Oligosaccharyltransferase Inhibition Overcomes Therapeutic Resistance to EGFR Tyrosine Kinase Inhibitors

Sambrooks, Cecilia López; Baro, Marta; Quijano, Amanda; Narayan, Azeet; Cui, Wei; Greninger, Patricia; Egan, Regina K.; Patel, Abhijit A.; Benes, Cyril H.; Saltzman, W. Mark; Contessa, Joseph N.

doi:10.1158/0008-5472.can-18-0505

Cited by 53 publications

(43 citation statements)

References 43 publications

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“…Analyses of epidermal growth factor receptors (EGFR) suggest that, independent of lectin-mediated effects, specific monosaccharides attached to N-linked glycans via specific linkages regulate receptor dimerization: both sialylation and outerarm fucosylation of EGFR N-linked glycans at specific sites within the receptor lead to decreased receptor dimerization and phosphorylation, whereas core fucosylation has the opposite effect (36,37,41). Intriguingly, inhibition of N-linked glycosylation with tunicamycin reduces RTK signaling in tumor cells (42)(43)(44)(45)(46). Understanding how changes in glycosylation lead to dysregulation of VEGFR2-mediated signaling is essential to the development of therapeutic strategies that facilitate tumor vessel normalization, prevent metastasis, and expand the reach of immunotherapy.…”

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confidence: 99%

N-Glycosylation regulates ligand-dependent activation and signaling of vascular endothelial growth factor receptor 2 (VEGFR2)

Chandler

Leon

Kuang

et al. 2019

Journal of Biological Chemistry

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The tumor microenvironment and proinflammatory signals significantly alter glycosylation of cell-surface proteins on endothelial cells. By altering the N-glycosylation machinery in the endoplasmic reticulum and Golgi, proinflammatory cytokines promote the modification of endothelial glycoproteins such as vascular endothelial growth factor receptor 2 (VEGFR2) with sialic acid-capped N-glycans. VEGFR2 is a highly N-glycosylated receptor tyrosine kinase involved in pro-angiogenic signaling in physiological and pathological contexts, including cancer. Here, using glycoside hydrolase and kinase assays and immunoprecipitation and MS-based analyses, we demonstrate that N-linked glycans at the Asn-247 site in VEGFR2 hinder VEGF ligand-mediated receptor activation and signaling in endothelial cells. We provide evidence that cell surfaceassociated VEGFR2 displays sialylated N-glycans at Asn-247 and, in contrast, that the nearby sites Asn-145 and Asn-160 contain lower levels of sialylated N-glycans and higher levels of high-mannose N-glycans, respectively. Furthermore, we report that VEGFR2 Asn-247-linked glycans capped with sialic acid oppose ligand-mediated VEGFR2 activation, whereas the uncapped asialo-glycans favor activation of this receptor. We propose that N-glycosylation, specifically the capping of N-glycans at Asn-247 by sialic acid, tunes ligand-dependent activation and signaling of VEGFR2 in endothelial cells.

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confidence: 99%

N-Glycosylation regulates ligand-dependent activation and signaling of vascular endothelial growth factor receptor 2 (VEGFR2)

Chandler

Leon

Kuang

et al. 2019

Journal of Biological Chemistry

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“… 0.024 (*) − 0.037 Moderate, acts as tumor suppressor in breast and other cancer types [ 24 ] p = 1.5E−3 p = 0.016 OSTC Oligosaccharyltransferase complex non-catalytic subunit 4 rs17038839 rs202168879 0.01 (*) 0.96 n.s. 0.024 (*) 0.026 Weak, subunit of the OST complex which has been associated with lung and ovarian cancer [ 25 , 26 ] p = 9.1E−4 p = 0.016 CDK2AP2 / DOC-1R Cyclin-dependent kinase 2-associated protein 2 11 rs147242558 rs530762126 0.024 (*) 1 n.s. 7.8E−3 (*) − 5.4E−3 Strong, inhibits CDK2 and G1/S phase transition, a paralog of p14 and CDK2AP1, binds CDK2AP1 [ 27 , 28 ] p = 2.7E−3 p = 0.4 POU5F1B / BRN4 POU class 5 homeobox 1B 8 *rs6983267 *rs6998061 0.027 (*) 0.02 (*) 0.09 1 n.s.…”

Section: Resultsmentioning

confidence: 99%

PWAS: proteome-wide association study—linking genes and phenotypes by functional variation in proteins

Brandes

Linial

2020

Genome Biol

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We introduce Proteome-Wide Association Study (PWAS), a new method for detecting gene-phenotype associations mediated by protein function alterations. PWAS aggregates the signal of all variants jointly affecting a protein-coding gene and assesses their overall impact on the protein’s function using machine learning and probabilistic models. Subsequently, it tests whether the gene exhibits functional variability between individuals that correlates with the phenotype of interest. PWAS can capture complex modes of heritability, including recessive inheritance. A comparison with GWAS and other existing methods proves its capacity to recover causal protein-coding genes and highlight new associations. PWAS is available as a command-line tool.

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“…Moreover, combination therapy could be used to tackle both acquired and intrinsic resistance. Furthermore, the use of molecules targeting N-glycosylation, such as the small molecule NGI-1, have shown promising results as a second-hit for cancer cells addicted to RTKs activation and resistant to TKIs [62]. Further development of 3D-cell culture techniques, especially the automation and additional advances of the high-throughput technologies, will certainly contribute to the progress in the drug discovery field.…”

Section: Discussionmentioning

confidence: 99%

Analysis of the Effect of Increased α2,3-Sialylation on RTK Activation in MKN45 Gastric Cancer Spheroids Treated with Crizotinib

Balmaña

Diniz

Feijão

et al. 2020

IJMS

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In the scenario of personalized medicine, targeted therapies are currently the focus of cancer drug development. These drugs can block the growth and spread of tumor cells by interfering with key molecules involved in malignancy, such as receptor tyrosine kinases (RTKs). MET and Recepteur d’Origine Nantais (RON), which are RTKs frequently overactivated in gastric cancer, are glycoprotein receptors whose activation have been shown to be modulated by the cellular glycosylation. In this work, we address the role of sialylation in gastric cancer therapy using an innovative 3D high-throughput cell culture methodology that mimics better the in vivo tumor features. We evaluate the response to targeted treatment of glycoengineered gastric cancer cell models overexpressing the sialyltransferases ST3GAL4 or ST3GAL6 by subjecting 3D spheroids to the tyrosine kinase inhibitor crizotinib. We show here that 3D spheroids of ST3GAL4 or ST3GAL6 overexpressing MKN45 gastric cancer cells are less affected by the inhibitor. In addition, we disclose a potential compensatory pathway via activation of the Insulin Receptor upon crizotinib treatment. Our results suggest that cell sialylation, in addition of being involved in tumor progression, could play a critical role in the response to tyrosine kinase inhibitors in gastric cancer.

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Oligosaccharyltransferase Inhibition Overcomes Therapeutic Resistance to EGFR Tyrosine Kinase Inhibitors

Cited by 53 publications

References 43 publications

N-Glycosylation regulates ligand-dependent activation and signaling of vascular endothelial growth factor receptor 2 (VEGFR2)

N-Glycosylation regulates ligand-dependent activation and signaling of vascular endothelial growth factor receptor 2 (VEGFR2)

PWAS: proteome-wide association study—linking genes and phenotypes by functional variation in proteins

Analysis of the Effect of Increased α2,3-Sialylation on RTK Activation in MKN45 Gastric Cancer Spheroids Treated with Crizotinib

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