Abstract
<div>Abstract<p>Despite the connection of secretory cells, including goblet and enteroendocrine (EEC) cells, to distinct mucus-containing colorectal cancer histologic subtypes, their role in colorectal cancer progression has been underexplored. Here, our analysis of The Cancer Genome Atlas (TCGA) and single-cell RNA-sequencing data demonstrates that EEC progenitor cells are enriched in <i>BRAF</i>-mutant colorectal cancer patient tumors, cell lines, and patient-derived organoids. In <i>BRAF</i>-mutant colorectal cancer, EEC progenitors were blocked from differentiating further by DNA methylation and silencing of NEUROD1, a key gene required for differentiation of intermediate EECs. Mechanistically, secretory cells and the factors they secrete, such as trefoil factor 3, promoted colony formation and activation of cell survival pathways in the entire cell population. Lysine-specific demethylase 1 (LSD1) was identified as a critical regulator of secretory cell specification <i>in vitro</i> and in a colon orthotopic xenograft model, where LSD1 loss blocks formation of EEC progenitors and reduces tumor growth and metastasis. These findings reveal an important role for EEC progenitors in supporting colorectal cancer.</p>Significance:<p>This study establishes enteroendocrine progenitors as a targetable population that promotes <i>BRAF</i>-mutant colorectal cancer and can be blocked by LSD1 inhibition to suppress tumor growth.</p></div>
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