Subclonal diversity arises early even in small colorectal tumours and contributes to differential growth fates.

Abstract:

OBJECTIVE AND DESIGN:The goal of the study was to determine whether the mutational profile of early colorectal polyps correlated with growth behaviour. The growth of small polyps (6-9 mm) that were first identified during routine screening of patients was monitored over time by interval imaging with CT colonography. Mutations in these lesions with known growth rates were identified by targeted next-generation sequencing. The timing of mutational events was estimated using computer modelling and statistical inference considering several parameters including allele frequency and fitness. RESULTS:The mutational landscape of small polyps is varied both within individual polyps and among the group as a whole but no single alteration was correlated with growth behaviour. Polyps carried 0-3 pathogenic mutations with the most frequent being in APC, KRAS/NRAS, BRAF, FBXW7 and TP53. In polyps with two or more pathogenic mutations, allele frequencies were often variable, indicating the presence of multiple populations within a single tumour. Based on computer modelling, detectable mutations occurred at a mean polyp size of 30±35 crypts, well before the tumour is of a clinically detectable size. CONCLUSIONS:These data indicate that small colon polyps can have multiple pathogenic mutations in crucial driver genes that arise early in the existence of a tumour. Understanding the molecular pathway of tumourigenesis and clonal evolution in polyps that are at risk for progressing to invasive cancers will allow us to begin to better predict which polyps are more likely to progress into adenocarcinomas and which patients are at greater risk of developing advanced disease.

journal_name

Gut

journal_title

Gut

authors

Sievers CK,Zou LS,Pickhardt PJ,Matkowskyj KA,Albrecht DM,Clipson L,Bacher JW,Pooler BD,Moawad FJ,Cash BD,Reichelderfer M,Vo TN,Newton MA,Larget BR,Halberg RB

doi

10.1136/gutjnl-2016-312232

subject

Has Abstract

pub_date

2017-12-01 00:00:00

pages

2132-2140

issue

12

eissn

0017-5749

issn

1468-3288

pii

gutjnl-2016-312232

journal_volume

66

pub_type

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