Targeting the Two Oncogenic Functional Sites of the HPV E6 Oncoprotein with a High‐Affinity Bivalent Ligand

Ramírez, Juan Antonio Ortega; Poirson, Juline; Foltz, Clémence; Chebaro, Yassmine; Schrapp, Maxime; Meyer, Amandine; Bonetta, Anaëlle; Förster, Anne; Jacob, Yves; Masson, Murielle; Deryckère, François; Travé, Gilles

doi:10.1002/anie.201502646

Cited by 34 publications

(38 citation statements)

References 37 publications

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“…The nature of the E6 PBM interaction with PDZ domains makes it an amenable peptide-protein interaction for inhibition by small molecules with the intention to develop novel therapeutics for the treatment of HPV–associated cancers [54, 55]. Since the E6 PBM is essential for viral replication [27], inhibition of this function may be considered a route of anti-viral intervention to treat active infections.…”

Section: Discussionmentioning

confidence: 99%

Mitotic control of human papillomavirus genome-containing cells is regulated by the function of the PDZ-binding motif of the E6 oncoprotein

et al. 2017

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The function of a conserved PDS95/DLG1/ZO1 (PDZ) binding motif (E6 PBM) at the C-termini of E6 oncoproteins of high-risk human papillomavirus (HPV) types contributes to the development of HPV-associated malignancies. Here, using a primary human keratinocyte-based model of the high-risk HPV18 life cycle, we identify a novel link between the E6 PBM and mitotic stability. In cultures containing a mutant genome in which the E6 PBM was deleted there was an increase in the frequency of abnormal mitoses, including multinucleation, compared to cells harboring the wild type HPV18 genome. The loss of the E6 PBM was associated with a significant increase in the frequency of mitotic spindle defects associated with anaphase and telophase. Furthermore, cells carrying this mutant genome had increased chromosome segregation defects and they also exhibited greater levels of genomic instability, as shown by an elevated level of centromere-positive micronuclei. In wild type HPV18 genome-containing organotypic cultures, the majority of mitotic cells reside in the suprabasal layers, in keeping with the hyperplastic morphology of the structures. However, in mutant genome-containing structures a greater proportion of mitotic cells were retained in the basal layer, which were often of undefined polarity, thus correlating with their reduced thickness. We conclude that the ability of E6 to target cellular PDZ proteins plays a critical role in maintaining mitotic stability of HPV infected cells, ensuring stable episome persistence and vegetative amplification.

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Section: Discussionmentioning

confidence: 99%

Mitotic control of human papillomavirus genome-containing cells is regulated by the function of the PDZ-binding motif of the E6 oncoprotein

et al. 2017

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“…[257] The human adenovirus type 9 (Ad9) E4 region ORF1 gene product, E4-ORF1, is another viral protein, which targets several PDZ-containing proteins through a C-terminal PDZ binding motif. d) Graphical model of the PDZbody [259,275] where the HPV18-E6 protein binds to the canonical binding pocket in the optimized SAP-97-PDZ2 through its C-terminal residues. [258] Adv.…”

Section: Targeting Pdz Domain Proteins Involved In Viral Infectionsmentioning

confidence: 99%

“…[258] Adv. [275] Human Papillomavirus (HPV) E6 and E7 hijack the cell during infection by interacting with endogenous proteins such as the well-described transcription factor and tumor suppressor, p53, and several PDZ-containing proteins. 2019, 2, show very similar insertion of the two peptides into the binding pocket.…”

Section: Targeting Pdz Domain Proteins Involved In Viral Infectionsmentioning

confidence: 99%

“…[272] This activation of PI3K deregulates cytosolic signalling pathway, which leads to cell survival and metabolism, and enhances virus replication. [275] In addition to the more well-studied interactions with viral proteins from HTLV-1, Ad9, and HPV, SAP-97 and Scribble have also been associated with Hepatitis C virus. [274] Because of the role HPV E6 plays in transforming infected cells into cancer cells, it is considered a potential drug target.…”

Section: Targeting the Pdz Domains Of Sap-97 And Scribblementioning

confidence: 99%

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PDZ Domains as Drug Targets

Christensen

Čalyševa

Fernandes

et al. 2019

Advanced Therapeutics

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Protein-protein interactions within protein networks shape the human interactome, which often is promoted by specialized protein interaction modules, such as the postsynaptic density-95 (PSD-95), discs-large, zona occludens 1 (ZO-1) (PDZ) domains. PDZ domains play a role in several cellular functions, from cell-cell communication and polarization, to regulation of protein transport and protein metabolism. PDZ domain proteins are also crucial in the formation and stability of protein complexes, establishing an important bridge between extracellular stimuli detected by transmembrane receptors and intracellular responses. PDZ domains have been suggested as promising drug targets in several diseases, ranging from neurological and oncological disorders to viral infections. In this review, the authors describe structural and genetic aspects of PDZ-containing proteins and discuss the current status of the development of small-molecule and peptide modulators of PDZ domains. An overview of potential new therapeutic interventions in PDZ-mediated protein networks is also provided.

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“…These results are particularly intriguing since the PBM deletion mutants of E6 target p53 as efficiently as wild type E6. This indicates that at least one aspect of E6 PDZ targeting links directly to pathways that are controlled by p53 [ 67 , 68 ]. It is also possible that the PDZ-PBM interaction of wild type E6 contributes towards the abrogation of a p53 function that is independent of the degradation of p53, and this functional ablation is necessary for viral genome maintenance.…”

Section: The E6 Pbm and The Viral Life Cyclementioning

confidence: 99%

The Human Papillomavirus E6 PDZ Binding Motif: From Life Cycle to Malignancy

Ganti

Broniarczyk

Manoubi

et al. 2015

Viruses

109

124

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Cancer-causing HPV E6 oncoproteins are characterized by the presence of a PDZ binding motif (PBM) at their extreme carboxy terminus. It was long thought that this region of E6 had a sole function to confer interaction with a defined set of cellular substrates. However, more recent studies have shown that the E6 PBM has a complex pattern of regulation, whereby phosphorylation within the PBM can regulate interaction with two classes of cellular proteins: those containing PDZ domains and the members of the 14-3-3 family of proteins. In this review, we explore the roles that the PBM and its ligands play in the virus life cycle, and subsequently how these can inadvertently contribute towards the development of malignancy. We also explore how subtle alterations in cellular signal transduction pathways might result in aberrant E6 phosphorylation, which in turn might contribute towards disease progression.

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Targeting the Two Oncogenic Functional Sites of the HPV E6 Oncoprotein with a High‐Affinity Bivalent Ligand

Cited by 34 publications

References 37 publications

Mitotic control of human papillomavirus genome-containing cells is regulated by the function of the PDZ-binding motif of the E6 oncoprotein

Mitotic control of human papillomavirus genome-containing cells is regulated by the function of the PDZ-binding motif of the E6 oncoprotein

PDZ Domains as Drug Targets

The Human Papillomavirus E6 PDZ Binding Motif: From Life Cycle to Malignancy

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