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Open AccessJournal ArticleDOI

Wnt addiction of genetically defined cancers reversed by PORCN inhibition

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TLDR
A novel potent, orally available PORCN inhibitor, ETC-1922159, that blocks the secretion and activity of all Wnts is developed that is remarkably effective in treating RSPO-translocation bearing colorectal cancer patient-derived xenografts.
Abstract
Enhanced sensitivity to Wnts is an emerging hallmark of a subset of cancers, defined in part by mutations regulating the abundance of their receptors. Whether these mutations identify a clinical opportunity is an important question. Inhibition of Wnt secretion by blocking an essential post-translational modification, palmitoleation, provides a useful therapeutic intervention. We developed a novel potent, orally available PORCN inhibitor, ETC-1922159 (henceforth called ETC-159) that blocks the secretion and activity of all Wnts. ETC-159 is remarkably effective in treating RSPO-translocation bearing colorectal cancer (CRC) patient-derived xenografts. This is the first example of effective targeted therapy for this subset of CRC. Consistent with a central role of Wnt signaling in regulation of gene expression, inhibition of PORCN in RSPO3-translocated cancers causes a marked remodeling of the transcriptome, with loss of cell cycle, stem cell and proliferation genes, and an increase in differentiation markers. Inhibition of Wnt signaling by PORCN inhibition holds promise as differentiation therapy in genetically defined human cancers.

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Citations
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Journal ArticleDOI

Autocrine Canonical Wnt Signaling Primes Noncanonical Signaling through ROR1 in Metastatic Castration-Resistant Prostate Cancer

TL;DR: Wang et al. as mentioned in this paper analyzed Wnt/β-catenin signaling in prostate cancer and identified effectors distinct from those found in other tissues, including aryl hydrocarbon receptor and RUNX1, which are linked to stem cell maintenance, and ROR1, a noncanonical Wnt5a coreceptor.
Book ChapterDOI

Lipid Modification of Proteins

TL;DR: Proteins can be covalently modified with a variety of different lipids, including fatty acids, cholesterol, isoprenoids, phospholipids, and diacylglyceryl lipids and each has been shown to regulate structure, localisation and/or function of the modified proteins.
Journal ArticleDOI

Characterization of RNF43 frameshift mutations that drive Wnt ligand‐ and R‐spondin‐dependent colon cancer

TL;DR: The results suggest that heterozygous R NF43 frameshift mutations contribute to CRC development via the serrated pathway; however, a second‐hit RNF43 mutation may be advantageous in tumorigenesis compared with a single‐hit mutation through further activation of Wnt signaling.
Journal ArticleDOI

Application of Porcupine inhibitors in stem cell fate determination

TL;DR: Porcupine (Porcn), a membrane‐bound O‐acyltransferase, is an endoplasmic reticulum‐located protein that has catalytic activity and its inhibitors.
Journal ArticleDOI

Discovery of an Orally Bioavailable Small-Molecule Inhibitor for the β-Catenin/B-Cell Lymphoma 9 Protein-Protein Interaction

TL;DR: In this paper, a drug-like small molecule, ZW4864, was reported to selectively disrupt the protein-protein interaction (PPI) between B-cell lymphoma 9 (BCL9) and β-catenin, while sparing the β-Catenin/E-cadherin PPI.
References
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Journal ArticleDOI

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Journal ArticleDOI

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Simon Anders, +1 more
- 27 Oct 2010 - 
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Journal ArticleDOI

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c-MYC-regulated micro RNAs modulate E2F1 expression

TL;DR: In this article, the proto-oncogene c-myc was found to activate expression of a cluster of six miRNAs on human chromosome 13 and showed that miR-17-5p and miR20a are negatively regulated by E2F1.
Journal ArticleDOI

c-Myc-regulated microRNAs modulate E2F1 expression.

TL;DR: A mechanism through which c-Myc simultaneously activates E2F1 transcription and limits its translation, allowing a tightly controlled proliferative signal is revealed.
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