Sequential cancer mutations in cultured human intestinal stem cells

Drost, Jarno; Jaarsveld, Richard H. van; Ponsioen, Bas; Zimberlin, Cheryl; Boxtel, Ruben van; Buijs, Arjan; Sachs, Norman; Overmeer, René M.; Offerhaus, G. Johan A.; Begthel, Harry; Korving, Jeroen; Wetering, Marc van de; Schwank, Gerald; Logtenberg, Meike E. W.; Cuppen, Edwin; Snippert, Hugo J.G.; Medema, Jan Paul; Kops, Geert J. P. L.; Clevers, Hans

doi:10.1038/nature14415

Cited by 886 publications

(928 citation statements)

References 33 publications

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“…As described, Triple SMAD4WT organoids consisted of multilayered disorganized epithelium, whereas quadruple mutant organoids mainly appeared as disorganized solid masses (SI Appendix, Fig. S2A) (7). Cell cycle analysis did not reveal major differences in proliferation rate among Triple APCWT , Triple SMAD4WT , Triple KRASWT , and quadruple mutant organoids in vitro (SI Appendix, Fig.…”

Section: Significancementioning

confidence: 99%

“…Importantly, the observation that cell growth depends on the deletion of P53 has consequences for the order of occurrence of mutations during the adenoma-carcinoma sequence. We and others (7,11) have demonstrated that loss of P53 function in intestinal stem cells induces chromosome instability (CIN). Because CIN can only lead to genetic alterations when cells divide (7,10), our data indicates that P53 is a gatekeeper that prevents acquisition of additional mutations.…”

Section: Significancementioning

confidence: 99%

“…Human intestinal stem cells can be grown "indefinitely" in vitro as 3D organoids in medium containing the stem cell niche factors Wnt, R-spondin, EGF, and Noggin while remaining genetically stable (5,6). Previously, we used CRISPR/Cas9 genome editing to engineer human colon organoids harboring mutations in four of the most frequently mutated pathways in CRC (Wnt, EGFR, P53, and TGF-β), i.e., mutations in APC [APC knock out (APC KO )], KRAS (KRAS G12D ), P53 (P53 KO ), and SMAD4 (SMAD4 KO ) (7), from here referred to as quadruple mutant organoids. Mutants were functionally selected by changing the medium composition.…”

Section: Generation Of Human Colon Organoids With Different Crc Mutationmentioning

confidence: 99%

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Genetic dissection of colorectal cancer progression by orthotopic transplantation of engineered cancer organoids

Fumagalli

Drost

Suijkerbuijk

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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In the adenoma-carcinoma sequence, it is proposed that intestinal polyps evolve through a set of defined mutations toward metastatic colorectal cancer (CRC). Here, we dissect this adenoma-carcinoma sequence in vivo by using an orthotopic organoid transplantation model of human colon organoids engineered to harbor different CRC mutation combinations. We demonstrate that sequential accumulation of oncogenic mutations in Wnt, EGFR, P53, and TGF-β signaling pathways facilitates efficient tumor growth, migration, and metastatic colonization. We show that reconstitution of specific niche signals can restore metastatic growth potential of tumor cells lacking one of the oncogenic mutations. Our findings imply that the ability to metastasize-i.e., to colonize distant sites-is the direct consequence of the loss of dependency on specific niche signals.colorectal cancer | adenoma-carcinoma sequence | organoids | metastasis | niche independence

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Section: Significancementioning

confidence: 99%

Section: Significancementioning

confidence: 99%

Section: Generation Of Human Colon Organoids With Different Crc Mutationmentioning

confidence: 99%

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Genetic dissection of colorectal cancer progression by orthotopic transplantation of engineered cancer organoids

Fumagalli

Drost

Suijkerbuijk

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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204

189

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“…Genome editing studies validating the contribution of recurrent mutations to colorectal carcinogenesis suggested that aneuploidy, as the gain of chromosomes such as 7, 13, and 20, may be associated with aggressive tumor phenotypes [97,98]. Direct confirmation of colorectal cancer exacerbation can be achieved by generating aneuploidy models by MMCT of such human chromosomes.…”

Section: In Vitro Models For Aneuploidy and Cancermentioning

confidence: 99%

Combinations of chromosome transfer and genome editing for the development of cell/animal models of human disease and humanized animal models

et al. 2017

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“…[19] Indeed, CIN has also been induced and observed in organoids, [20] but so far, side by side comparisons of CIN rates between 2D and 3D cultures in an isogenic background are still lacking.…”

Section: How and Why Is Cin Measured In Vitro?mentioning

confidence: 99%

CIN and Aneuploidy: Different Concepts, Different Consequences

Schukken

Foijer

2017

BioEssays

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Chromosomal instability (CIN) and aneuploidy are similar concepts but not synonymous. CIN is the process that leads to chromosome copy number alterations, and aneuploidy is the result. While CIN and resulting aneuploidy often cause growth defects, they are also selected for in cancer cells. Although such contradicting fates may seem paradoxical at first, they can be better understood when CIN and aneuploidy are assessed separately, taking into account the in vitro or in vivo context, the rate of CIN, and severity of the aneuploid karyotype. As CIN can only be measured in living cells, which proves to be technically challenging in vivo, aneuploidy is more frequently quantified. However, CIN rates might be more predictive for tumor outcome than assessing aneuploidy rates alone. In reviewing the literature, we therefore conclude that there is an urgent need for new models in which we can monitor chromosome mis-segregation and its consequences in vivo. Also see the video abstract here: https://youtu.be/fL3LxZduchg

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Sequential cancer mutations in cultured human intestinal stem cells

Cited by 886 publications

References 33 publications

Genetic dissection of colorectal cancer progression by orthotopic transplantation of engineered cancer organoids

Genetic dissection of colorectal cancer progression by orthotopic transplantation of engineered cancer organoids

Combinations of chromosome transfer and genome editing for the development of cell/animal models of human disease and humanized animal models

CIN and Aneuploidy: Different Concepts, Different Consequences

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