Minimal barriers to invasion during human colorectal tumor growth

Author:

Ryser Marc D.,Mallo DiegoORCID,Hall Allison,Hardman Timothy,King Lorraine M.,Tatishchev Sergei,Sorribes Inmaculada C.,Maley Carlo C.ORCID,Marks Jeffrey R.,Hwang E. Shelley,Shibata Darryl

Abstract

AbstractIntra-tumoral heterogeneity (ITH) could represent clonal evolution where subclones with greater fitness confer more malignant phenotypes and invasion constitutes an evolutionary bottleneck. Alternatively, ITH could represent branching evolution with invasion of multiple subclones. The two models respectively predict a hierarchy of subclones arranged by phenotype, or multiple subclones with shared phenotypes. We delineate these modes of invasion by merging ancestral, topographic, and phenotypic information from 12 human colorectal tumors (11 carcinomas, 1 adenoma) obtained through saturation microdissection of 325 small tumor regions. The majority of subclones (29/46, 60%) share superficial and invasive phenotypes. Of 11 carcinomas, 9 show evidence of multiclonal invasion, and invasive and metastatic subclones arise early along the ancestral trees. Early multiclonal invasion in the majority of these tumors indicates the expansion of co-evolving subclones with similar malignant potential in absence of late bottlenecks and suggests that barriers to invasion are minimal during colorectal cancer growth.

Funder

National Science Foundation

U.S. Department of Health & Human Services | National Institutes of Health

Triangle Center for Evolutionary Medicine - pilot funding

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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