An Enhancer-Driven Stem Cell–Like Program Mediated by SOX9 Blocks Intestinal Differentiation in Colorectal Cancer

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dc.contributor.authorLiang, X.
dc.contributor.authorDuronio, G.N.
dc.contributor.authorYang, Y.
dc.contributor.authorBala, P.
dc.contributor.authorHebbar, P.
dc.contributor.authorSpisák, S.
dc.contributor.authorSahgal, P.
dc.contributor.authorSingh, H.
dc.contributor.authorZhang, Y.
dc.contributor.authorXie, Y.
dc.contributor.authorCejas, P.
dc.contributor.authorLong, H.W.
dc.contributor.authorBass, A.J.
dc.contributor.authorSethi, N.S.
dc.date.accessioned2026-02-04T12:28:39Z
dc.date.issued2022
dc.description.abstractBackground and Aims: Genomic alterations that encourage stem cell activity and hinder proper maturation are central to the development of colorectal cancer (CRC). Key molecular mediators that promote these malignant properties require further elucidation to galvanize translational advances. We therefore aimed to characterize a key factor that blocks intestinal differentiation, define its transcriptional and epigenetic program, and provide preclinical evidence for therapeutic targeting in CRC. Methods: Intestinal tissue from transgenic mice and patients were analyzed by means of histopathology and immunostaining. Human CRC cells and neoplastic murine organoids were genetically manipulated for functional studies. Gene expression profiling was obtained through RNA sequencing. Histone modifications and transcription factor binding were determined with the use of chromatin immunoprecipitation sequencing. Results: We demonstrate that SRY-box transcription factor 9 (SOX9) promotes CRC by activating a stem cell–like program that hinders intestinal differentiation. Intestinal adenomas and colorectal adenocarcinomas from mouse models and patients demonstrate ectopic and elevated expression of SOX9. Functional experiments indicate a requirement for SOX9 in human CRC cell lines and engineered neoplastic organoids. Disrupting SOX9 activity impairs primary CRC tumor growth by inducing intestinal differentiation. By binding to genome wide enhancers, SOX9 directly activates genes associated with Paneth and stem cell activity, including prominin 1 (PROM1). SOX9 up-regulates PROM1 via a Wnt-responsive intronic enhancer. A pentaspan transmembrane protein, PROM1 uses its first intracellular domain to support stem cell signaling, at least in part through SOX9, reinforcing a PROM1-SOX9 positive feedback loop. Conclusions: These studies establish SOX9 as a central regulator of an enhancer-driven stem cell–like program and carry important implications for developing therapeutics directed at overcoming differentiation defects in CRC. © 2022
dc.identifier.citationGastroenterology, 2022, 162, 1, pp. 209-222
dc.identifier.issn165085
dc.identifier.urihttps://doi.org/10.1053/j.gastro.2021.09.044
dc.identifier.urihttps://idr.nitk.ac.in/handle/123456789/22851
dc.publisherW.B. Saunders
dc.subjectCD133 antigen
dc.subjecthistone
dc.subjectmembrane protein
dc.subjectprominin 1
dc.subjecttranscription factor
dc.subjecttranscription factor Sox9
dc.subjectunclassified drug
dc.subjectWnt protein
dc.subjectPROM1 protein, human
dc.subjectProm1 protein, mouse
dc.subjectSOX9 protein, human
dc.subjectSox9 protein, mouse
dc.subjectadenoma
dc.subjectadult
dc.subjectanimal experiment
dc.subjectanimal model
dc.subjectanimal tissue
dc.subjectArticle
dc.subjectcancer growth
dc.subjectcell activity
dc.subjectcell proliferation
dc.subjectchromatin immunoprecipitation sequencing
dc.subjectclinical outcome
dc.subjectcolorectal cancer
dc.subjectcolorectal cancer cell line
dc.subjectcolorectal carcinoma
dc.subjectcontrolled study
dc.subjectectopic expression
dc.subjectenhancer region
dc.subjectepigenetics
dc.subjectfeedback system
dc.subjectgene expression profiling
dc.subjectgene overexpression
dc.subjectgenome-wide association study
dc.subjectHCC cell line (colorectal cancer)
dc.subjecthistone modification
dc.subjecthistopathology
dc.subjecthuman
dc.subjecthuman cell
dc.subjecthuman tissue
dc.subjectimmunohistochemistry
dc.subjectin vitro study
dc.subjectintestinal organoid
dc.subjectintestinal stem cell
dc.subjectintestine tissue
dc.subjectintestine tumor
dc.subjectintron
dc.subjectmolecular biology
dc.subjectmouse
dc.subjectnonhuman
dc.subjectPaneth cell
dc.subjectpositive feedback
dc.subjectprotein binding
dc.subjectprotein domain
dc.subjectprotein expression level
dc.subjectprotein function
dc.subjectregulatory mechanism
dc.subjectRNA sequencing
dc.subjectsignal transduction
dc.subjecttissue differentiation
dc.subjecttranscription regulation
dc.subjecttumor growth
dc.subjectupregulation
dc.subjectWnt signaling
dc.subjectanimal
dc.subjectcancer stem cell
dc.subjectcell differentiation
dc.subjectcolorectal tumor
dc.subjectgene expression regulation
dc.subjectgenetics
dc.subjectHT-29 cell line
dc.subjectmetabolism
dc.subjectpathology
dc.subjecttransgenic mouse
dc.subjecttumor cell culture
dc.subjecttumor suppressor gene
dc.subjecttumor volume
dc.subjectAC133 Antigen
dc.subjectAnimals
dc.subjectCell Differentiation
dc.subjectCell Proliferation
dc.subjectColorectal Neoplasms
dc.subjectEnhancer Elements, Genetic
dc.subjectGene Expression Regulation, Neoplastic
dc.subjectGenes, APC
dc.subjectHT29 Cells
dc.subjectHumans
dc.subjectMice, Transgenic
dc.subjectNeoplastic Stem Cells
dc.subjectSOX9 Transcription Factor
dc.subjectTumor Burden
dc.subjectTumor Cells, Cultured
dc.subjectWnt Signaling Pathway
dc.titleAn Enhancer-Driven Stem Cell–Like Program Mediated by SOX9 Blocks Intestinal Differentiation in Colorectal Cancer

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