Mutated in colorectal cancer, a putative tumor suppressor for serrated colorectal cancer, selectively represses β-catenin-dependent transcription

Fukuyama, Ryuichi; Niculaita, Roxana; Ng, Kwok Peng; Obusez, Emmanuel C.; Sánchez, Julián; Kalady, Matthew F.; Aung, Phyu P.; Casey, Graham; Sizemore, Nywana

doi:10.1038/onc.2008.204

Cited by 74 publications

(133 citation statements)

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“…In immunohistochemical studies, strong APC expression was observed in most SSA/Ps, whereas MCC expression was reported to be frequently lost. 21,22 MCC methylation is more common in SSA/Ps (89%) than in adenomas (35%). 20 Our study showed that MCC was methylated in 15% of SSA/Ps, and in all of SSA/Ps with high-grade dysplasia and those with submucosal carcinoma, but only 11-16% of the adenoma series.…”

Section: Modern Pathology (2015) 28 146-158mentioning

confidence: 99%

“…As a result, free b-catenin accumulates and translocates into the nucleus and subsequently binds to the T-cell factor/ lymphoid enhancer factor initiating transcription of target genes such as c-myc. 17 b-Catenin is also regulated by various other components such as mutated in colorectal cancer (MCC) and secreted frizzled-related proteins (SFRPs); 17 the functions of MCC or SFRPs as negative regulators of WNT/b-catenin signaling may have important implications in genesis of colorectal carcinomas [19][20][21] as well as SSA/P. 22 AXIN2 has been found to be silenced, apparently as a result of methylation of its promoter region, specifically in colorectal carcinomas with high levels of microsatellite instability.…”

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confidence: 99%

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Distinct WNT/β-catenin signaling activation in the serrated neoplasia pathway and the adenoma-carcinoma sequence of the colorectum

et al. 2015

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Sessile serrated adenoma/polyp (SSA/P) is considered as an early precursor in the serrated neoplasia pathway leading to colorectal cancer development. The conventional adenoma-carcinoma sequence is associated with activation of the WNT signaling pathway, although its role in serrated lesions is still controversial. To clarify differences in WNT signaling activation in association with MLH1 methylation or BRAF/KRAS mutations between serrated and conventional routes, we performed b-catenin immunostaining, methylation-specific PCR for MLH1 and WNT signaling associated genes such as AXIN2, APC, and MCC and secreted frizzled-related proteins (SFRPs), and direct sequencing of BRAF/KRAS in 27 SSA/Ps, 14 SSA/Ps with high-grade dysplasia and 9 SSA/Ps with submucosal carcinoma, as well as 19 conventional adenomas, 26 adenomas with high-grade dysplasia and 25 adenomas with submucosal carcinoma. Nuclear b-catenin labelings were significantly lower in the serrated series than in their adenoma counterparts, and a significant increment in those labelings was found from SSA/Ps to those with high-grade dysplasia or submucosal carcinoma. The frequency of MLH1 and SFRP4 methylation was significantly higher in SSA/P series, as compared with corresponding adenoma series. AXIN2 and MCC were more frequently methylated in SSA/Ps with high-grade dysplasia and those with submucosal carcinoma than in adenoma counterparts. Stepwise increment of AXIN2 and MCC methylation was identified from SSA/Ps through those with high-grade dysplasia to those with submucosal carcinoma. A significant correlation was seen between nuclear b-catenin expression and methylation of AXIN2 or MCC in the SSA/P series. BRAF mutation was more frequent, whereas KRAS mutation was less frequent in the SSA/P series as compared with the adenoma series. There was an inverse association of BRAF mutation with AXIN2 methylation in SSA/P series. In conclusion, WNT/b-catenin signal activation mediated by the methylation of SFRP4, MCC, and AXIN2 may make different contributions to colorectal neoplasia between the serrated and conventional routes.

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Section: Modern Pathology (2015) 28 146-158mentioning

confidence: 99%

mentioning

confidence: 99%

Distinct WNT/β-catenin signaling activation in the serrated neoplasia pathway and the adenoma-carcinoma sequence of the colorectum

et al. 2015

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“…In overexpression studies, MCC was shown to physically associate with β-catenin in the nucleus to negatively regulate canonical TCF/ LEF-dependent Wnt signaling and to inhibit cell proliferation (Fukuyama et al, 2008;Matsumine et al, 1996). More recently, MCC was observed to be mainly localized in the cytoplasm of colon cancer cell lines but translocated to the nucleus in response to DNA damage to induce cell cycle arrest (Pangon et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

“…MCC has previously been reported to antagonize canonical Wnt signaling in CRC cell lines (Fukuyama et al, 2008). We evaluated whether Mcc can inhibit β-catenin-dependent activation of the −0.8 kb Xenopus Siamois luciferase reporter, and found that Mcc overexpression has no effect on reporter activation -neither synergy nor inhibition -upon co-injection of mRNA encoding either the canonical Wnt8 ligand, which normally suppresses dorsal organizer genes and patterns ventrolateral mesoderm, or its effector β-catenin (Baker et al, 2010) (supplementary material Fig.…”

Section: Introductionmentioning

confidence: 99%

“…Immunolocalization studies in a variety of cell types show that MCC is principally a cytoplasmic protein (Fukuyama et al, 2008;Matsumine et al, 1996;Pangon et al, 2010;Senda et al, 1999). We determined the subcellular distribution of Mcc in the gastrulating zebrafish embryo by injecting mRNA encoding an N-terminal GFP-Mcc fusion protein and imaging GFP fluorescence at shield stage.…”

Section: Introductionmentioning

confidence: 99%

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The PDZ domain protein Mcc is a novel effector of non-canonical Wnt signaling during convergence and extension in zebrafish

et al. 2014

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During vertebrate gastrulation, a complex set of mass cellular rearrangements shapes the embryonic body plan and appropriately positions the organ primordia. In zebrafish and Xenopus, convergence and extension (CE) movements simultaneously narrow the body axis mediolaterally and elongate it from head to tail. This process is governed by polarized cell behaviors that are coordinated by components of the non-canonical, β-catenin-independent Wnt signaling pathway, including Wnt5b and the transmembrane planar cell polarity (PCP) protein Vangl2. However, the intracellular events downstream of Wnt/PCP signals are not fully understood. Here, we show that zebrafish mutated in colorectal cancer (mcc), which encodes an evolutionarily conserved PDZ domain-containing putative tumor suppressor, is required for Wnt5b/Vangl2 signaling during gastrulation. Knockdown of mcc results in CE phenotypes similar to loss of vangl2 and wnt5b, whereas overexpression of mcc robustly rescues the depletion of wnt5b, vangl2 and the Wnt5b tyrosine kinase receptor ror2. Biochemical experiments establish a direct physical interaction between Mcc and the Vangl2 cytoplasmic tail. Lastly, CE defects in mcc morphants are suppressed by downstream activation of RhoA and JNK. Taken together, our results identify Mcc as a novel intracellular effector of non-canonical Wnt5b/ Vangl2/Ror2 signaling during vertebrate gastrulation.

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Norepinephrine‐CREB1‐miR‐373 axis promotes progression of colon cancer

Han

Jiang

et al. 2020

Molecular Oncology

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The adrenergic system contributes to the stress-induced onset and progression of cancer. Adrenergic fibers are the primary source of norepinephrine (NE). The underlying mechanisms involved in NE-induced colon cancer remain to be understood. In this study, we describe the function and regulatory network of NE in the progression of colon cancer. We demonstrate that NE-induced phosphorylation of cAMP response element-binding protein 1 (CREB1) promotes proliferation, migration, and invasion of human colon cancer cells. The downstream effector of NE, CREB1, bound to the promoter of miR-373 and transcriptionally activated its expression. miR-373 expression was shown to be necessary for NE-induced cell proliferation, invasion, and tumor growth. We confirmed that proliferation and invasion of colon cancer cells are regulated in vitro and in vivo by miR-373 through targeting of the tumor suppressors TIMP2 and APC. Our data suggest that NE promotes colon cancer cell proliferation and metastasis by activating the CREB1-miR-373 axis. The study of this novel signaling axis may provide mechanistic insights into the neural regulation of colon cancer and help in the design of future clinical studies on stress biology in colorectal cancer.Abbreviations APC, adenomatous polyposis coli; CRC, colorectal cancer; CREB1, cAMP response element-binding protein 1; NE, norepinephrine; qRT-PCR, quantitative real-time polymerase chain reaction; TCGA, The Cancer Genome Atlas; TH, tyrosine hydroxylase; TIMP2, tissue inhibitor of metalloproteinases 2.

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Mutated in colorectal cancer, a putative tumor suppressor for serrated colorectal cancer, selectively represses β-catenin-dependent transcription

Cited by 74 publications

References 36 publications

Distinct WNT/β-catenin signaling activation in the serrated neoplasia pathway and the adenoma-carcinoma sequence of the colorectum

Distinct WNT/β-catenin signaling activation in the serrated neoplasia pathway and the adenoma-carcinoma sequence of the colorectum

The PDZ domain protein Mcc is a novel effector of non-canonical Wnt signaling during convergence and extension in zebrafish

Norepinephrine‐CREB1‐miR‐373 axis promotes progression of colon cancer

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