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dc.creatorPipinikas, C. P.en
dc.creatorKiropoulos, T. S.en
dc.creatorTeixeira, V. H.en
dc.creatorBrown, J. M.en
dc.creatorVaranou, A.en
dc.creatorFalzon, M.en
dc.creatorCapitanio, A.en
dc.creatorBottoms, S. E.en
dc.creatorCarrol, B.en
dc.creatorNavani, N.en
dc.creatorMcCaughan, F.en
dc.creatorGeorge, J. P.en
dc.creatorGiangreco, A.en
dc.creatorWright, N. A.en
dc.creatorMcDonald, S. A. C.en
dc.creatorGraham, T. A.en
dc.creatorJanes, S. M.en
dc.date.accessioned2015-11-23T10:45:40Z
dc.date.available2015-11-23T10:45:40Z
dc.date.issued2014
dc.identifier10.1136/thoraxjnl-2013-204198
dc.identifier.issn406376
dc.identifier.urihttp://hdl.handle.net/11615/32286
dc.description.abstractBackground Squamous cell carcinoma of the lung is a common cancer with 95% mortality at 5 years. These cancers arise from preinvasive lesions, which have a natural history of development progressing through increasing severity of dysplasia to carcinoma in situ (CIS), and in some cases, ending in transformation to invasive carcinoma. Synchronous preinvasive lesions identified at autopsy have been previously shown to be clonally related. Methods Using autofluorescence bronchoscopy that allows visual observation of preinvasive lesions within the upper airways, together with molecular profiling of biopsies using gene sequencing and loss-of-heterozygosity analysis from both preinvasive lesions and from intervening normal tissue, we have monitored individual lesions longitudinally and documented their visual, histological and molecular relationship. Results We demonstrate that rather than forming a contiguous field of abnormal tissue, clonal CIS lesions can develop at multiple anatomically discrete sites over time. Further, we demonstrate that patients with CIS in the trachea have invariably had previous lesions that have migrated proximally, and in one case, into the other lung over a period of 12 years. Conclusions Molecular information from these unique biopsies provides for the first time evidence that field cancerisation of the upper airways can occur through cell migration rather than via local contiguous cellular expansion as previously thought. Our findings urge a clinical strategy of ablating high-grade premalignant airway lesions with subsequent attentive surveillance for recurrence in the bronchial tree.en
dc.source.urihttp://www.scopus.com/inward/record.url?eid=2-s2.0-84901245830&partnerID=40&md5=5ec1be655f45917fda924d10214f13e0
dc.subjectadulten
dc.subjectageden
dc.subjectarticleen
dc.subjectautofluorescenceen
dc.subjectbronchoscopyen
dc.subjectcancer stagingen
dc.subjectcarcinoma in situen
dc.subjectcell expansionen
dc.subjectcell migrationen
dc.subjectclinical articleen
dc.subjectclonal variationen
dc.subjectcontrolled studyen
dc.subjectepithelium cellen
dc.subjectgene deletionen
dc.subjectgene sequenceen
dc.subjectheterozygosity lossen
dc.subjecthistopathologyen
dc.subjecthumanen
dc.subjecthuman tissueen
dc.subjectlung biopsyen
dc.subjectmaleen
dc.subjectmiddle ageden
dc.subjectmolecular modelen
dc.subjectmutational analysisen
dc.subjectpriority journalen
dc.subjecttrachea carcinomaen
dc.subjecttracheobronchial treeen
dc.subjecttumor suppressor geneen
dc.subjectAirway Epitheliumen
dc.subjectLung Canceren
dc.subjectCarcinoma, Squamous Cellen
dc.subjectCell Movementen
dc.subjectGenes, p53en
dc.subjectHumansen
dc.subjectLoss of Heterozygosityen
dc.subjectLung Neoplasmsen
dc.subjectMutationen
dc.subjectNeoplasm Invasivenessen
dc.subjectPrecancerous Conditionsen
dc.subjectTracheal Neoplasmsen
dc.titleCell migration leads to spatially distinct but clonally related airway cancer precursorsen
dc.typejournalArticleen


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