in a multistage progression from normal bronchial epithelium through dysplasia to invasive disease. Identifying the key driver events in the early pathogenesis of SQC will facilitate the search for predictive molecular biomarkers and the identification of novel molecular targets for chemoprevention and therapeutic strategies. For technical reasons, previous attempts to analyze 3q amplification in preinvasive lesions have focused on small numbers of predetermined candidate loci rather than an unbiased survey of copy-number variation.<bold>Objectives: </bold>To perform a detailed analysis of the 3q amplicon in bronchial dysplasia of different histological grades.<bold>Methods: </bold>We use molecular copy-number counting (MCC) to analyze the structure of chromosome 3 in 19 preinvasive bronchial biopsy specimens from 15 patients and sequential biopsy specimens from 3 individuals.<bold>Measurements and Main Results: </bold>We demonstrate that no low-grade lesions, but all high-grade lesions, have 3q amplification. None of seven low-grade lesions progressed clinically, whereas 8 of 10 patients with high-grade disease progressed to cancer. We identify a minimum commonly amplified region on chromosome 3 consisting of 17 genes, including 2 known oncogenes, SOX2 and PIK3CA. We confirm that both genes are amplified in all high-grade dysplastic lesions tested. We further demonstrate, in three individuals, that the clinical progression of high-grade preinvasive disease is associated with incremental amplification of SOX2, suggesting this promotes malignant progression.<bold>Conclusions: </bold>These findings demonstrate progressive 3q amplification in the evolution of preinvasive SQC and implicate SOX2 as a key target of this dynamic process. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
1073449X
Volume :
182
Issue :
1
Database :
Complementary Index
Journal :
American Journal of Respiratory & Critical Care Medicine
Publication Type :
Academic Journal
Accession number :
105044383
Full Text :
https://doi.org/10.1164/rccm.201001-0005OC