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Interaction of the Human Papillomavirus E6 Oncoprotein with Sorting Nexin 27 Modulates Endocytic Cargo Transport Pathways

Overview
Journal PLoS Pathog
Specialty Microbiology
Date 2016 Sep 21
PMID 27649450
Citations 26
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Abstract

A subset of high-risk Human Papillomaviruses (HPVs) are the causative agents of a large number of human cancers, of which cervical is the most common. Two viral oncoproteins, E6 and E7, contribute directly towards the development and maintenance of malignancy. A characteristic feature of the E6 oncoproteins from cancer-causing HPV types is the presence of a PDZ binding motif (PBM) at its C-terminus, which confers interaction with cellular proteins harbouring PDZ domains. Here we show that this motif allows E6 interaction with Sorting Nexin 27 (SNX27), an essential component of endosomal recycling pathways. This interaction is highly conserved across E6 proteins from multiple high-risk HPV types and is mediated by a classical PBM-PDZ interaction but unlike many E6 targets, SNX27 is not targeted for degradation by E6. Rather, in HPV-18 positive cell lines the association of SNX27 with components of the retromer complex and the endocytic transport machinery is altered in an E6 PBM-dependent manner. Analysis of a SNX27 cargo, the glucose transporter GLUT1, reveals an E6-dependent maintenance of GLUT1 expression and alteration in its association with components of the endocytic transport machinery. Furthermore, knockdown of E6 in HPV-18 positive cervical cancer cells phenocopies the loss of SNX27, both in terms of GLUT1 expression levels and its vesicular localization, with a concomitant marked reduction in glucose uptake, whilst loss of SNX27 results in slower cell proliferation in low nutrient conditions. These results demonstrate that E6 interaction with SNX27 can alter the recycling of cargo molecules, one consequence of which is modulation of nutrient availability in HPV transformed tumour cells.

Citing Articles

HPV-18 E6 enhances the interaction between EMILIN2 and SNX27 to promote WNT signaling.

Broniarczyk J, Trejo-Cerro O, Massimi P, Kavcic N, Myers M, Banks L J Virol. 2024; 98(7):e0073524.

PMID: 38874360 PMC: 11265340. DOI: 10.1128/jvi.00735-24.


HPV16 E7 modulates the cell surface expression of MET and CD109 via the AP2 complex.

Trejo-Cerro O, Basukala O, Myers M, Banks L Tumour Virus Res. 2024; 17:200279.

PMID: 38485055 PMC: 10958106. DOI: 10.1016/j.tvr.2024.200279.


Additive energetic contributions of multiple peptide positions determine the relative promiscuity of viral and human sequences for PDZ domain targets.

Tahti E, Blount J, Jackson S, Gao M, Gill N, Smith S Protein Sci. 2023; 32(4):e4611.

PMID: 36851847 PMC: 10022582. DOI: 10.1002/pro.4611.


Additive energetic contributions of multiple peptide positions determine the relative promiscuity of viral and human sequences for PDZ domain targets.

Tahti E, Blount J, Jackson S, Gao M, Gill N, Smith S bioRxiv. 2023; .

PMID: 36711692 PMC: 9881875. DOI: 10.1101/2022.12.31.522388.


HPV-18E6 Inhibits Interactions between TANC2 and SNX27 in a PBM-Dependent Manner and Promotes Increased Cell Proliferation.

Broniarczyk J, Massimi P, Trejo-Cerro O, Myers M, Banks L J Virol. 2022; 96(22):e0136522.

PMID: 36326272 PMC: 9683006. DOI: 10.1128/jvi.01365-22.


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