A conserved C-terminal sequence of high-risk cutaneous beta-human papillomavirus E6 proteins alters localization and signalling of β1-integrin to promote cell migration

Holloway, Amy; Storey, Alan

doi:10.1099/vir.0.057695-0

Cited by 10 publications

(4 citation statements)

References 84 publications

(102 reference statements)

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“…A specific characteristic of the oncogenic mucosal HPV types is a PDZ-binding motif on the carboxyl terminus of E6, which is important in cell proliferation, cell polarity and cell transformation (Cavatorta et al, 2004). Although the PDZbinding domains were not found at the carboxyl terminus of the novel γ-PV types here described, it has been shown that the E6 proteins of some oncogenic β-PV types encode a conserved domain (YXDM) at the carboxyl terminus which alters the localization and signalling of the β1-integrin that was associated with increased cell migration, and therefore with a higher pathogenicity of these β-HPV types (Holloway and Storey, 2014). Binding partners and possible functions of the different conserved C-terminal motifs of the E6 proteins should be explored in order to investigate the pathological mechanism of some γ-PV types.…”

Section: Discussionmentioning

confidence: 84%

Characterization of novel human papillomavirus types 157, 158 and 205 from healthy skin and recombination analysis in genus γ-Papillomavirus

Bolatti

Chouhy

Casal

et al. 2016

Infection, Genetics and Evolution

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Section: Discussionmentioning

confidence: 84%

Characterization of novel human papillomavirus types 157, 158 and 205 from healthy skin and recombination analysis in genus γ-Papillomavirus

Bolatti

Chouhy

Casal

et al. 2016

Infection, Genetics and Evolution

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“…Hpv-positive NPC tends to have a poor prognosis [ 42 ]. It has been shown that the conserved C-terminal sequence of the E6 protein of high-risk cutaneous β-HPV promotes cell migration by altering β1-integrin localization and signaling, which may be involved in contributing to the pathogenicity of these β-HPV types [ 43 ].…”

Section: Discussionmentioning

confidence: 99%

Comprehensive pan-carcinoma analysis of ITGB1 distortion and its potential clinical significance for cancer immunity

Fei,

Wu,

Chen

et al. 2024

Discov Onc

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The human protein-coding gene ITGB1 (Integrin 1), also known as CD29, has a length of 58048 base pairs. The Integrin family's most prevalent subunit, it participates in the transmission of numerous intracellular signaling pathways. A thorough examination of ITGB1's functions in human malignancies, however, is inadequate and many of their relationships to the onset and development of human cancers remain unknown. In this work, we examined ITGB1's role in 33 human cancers. Finally, a multi-platform analysis revealed that three of the 33 malignancies had significantly altered ITGB1 expression in tumor tissues in comparison to normal tissues. In addition, it was discovered through survival analysis that ITGB1 was a stand-alone prognostic factor in a number of cancers. ITGB1 expression was linked to immune cell infiltration in colon cancer, according to an investigation of immune infiltration in pan-cancer. In the gene co-expression research, ITGB1 showed a positive connection with the majority of the cell proliferation and EMT indicators, indicating that ITGB1 may have an essential function in controlling cancer metastasis and proliferation. Our pan-cancer analysis of ITGB1 gives evidence in favor of a further investigation into its oncogenic function in various cancer types.

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“…Ultrastructural studies show integrin chains’ distribution in the basal cell layer of the squamous epithelium, which is crucial for the interaction between the epithelium and basal lamina [ 20 ]. The interactions between them can be altered during the first steps of dysplastic transformations that come before micro-invasive cervical cancer [ 21 , 22 , 23 ].…”

Section: Discussionmentioning

confidence: 99%

The Role of β1 Integrin/CD29 as a Potential Prognostic Factor for the Risk of Progression to Cervical Carcinoma in HPV-Associated Lesions

Schettino,

Preti,

Vietri

et al. 2024

Medicina

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Background and Objectives: Available evidence reports the overexpression of β1 integrin in dysplastic rather than normal cervical tissue. We aimed to evaluate the involvement of β1 (CD29) integrin in the progressive pathogenesis of cervical intraepithelial neoplasia (CIN). Materials and Methods: From January 2019 to December 2021, we prospectively enrolled women undergoing a colposcopy with a cervical biopsy for abnormal cervical cytology and/or undefined cytology with a positive HPV DNA test and women with relapsing cervical inflammatory disorders. Based on the histopathological results, women were divided into four groups: group A (CIN1), group B (CIN2), group C (CIN3), and group D (no CIN diagnosis) as a control group. Subsequently, cytofluorimetry and immunohistochemical analysis (based on the identified positive cell ratios as follows: ≤10%, negative; 10–25%, 1+ (weak); 25–50%, 2+ (medium); ≥50%, and 3+ (high)) for β1 integrin were carried out. Results: In total, 154 women were included. The average fluorescence intensity in the four groups was 2.35 ± 1.37, 2.73 ± 1.56, 3.09 ± 1.56, and 2.13 ± 1.25 UA from groups A to D, respectively; this figure was significantly different for CIN3 (group C) women relative to the other groups (p = 0.0132). Higher β1 integrin/CD29 concentrations in the CIN groups with HR-HPV 16 and 18 were also detected (p = 0.0292, 0.0367, and 0.0357 respectively for CIN3, CIN2, and CIN1). Immunohistochemistry analysis showed higher results for the CIN3 group compared to controls and all the other groups (p < 0.001). Conclusions: β1/CD29 integrin expression increased with CIN grade, and it was significantly higher in CIN3 lesions. This could be used as a promising screening tool to identify women prone to developing high-grade cervical lesions. However, additional evidence is needed to strengthen these findings.

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A conserved C-terminal sequence of high-risk cutaneous beta-human papillomavirus E6 proteins alters localization and signalling of β1-integrin to promote cell migration

Cited by 10 publications

References 84 publications

Characterization of novel human papillomavirus types 157, 158 and 205 from healthy skin and recombination analysis in genus γ-Papillomavirus

Characterization of novel human papillomavirus types 157, 158 and 205 from healthy skin and recombination analysis in genus γ-Papillomavirus

Comprehensive pan-carcinoma analysis of ITGB1 distortion and its potential clinical significance for cancer immunity

The Role of β1 Integrin/CD29 as a Potential Prognostic Factor for the Risk of Progression to Cervical Carcinoma in HPV-Associated Lesions

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