Cancer Cells Retrace a Stepwise Differentiation Program during Malignant Progression

Hanahan, Douglas

doi:10.1158/2159-8290.CD-20-1637

Publication:
Cancer Cells Retrace a Stepwise Differentiation Program during Malignant Progression

cris.lastimport.scopus	2024-08-08T08:14:06Z
cris.legacyId	289597
cris.virtual.department	CMSO
cris.virtual.department	CMSO
cris.virtual.parent-organization	ISREC
cris.virtual.parent-organization	SV
cris.virtual.parent-organization	EPFL
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cris.virtual.unitManager	Oricchio, Elisa
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datacite.rights	metadata-only
dc.contributor.author	Saghafinia, Sadegh
dc.contributor.author	Homicsko, Krisztian
dc.contributor.author	Di Domenico, Annunziata
dc.contributor.author	Wullschleger, Stephan
dc.contributor.author	Perren, Aurel
dc.contributor.author	Marinoni, Ilaria
dc.contributor.author	Ciriello, Giovanni
dc.contributor.author	Michael, Iacovos P.
dc.contributor.author	Hanahan, Douglas
dc.date.accessioned	2021-10-23T02:34:15
dc.date.available	2021-10-23T02:34:15
dc.date.created	2021-10-23
dc.date.issued	2021-10-01
dc.date.modified	2024-10-18T12:09:31.479529Z
dc.description.abstract	Pancreatic neuroendocrine tumors (PanNET) comprise two molecular subtypes, relatively benign islet tumors (IT) and invasive, metastasis-like primary (MLP) tumors. Until now, the origin of aggressive MLP tumors has been obscure. Herein, using multi-omics approaches, we revealed that MLP tumors arise from IT via dedifferentiation following a reverse trajectory along the developmental pathway of islet beta cells, which results in the acquisition of a progenitor-like molecular phenotype. Functionally, the miR-181cd cluster induces the IT-to-MLP transition by suppressing expression of the Meis2 transcription factor, leading to upregulation of a developmental transcription factor, Hmgb3. Notably, the IT-to-MLP transition constitutes a distinct step of tumorigenesis and is separable from the classic proliferation-associated hallmark, temporally preceding accelerated proliferation of cancer cells. Furthermore, patients with PanNET with elevated HMGB3 expression and an MLP transcriptional signature are associated with higher-grade tumors and worse survival. Overall, our results unveil a new mechanism that modulates cancer cell plasticity to enable malignant progression.
dc.description.abstract	SIGNIFICANCE: Dedifferentiation has long been observed as a histopathologic characteristic of many cancers, albeit inseparable from concurrent increases in cell proliferation. Herein, we demonstrate that dedifferentiation is a mechanistically and temporally separable step in the multistage tumorigenesis of pancreatic islet cells, retracing the developmental lineage of islet beta cells.
dc.description.sponsorship	CMSO
dc.identifier.doi	10.1158/2159-8290.CD-20-1637
dc.identifier.isi	WOS:000704194700035
dc.identifier.uri	https://infoscience.epfl.ch/handle/20.500.14299/182532
dc.publisher	AMER ASSOC CANCER RESEARCH
dc.publisher.place	Philadelphia
dc.relation.issn	2159-8274
dc.relation.issn	2159-8290
dc.relation.journal	Cancer Discovery
dc.source	WoS
dc.subject	Oncology
dc.subject	pancreatic neuroendocrine tumors
dc.subject	beta-cell
dc.subject	reveals
dc.subject	expression
dc.subject	hmgb3
dc.subject	tumorigenesis
dc.subject	stemness
dc.subject	matrix
dc.subject	growth
dc.subject	dna
dc.title	Cancer Cells Retrace a Stepwise Differentiation Program during Malignant Progression
dc.type	text::journal::journal article::research article
dspace.entity.type	Publication
dspace.legacy.oai-identifier	oai:infoscience.epfl.ch:289597
epfl.curator.email	jorge.rodriguesdematos@epfl.ch
epfl.legacy.itemtype	Journal Articles
epfl.legacy.submissionform	ARTICLE
epfl.oai.currentset	OpenAIREv4
epfl.oai.currentset	SV
epfl.oai.currentset	article
epfl.peerreviewed	REVIEWED
epfl.publication.version	http://purl.org/coar/version/c_970fb48d4fbd8a85
epfl.writtenAt	EPFL
oaire.citation.endPage	2657
oaire.citation.issue	10
oaire.citation.startPage	2638
oaire.citation.volume	11

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Cancer Cells Retrace a Stepwise Differentiation Program during Malignant Progression