Systematic identification of interactions between host cell proteins and E7 oncoproteins from diverse human papillomaviruses

White, Elizabeth; Sowa, Mathew E.; Tan, Min; Jeudy, Sheila; Hayes, Sebastian; Santha, Sreevidya; Münger, Karl; Harper, J. Wade; Howley, Peter M.

doi:10.1073/pnas.1116776109

Cited by 191 publications

(254 citation statements)

References 49 publications

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“…The HPV types have also been grouped into mucosal or cutaneous types, based on their tropism for specific epithelial sites. Mucosal HPV types found preferentially in precancerous and cancerous lesions have been designated as 'high-risk' types and these include types 16,18,31,33,34,35,39,45,51,52,56,58,59, 66, 68, and 70. Mucosal HPVs found in benign genital warts and other non-malignant lesions are generally labeled as 'low-risk' types, the most important ones being HPV 6,11,42,43, and 44 [1,2].…”

Section: Human Papillomaviruses (Structure and Classification)mentioning

confidence: 99%

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Biology of Human Papillomavirus Infections in Head and Neck Carcinogenesis

Rautava

Syrjänen

2012

Head and Neck Pathol

123

135

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Section: Human Papillomaviruses (Structure and Classification)mentioning

confidence: 99%

“…The HPV E7 gene can immortalize human keratinocytes alone when expressed at high levels [for review see 24,34,35]. E7 protein of the low-risk HPV types also binds to pRb, although with lower affinity, but thus indicating its significance in transformation.…”

Section: Cell Transformation By Hpvsmentioning

confidence: 99%

Biology of Human Papillomavirus Infections in Head and Neck Carcinogenesis

Rautava

Syrjänen

2012

Head and Neck Pathol

123

135

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“…Different from other N-recognins, UBR4 does not have a known ubiquitylation domain (7), suggesting that the action mechanism of UBR4 in N-end rule degradation could be different from those of canonical N-recognins. Recent studies using cultured cells suggest that UBR4 plays a role in membrane morphogenesis and extracellular matrix-mediated cell survival and signaling (15), human papillomavirus (HPV) E7-mediated cellular immortalization (16)(17)(18), and migration and development of neurons (19).…”

mentioning

confidence: 99%

UBR box N-recognin-4 (UBR4), an N-recognin of the N-end rule pathway, and its role in yolk sac vascular development and autophagy

Tasaki

Kim

Zakrzewska

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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The N-end rule pathway is a proteolytic system in which destabilizing N-terminal residues of short-lived proteins act as degradation determinants (N-degrons). Substrates carrying N-degrons are recognized by N-recognins that mediate ubiquitylation-dependent selective proteolysis through the proteasome. Our previous studies identified the mammalian N-recognin family consisting of UBR1/ E3α, UBR2, UBR4/p600, and UBR5, which recognize destabilizing N-terminal residues through the UBR box. In the current study, we addressed the physiological function of a poorly characterized N-recognin, 570-kDa UBR4, in mammalian development. UBR4-deficient mice die during embryogenesis and exhibit pleiotropic abnormalities, including impaired vascular development in the yolk sac (YS). Vascular development in UBR4-deficient YS normally advances through vasculogenesis but is arrested during angiogenic remodeling of primary capillary plexus associated with accumulation of autophagic vacuoles. In the YS, UBR4 marks endoderm-derived, autophagy-enriched cells that coordinate differentiation of mesoderm-derived vascular cells and supply autophagy-generated amino acids during early embryogenesis. UBR4 of the YS endoderm is associated with a tissue-specific autophagic pathway that mediates bulk lysosomal proteolysis of endocytosed maternal proteins into amino acids. In cultured cells, UBR4 subpopulation is degraded by autophagy through its starvation-induced association with cellular cargoes destined to autophagic double membrane structures. UBR4 loss results in multiple misregulations in autophagic induction and flux, including synthesis and lipidation/activation of the ubiquitin-like protein LC3 and formation of autophagic double membrane structures. Our results suggest that UBR4 plays an important role in mammalian development, such as angiogenesis in the YS, in part through regulation of bulk degradation by lysosomal hydrolases. cardiovascular system | ubiquitin ligase

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“…These MS data were then analyzed with CompPASS (Comparative Proteomic Analysis Software Suite), which relies on an unbiased comparative approach for identifying high-confidence candidate-interacting proteins (HCIPs) (85). This technology has been successfully used to identify protein interactors among the hundreds of proteins typically identified in immunoprecipitation-MS experiments (5,12,72,73,95).…”

mentioning

confidence: 99%

Identification and Proteomic Analysis of Distinct UBE3A/E6AP Protein Complexes

Martínez-Noël

Galligan

Sowa

et al. 2012

Molecular and Cellular Biology

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113

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The E6AP ubiquitin ligase catalyzes the high-risk human papillomaviruses' E6-mediated ubiquitylation of p53, contributing to the neoplastic progression of cells infected by these viruses. Defects in the activity and the dosage of E6AP are linked to Angelman syndrome and to autism spectrum disorders, respectively, highlighting the need for precise control of the enzyme. With the exception of HERC2, which modulates the ubiquitin ligase activity of E6AP, little is known about the regulation or function of E6AP normally. Using a proteomic approach, we have identified and validated several new E6AP-interacting proteins, including HIF1AN, NEURL4, and mitogen-activated protein kinase 6 (MAPK6). E6AP exists as part of several different protein complexes, including the proteasome and an independent high-molecular-weight complex containing HERC2, NEURL4, and MAPK6. In examining the functional consequence of its interaction with the proteasome, we found that UBE3C (another proteasome-associated ubiquitin ligase), but not E6AP, contributes to proteasomal processivity in mammalian cells. We also found that E6 associates with the HERC2-containing high-molecular-weight complex through its binding to E6AP. These proteomic studies reveal a level of complexity for E6AP that has not been previously appreciated and identify a number of new cellular proteins through which E6AP may be regulated or functioning. E6AP was originally discovered as the cellular protein that mediates the binding of the E6 protein of the high-risk human papillomaviruses (HPVs) to the tumor suppressor p53 (35). Subsequently, E6AP was shown to catalyze the E6-dependent transfer of ubiquitin to p53, targeting it for degradation by the 26S proteasome. As such, E6AP was the first mammalian ubiquitin (Ub) ligase to be described (36,37,80).E6AP is a 100-kDa protein containing a conserved carboxyterminal domain spanning 350 amino acids, referred to as the HECT domain (homologous to E6AP carboxy terminus), that defines a family of E3 Ub ligases (34). This domain participates directly in the transfer of ubiquitin from an E2 ubiquitin-conjugating enzyme to a conserved cysteine residue through a thiolester bond (34). E6AP then directs the transfer of ubiquitin from this active-site cysteine to a lysine residue of an associated substrate. Replacement of the active-site cysteine with alanine renders E6AP unable to accept ubiquitin and therefore unable to catalyze the transfer of ubiquitin to the target protein. This C/A substitution mutant is inactive and functions in a dominant-negative (DN) manner (88). Three different isoforms of E6AP that are generated by differential splicing from the same gene have been described (98). These three isoforms differ in their amino-terminal sequences, and it is not yet known whether they differ in function or substrate specificity.The E6AP protein is encoded by the UBE3A gene located in an imprinted region on chromosome 15q11-q13. As a consequence of the imprinting, only the maternal UBE3A allele is expressed in certain areas of the br...

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Systematic identification of interactions between host cell proteins and E7 oncoproteins from diverse human papillomaviruses

Cited by 191 publications

References 49 publications

Biology of Human Papillomavirus Infections in Head and Neck Carcinogenesis

Biology of Human Papillomavirus Infections in Head and Neck Carcinogenesis

UBR box N-recognin-4 (UBR4), an N-recognin of the N-end rule pathway, and its role in yolk sac vascular development and autophagy

Identification and Proteomic Analysis of Distinct UBE3A/E6AP Protein Complexes

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