AZ1366: An Inhibitor of Tankyrase and the Canonical Wnt Pathway that Limits the Persistence of Non–Small Cell Lung Cancer Cells Following EGFR Inhibition

Scarborough, Hannah A.; Helfrich, Barbara A.; Casás‐Selves, Matias; Schuller, Alwin G.; Grosskurth, Shaun; Kim, Jihye; Tan, Aik Choon; Chan, Daniel C.; Zhang, Zhiyong; Zaberezhnyy, Vadym; Bunn, Paul A.; DeGregori, James

doi:10.1158/1078-0432.ccr-16-1179

Cited by 46 publications

(39 citation statements)

References 51 publications

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“…3A), it significantly impacted cell-cycle profiles of both PC9 and HCC4006 EGFR-mutant cell lines. Knockdown of CPS1 by itself did not significantly affect cell-cycle progression, while treatment with erlotinib led to an increase in G 1 phase and a decrease in S phases as has been shown previously (34). Importantly, knockdown of CPS1 with EGFR inhibition led to a further increase of cells in G 1 phase in PC9 and a further decrease in S phase in HCC4006 and to a lesser extent PC9 cells ( Fig.…”

Section: Cps1 Knockdown In Combination With Egfr Inhibition Affects Csupporting

confidence: 82%

Urea Cycle Sustains Cellular Energetics upon EGFR Inhibition in EGFR-Mutant NSCLC

Pham-Danis

Gehrke

Danis

et al. 2019

Molecular Cancer Research

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Mutations in oncogenes and tumor suppressor genes engender unique metabolic phenotypes crucial to the survival of tumor cells. EGFR signaling has been linked to the rewiring of tumor metabolism in non-small cell lung cancer (NSCLC). We have integrated the use of a functional genomics screen and metabolomics to identify metabolic vulnerabilities induced by EGFR inhibition. These studies reveal that following EGFR inhibition, EGFR-driven NSCLC cells become dependent on the urea cycle and, in particular, the urea cycle enzyme CPS1. Combining knockdown of CPS1 with EGFR inhibition further reduces cell proliferation and impedes cell-cycle progression. Profiling of the metabolome demonstrates that suppression of CPS1 potentiates the effects of EGFR inhibition on central carbon metabolism, pyrimidine biosynthesis, and arginine metabolism, coinciding with reduced glycolysis and mitochondrial respiration. We show that EGFR inhibition and CPS1 knockdown lead to a decrease in arginine levels and pyrimidine derivatives, and the addition of exogenous pyrimidines partially rescues the impairment in cell growth. Finally, we show that high expression of CPS1 in lung adenocarcinomas correlated with worse patient prognosis in publicly available databases. These data collectively reveal that NSCLC cells have a greater dependency on the urea cycle to sustain central carbon metabolism, pyrimidine biosynthesis, and arginine metabolism to meet cellular energetics upon inhibition of EGFR.Implications: Our results reveal that the urea cycle may be a novel metabolic vulnerability in the context of EGFR inhibition, providing an opportunity to develop rational combination therapies with EGFR inhibitors for the treatment of EGFRdriven NSCLC. Analysis and interpretation of data (e.g., statistical analysis, biostatistics, computational analysis): C. Pham-Danis, S.

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Section: Cps1 Knockdown In Combination With Egfr Inhibition Affects Csupporting

confidence: 82%

Urea Cycle Sustains Cellular Energetics upon EGFR Inhibition in EGFR-Mutant NSCLC

Pham-Danis

Gehrke

Danis

et al. 2019

Molecular Cancer Research

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“…The enzyme TNKS1 and the closely related paralog TNKS2, which is less abundant, but was still identified in HeLa cells, are poly-ADP-ribosyltransferases involved in various processes such as telomere length regulation 53 , mitotic spindle formation 54 , proteasomal degradation 55,56 , vesicle trafficking 57 , and Wnt signaling pathway 6 AXIN1 and AXIN2, two key components of the β-catenin destruction complex 6 . The inhibition of TNKS1 catalytic activity antagonizes Wnt signaling and has promising implications for cancer therapy, particularly colorectal cancer and non-small cell lung cancer 6,58,59 . Tankyrase is also crucial for embryonic development and adult homeostasis 60 .…”

Section: Discussionmentioning

confidence: 99%

Sjögren syndrome/scleroderma autoantigen 1 is a direct Tankyrase binding partner in cancer cells

et al. 2020

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Sjögren syndrome/scleroderma autoantigen 1 (SSSCA1) was first described as an autoantigen over-expressed in Sjögren's syndrome and in scleroderma patients. SSSCA1 has been linked to mitosis and centromere association and as a potential marker candidate in diverse solid cancers. Here we characterize SSSCA1 for the first time, to our knowledge, at the molecular, structural and subcellular level. We have determined the crystal structure of a zinc finger fold, a zinc ribbon domain type 2 (ZNRD2), at 2.3 Å resolution. We show that the Cterminal domain serves a dual function as it both behaves as the interaction site to Tankyrase 1 (TNKS1) and as a nuclear export signal. We identify TNKS1 as a direct binding partner of SSSCA1, map the binding site to TNKS1 ankyrin repeat cluster 2 (ARC2) and thus define a new binding sequence. We experimentally verify and map a new nuclear export signal sequence in SSSCA1.

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“…(c) β-Catenin fold induction is essential for the activation of β-catenin target genes [119][120][121] . (d) Increased AXIN1 by Tankyrase inhibitor suppresses cell proliferation of cancer cells where Wnt/β-catenin signaling is genetically hyperactive 43,90,93,95,122 . (e) Mutations in RNF43 and ZNRF3 E3 ligases that degrade Wnt receptors contribute to tumor development 111,115 .…”

Section: Additional Layers Of Wnt/β-catenin Signaling Activationmentioning

confidence: 99%

Wnt signaling in cancer: therapeutic targeting of Wnt signaling beyond β-catenin and the destruction complex

2020

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Wnt/β-catenin signaling is implicated in many physiological processes, including development, tissue homeostasis, and tissue regeneration. In human cancers, Wnt/β-catenin signaling is highly activated, which has led to the development of various Wnt signaling inhibitors for cancer therapies. Nonetheless, the blockade of Wnt signaling causes side effects such as impairment of tissue homeostasis and regeneration. Recently, several studies have identified cancer-specific Wnt signaling regulators. In this review, we discuss the Wnt inhibitors currently being used in clinical trials and suggest how additional cancer-specific regulators could be utilized to treat Wnt signaling-associated cancer.

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AZ1366: An Inhibitor of Tankyrase and the Canonical Wnt Pathway that Limits the Persistence of Non–Small Cell Lung Cancer Cells Following EGFR Inhibition

Cited by 46 publications

References 51 publications

Urea Cycle Sustains Cellular Energetics upon EGFR Inhibition in EGFR-Mutant NSCLC

Urea Cycle Sustains Cellular Energetics upon EGFR Inhibition in EGFR-Mutant NSCLC

Sjögren syndrome/scleroderma autoantigen 1 is a direct Tankyrase binding partner in cancer cells

Wnt signaling in cancer: therapeutic targeting of Wnt signaling beyond β-catenin and the destruction complex

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