Unique variants of human papillomavirus genotypes 52 and 58 and risk of cervical neoplasia

Chang, Yu-Hao; Chen, Hui‐Chi; Lee, Bor-Heng; You, San–Lin; Lin, Chien Ju; Pan, Mei‐Hung; Chou, Yi-Chun; Hsieh, Chang‐Yao; Chen, Yi-Ming A.; Cheng, Yiping; Chen, Chien-Jen

doi:10.1002/ijc.25724

Cited by 46 publications

(62 citation statements)

References 33 publications

(70 reference statements)

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“…The E6 K93R variant in our construct is present in 98% of the HPV52-positive cervical cancers in Japan (39,40,56) and has been significantly associated with an increased CIN2/3 risk, suggesting that it represents a carcinogenic variant (57), yet the findings that p53 expression levels were unaltered and immortalization was unsuccessful in our hands indicate that this highly common variant is not as oncogenic as other hrHPV types, at least in a Caucasian genetic background. HPV59, which is less prevalent in invasive cervical cancers (7), showed a better immortalization capacity.…”

Section: Discussionmentioning

confidence: 70%

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Differential In Vitro Immortalization Capacity of Eleven, Probable High-Risk Human Papillomavirus Types

Schütze

Snijders

Bosch

et al. 2014

J Virol

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bEpidemiological studies identified 12 high-risk HPV (hrHPV) types and 8 probable/possible hrHPV types that display different cancer risks. Functional studies on transforming properties of hrHPV are mainly limited to HPV16 and -18, which induce immortalization of human foreskin keratinocytes (HFKs) by successive bypass of two proliferative life span barriers, senescence and crisis. Here, we systematically compared the in vitro immortalization capacities, as well as influences on p53, pRb, hTERT, growth behavior, and differentiation capacity, of nine hrHPV types (HPV16, -18, -31, -33, -35, -45, -51, -52, and -59), and two probable hrHPV types (HPV66 and -70). By retroviral transduction, the respective E6/E7 coding sequences were expressed in HFKs from two or three independent donors. Reduced p53 levels and low-level hTERT expression in early-passage cells, as seen in HPV16-, -31-, -33-, and -35-, and to a lesser extent HPV18-transduced HFKs, was associated with continuous growth and an increased immortalization capacity. Less frequent immortalization by HPV45 and -51 and immortalization by HPV66 and -70 was preceded by an intervening period of strongly reduced growth (crisis) without prior increase in hTERT expression. Immortalization by HPV59 was also preceded by a period crisis, despite the onset of low hTERT expression at early passage. HPV52 triggered an extended life span but failed to induce immortality. Variations in p53 and pRb levels were not correlated with differences in alternative E6/E7 mRNA splicing in all hrHPV-transduced HFKs. On collagen rafts, transductants showed disturbed differentiation reminiscent of precancerous lesions. In conclusion, in vitro oncogenic capacities differ between the established hrHPV types, and both some established and probable hrHPV types display weak or moderate immortalization potential. C ervical cancer, the third most common cancer among women worldwide, is caused by a persistent infection with certain types of human papillomavirus (HPV) (1, 2). Most HPV infections are transient and are cleared within 1 to 2 years. However, a fraction of infections eventually give rise to either squamous cell carcinoma (SCC) or adenocarcinoma (AdCA) of the cervix. SCCs develop from so-called cervical intraepithelial neoplasia (CIN) precursor lesions. Low-grade CIN lesions (CIN1) mostly reflect a productive infection in which viral replication and virion production are linked to the differentiation program of the epithelium. High-grade CIN lesions (CIN2/3) mainly represent transforming infections and are characterized by deregulated expression of the early viral E6 and E7 genes in the proliferating basal cells of the epithelium (3, 4).HPV types belonging to the alpha (␣) genus can infect the cervical mucosa (5) and are classified into low-risk (lrHPV) and high-risk (hrHPV) HPV based on their association with malignancy (6). Infections with lrHPV types, e.g., HPV type 6 (HPV6) and HPV11, are associated with benign warts or low-grade lesions, whereas infections with hrHPV can give rise ...

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Section: Discussionmentioning

confidence: 70%

“…HPV52 was also amplified from a full-length HPV plasmid and contained a sequence variation in E6 (K93R). This HPV52 variant has frequently been detected in cervical cancers in Asia (39,40). HPV51 and HPV59 E6/E7 were cloned from cervical scrapes, and HPV70 was cloned from a tumor sample.…”

Section: Generation Of Hpv E6/e7-transduced Hfksmentioning

confidence: 99%

Differential In Vitro Immortalization Capacity of Eleven, Probable High-Risk Human Papillomavirus Types

Schütze

Snijders

Bosch

et al. 2014

J Virol

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“…It is worth noticing that this cited study included 2 samples from Mexico. They hypothesized that lineage A (probably sublineage A2) was the oldest lineage, which disseminated with early human evolution and assigned A1 to the sublineage that contained the prototype, being rarely detected except in Asia [38]. The geographical origin of the sequences shows a somehow even distribution of the Yucatan sequences along the trees obtained; all sequences were A lineage in E6 and E7, and a large proportion closely related to A1 sublineage.…”

Section: Doi: 101159/000489306mentioning

confidence: 99%

“…In contrast to HPV16 geographic definition of the variants, and their more convincing association with disease (reviewed by Burk et al [30]), in the case of HPV58, the studies have been complicated by the heterogeneity of the sequences and their distribution worldwide [29,38,39].…”

Section: Doi: 101159/000489306mentioning

confidence: 99%

“…Calleja-Macias et al [22] analyzed the LCR region and defined 21 variants without any geographical association. Later, a study by Chan et al [38] used concatenated sequences of E6-E7-E2-E5-L1-LCR showing a limited geographic correlation for HPV-58 lineages distribution, where lineage A was the most generally distributed, with sublineages A1, and A3 present in higher frequencies in Asia, while sublineage A2 was more predominant in Africa, the Americas, and, Europe. It is worth noticing that this cited study included 2 samples from Mexico.…”

Section: Doi: 101159/000489306mentioning

confidence: 99%

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Genetic Variability in E6 and E7 Oncogenes from Human Papillomavirus Type 58 in Mexican Women

et al. 2017

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Background/Aims: The study aimed to describe human papillomavirus (HPV) 58 genetic variability in E6 and E7 oncogenes from women in southeast Mexico and their phylogenetic relationships with the sequences from other geographical regions. Methods: The E6-E7 region was amplified by nested PCR, and sequenced for identification of polymorphisms, phylogenetic trees construction, and haplotype and fixation tests. Results: HPV58 positive samples were obtained from a repository, 54 were amplified, 47 sequences for the E6 gene, and 51 sequences for the E7 gene were obtained. Fifteen new E6 mutations were found; the most frequent were G279T (G57V; 29.78%), T249G (F47C; 34.04%), and A270G (Y54C; 34.04%), and previously reported c307t (63.82%). For E7, 17 known mutations were found, the most frequent were C632T (T20I), 35.30%, G760A (G63S), 35.30%, and t744g 74.50%. No significant association with the severity of the lesions was found. The polytomy in the E6 tree did not allow proposing phylogenetic relationship, and E7 tree presented defined branches. All sequences were presumably A lineage, most closely related to A1 and/or A3 sublineage. HPV58 variants are not specific for a geographical area. Population and fixation analyses suggest a possible Asian origin of HPV58 from Yucatan. The most frequent E7 haplotype in Yucatan groups with other populations of the world. Conclusion: The genetic variability of HPV58 from Mexico was described for the first time. E7 was more conserved than E6. New mutants present exclusively in Yucatan were identified.

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Human papillomavirus type 52 polymorphism and high‐grade lesions of the uterine cervix

Formentin

Archambault

Koushik

et al. 2012

Intl Journal of Cancer

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The association between polymorphism of human papillomavirus type 52 (HPV52) and high-grade cervical intraepithelial neoplasia (CIN2,3) was investigated in Canadian women. HPV-52-positive endocervical specimens collected from 216 women selected from a total of 3,614 participants recruited in two case-control and two cohort studies conducted in Canada, were further analyzed by PCR-sequencing of the LCR and E6 gene. Overall, the HPV52 LCR prototype was detected more frequently in Caucasian women (69 of 132, 52.3%, 95% confidence interval (CI): 43.8%-60.6%) than in non-Caucasian women (15 of 48, 31.3%, 95% CI 19.9%-45.4%). In two cohort studies, HPV52 prototype was detected in seven of 15 (46.7%, 95% CI 24.8-69.9) HPV52 persistent infections and 14 of 35 (40.0%, 95% CI 25.5-56.5) transient infections (p = 0.76). In two case-control studies, 30 participants did not have CIN, 18 had low-grade CIN (CIN1), 64 had CIN2,3, seven had cervical cancer and the diagnosis was undefined for 27 women. Variant MTL-52-LCR-02 was detected more frequently in women with cancer (28.6%, 95% CI 7.6%-64.8%) than in women without cancer or CIN2,3 (0%, 95% CI 0.0%-9.2%; p = 0.015). CIN2,3 risk was significantly associated with a deletion at nucleotide position 7695 in the LCR (OR 4.9, 95% CI 1.2-20.8), the T7744C variation in the LCR (OR 5.7, 95% CI 1.1-32.0), and the K93R variation in E6 (OR 6.9, 95% CI 1.3-36.8), after adjusting for age, detection of HPV16 or 18 and study site. These findings indicate that HPV52 polymorphism influences risk of CIN-2,3 and possibly invasive cancer.

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Unique variants of human papillomavirus genotypes 52 and 58 and risk of cervical neoplasia

Cited by 46 publications

References 33 publications

Differential In Vitro Immortalization Capacity of Eleven, Probable High-Risk Human Papillomavirus Types

Differential In Vitro Immortalization Capacity of Eleven, Probable High-Risk Human Papillomavirus Types

Genetic Variability in E6 and E7 Oncogenes from Human Papillomavirus Type 58 in Mexican Women

Human papillomavirus type 52 polymorphism and high‐grade lesions of the uterine cervix

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