Abstract
Colon cancers are composed of phenotypically heterogeneous tumor cell subpopulations with variable expression of putative stem cell and differentiation antigens. While in normal colonic mucosa, clonal repopulation occurs along differentiation gradients from crypt base toward crypt apex, the clonal architecture of colon cancer and the relevance of tumor cell subpopulations for clonal outgrowth are poorly understood. Using a multicolor lineage tracing approach in colon cancer xenografts that reflect primary colon cancer architecture, we here demonstrate that clonal outgrowth is mainly driven by tumor cells located at the leading tumor edge with clonal axis formation toward the tumor center. While our findings are compatible with lineage outgrowth in a cancer stem cell model, they suggest that in colorectal cancer tumor cell position may be more important for clonal outgrowth than tumor cell phenotype.
Highlights
Colon cancers are composed of phenotypically heterogeneous tumor cell subpopulations with variable expression of putative stem cell and differentiation antigens
Current studies demonstrated clonal outgrowth from colon cancer cells with high MAPK activity or expression of the WNT target gene LGR5, and provided direct evidence for a cellular hierarchy emanating from these tumor cell subsets in vivo[13, 14]
We demonstrate that clonal expansion starts at the leading tumor edge, where tumor cells compete for outgrowth toward the tumor center, where clones may be lost due to tumor necrosis
Summary
Colon cancers are composed of phenotypically heterogeneous tumor cell subpopulations with variable expression of putative stem cell and differentiation antigens. From these data, the role of distinct tumor cell phenotypes for the dynamics of clonal expansion in colon cancer has remained unclear.
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