Inactivating mutations of
            <i>RNF43</i>
            confer Wnt dependency in pancreatic ductal adenocarcinoma

Jiang, Xiaomo; Hao, Huai-Xiang; Growney, Joseph D.; Woolfenden, Steve; Bottiglio, Cindy; Ng, Nicholas; Lü, Bo; Hsieh, Mindy H.; Bagdasarian, Linda; Meyer, Ronald A.; Smith, Timothy R.; Avello, Monika; Charlat, Olga; Xie, Yang; Porter, Jeffery A.; Pan, Shifeng; Li, Jun; McLaughlin, Margaret E.; Cong, Feng

doi:10.1073/pnas.1307218110

Cited by 373 publications

(403 citation statements)

References 42 publications

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“…The prevention of Wnt ligand secretion after treatment with WNT974 results in decreased phosphorylation of the surface receptor LRP6 and decreased expression of Wnt target genes like AXIN2. 16,17 WNT974 has shown anti-tumor activity in pancreatic adenocarcinoma and head and neck squamous cell cancer. Jiang et al 17 identified both WNT974 sensitive tumor cells and a potential predictive biomarker after demonstrating tumor growth inhibition through cell cycle arrest in in vivo pancreatic tumors treated with WNT974 with inactivating mutations in the RNF43 gene.…”

Section: Discussionmentioning

confidence: 99%

“…16 WNT974 has been shown to suppress growth of Wnt-driven tumors, such as pancreatic and head and neck squamous cell cancer with mutations in Wnt pathway modulators such as Ring finger 43 (RNF43). 17 The R-spondin (RSPO) protein family is comprised of four secreted growth factors. Secreted RSPO proteins activate Wnt/ β-catenin signaling, and RSPO mutations can further upregulate Wnt/β-catenin signaling.…”

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confidence: 99%

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Targeting the Wnt/β-catenin pathway in primary ovarian cancer with the porcupine inhibitor WNT974

Boone

Arend

Johnston

et al. 2016

Laboratory Investigation

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Preclinical studies in ovarian cancer have demonstrated upregulation of the Wnt/β-catenin pathway promoting tumor proliferation and chemoresistance. Our objective was to evaluate the effect of the Wnt/β-catenin pathway inhibitor, WNT974, in primary ovarian cancer ascites cells. Ascites cells from patients with papillary serous ovarian cancer were isolated and treated with 1 μM WNT974 ± 100 μM carboplatin. Viability was evaluated with the ATPlite assay. The IC 50 was calculated using a dose-response analysis. Immunohistochemistry (IHC) was performed on ascites cells and tumor. Expression of R-spondin 2 (RSPO2), RSPO3, PORCN, WLS, AXIN2, and three previously characterized RSPO fusion transcripts were assessed using Taqman assays. Sixty ascites samples were analyzed for response to WNT974. The ascites samples that showed a decrease in ATP concentration after treatment demonstrated no difference from the untreated cells in percent viability with trypan blue staining. Flow cytometry demonstrated fewer cells in the G2 phase and more in the G1 and S phases after treatment with WNT974. Combination therapy with WNT974 and carboplatin resulted in a higher percentage of samples that showed ≥ 30% reduction in ATP concentration than either single drug treatment. IHC analysis of Wnt pathway proteins suggests cell cycle arrest rather than cytotoxicity after WNT974 treatment. QPCR indicated that RSPO fusions are not prevalent in ovarian cancer tissues or ascites. However, higher PORCN expression correlated to sensitivity to WNT974 (P = 0.0073). In conclusion, WNT974 produces cytostatic effects in patient ascites cells with primary ovarian cancer through inhibition of the Wnt/β-catenin pathway. The combination of WNT974 and carboplatin induces cytotoxicity plus cell cycle arrest in a higher percentage of ascites samples than with single drug treatment. RSPO fusions do not contribute to WNT974 sensitivity; however, higher PORCN expression indicates increased WNT974 sensitivity.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Targeting the Wnt/β-catenin pathway in primary ovarian cancer with the porcupine inhibitor WNT974

Boone

Arend

Johnston

et al. 2016

Laboratory Investigation

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“…Recent studies (ref. 44; Madan and colleagues; unpublished data) have demonstrated that the proliferation of pancreatic cancer cell lines and patient-derived xenografts with inactivating RNF43 mutations is inhibited by PORCN inhibitors, including LGK974, Wnt-C59, and ETC-159. Hence, RNF43 and ZNRF3 mutations, by sensitizing cells to Wnts, may also be predictive of response to both PORCN inhibitors and Frizzled antibodies.…”

Section: Rnf43 and Znrf3 Loss-of-function Mutationsmentioning

confidence: 99%

Targeting Wnts at the Source—New Mechanisms, New Biomarkers, New Drugs

Madan

Virshup

2015

Molecular Cancer Therapeutics

102

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Wnt signaling is dysregulated in many cancers and is therefore an attractive therapeutic target. The focus of drug development has recently shifted away from downstream inhibitors of b-catenin. Active inhibitors of Wnt secretion and Wnt/receptor interactions have been developed that are now entering clinical trials. Such agents include inhibitors of Wnt secretion, as well as recombinant proteins that minimize Wnt-Frizzled interactions. These new therapies arrive together with the recent insight that cancer-specific upregulation of Wnt receptors at the cell surface regulates cellular sensitivity to Wnts. Loss-of-function mutations in RNF43 or ZNRF3 and gain-of-function chromosome translocations involving RSPO2 and RSPO3 are surprisingly common and markedly increase Wnt/b-catenin signaling in response to secreted Wnts. These mutations may be predictive biomarkers to select patients responsive to newly developed upstream Wnt inhibitors.

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“…8 RNF43 mutations have also been shown to confer Wnt dependency in pancreatic cancer cells. 9 However, the clinicopathological relevance of RNF43 mutations in intraductal papillary mucinous neoplasms remains unclear.…”

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confidence: 99%

Clinicopathological significance of somatic RNF43 mutation and aberrant expression of ring finger protein 43 in intraductal papillary mucinous neoplasms of the pancreas

et al. 2015

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Mutations in RNF43, which encodes the ubiquitin E3 ligase ring finger protein 43, were recently found in intraductal papillary mucinous neoplasms of the pancreas. We evaluated somatic mutations of RNF43 and the expression of ring finger protein 43 as well as their associations with the molecular and clinicopathological features in 176 surgically resected intraductal papillary mucinous neoplasms. Frozen tissues were available for 57 cases and were used for next-generation sequencing analysis of the entire coding exons of RNF43. Formalin-fixed and paraffinembedded tissues from all 176 cases were used for the immunohistochemical analysis of the expression of ring finger protein 43. Mutations detected with the next-generation sequencing analysis were validated by using Sanger sequencing. Statistical analysis was used to evaluate the associations between RNF43 aberrations and molecular and clinicopathological features including GNAS mutations, KRAS mutations, loss of SMA and MAD4 homologue expression, tumor protein 53 overexpression, tumor grade, histological type, mural nodule detection, macroscopic type, stage, recurrence, and survival. Somatic RNF43 mutations were found in 8 (14%) of the 57 examined cases, and included 5 frameshift mutations (p.F69fs, p.S264fs, p.L311fs, p.R363fs, and p.V490fs), 1 non-sense mutation (p.Q153X), and 2 missense mutations (p.I164N and p.P310A). The expression of ring finger protein 43 was downregulated in 52 (29.5%) of the 176 examined cases. RNF43 mutations were significantly associated with the downregulated expression of ring finger protein 43 (P ¼ 0.011), GNAS mutation (P ¼ 0.020), and mural nodule detection (P ¼ 0.038). The expression of ring finger protein 43 was not associated with any clinicopathological features except RNF43 mutation. These results indicate that RNF43 mutation might cause downregulation of the expression of ring finger protein 43 and play a crucial role and associate synergistically with GNAS mutation during development of intraductal papillary mucinous neoplasm of the pancreas.

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Inactivating mutations of RNF43 confer Wnt dependency in pancreatic ductal adenocarcinoma

Cited by 373 publications

References 42 publications

Targeting the Wnt/β-catenin pathway in primary ovarian cancer with the porcupine inhibitor WNT974

Targeting the Wnt/β-catenin pathway in primary ovarian cancer with the porcupine inhibitor WNT974

Targeting Wnts at the Source—New Mechanisms, New Biomarkers, New Drugs

Clinicopathological significance of somatic RNF43 mutation and aberrant expression of ring finger protein 43 in intraductal papillary mucinous neoplasms of the pancreas

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