Study of the carcinogenic potential of the E6 protein of human papillomavirus type 16

dc.contributor.authorCabiles, Dana Rose
dc.contributor.examiningcommitteeMeyers, Adrienne (Medical Microbiology) Drebot, Mike (Medical Microbiology) Mowat, Michael (Biochemistry & Medical Genetics)en_US
dc.contributor.supervisorSeverini, Alberto (Medical Microbiology)en_US
dc.date.accessioned2014-03-25T13:38:22Z
dc.date.available2014-03-25T13:38:22Z
dc.date.issued2014-03-25
dc.degree.disciplineMedical Microbiologyen_US
dc.degree.levelMaster of Science (M.Sc.)en_US
dc.description.abstractWhile most Human papillomavirus (HPV) infections are asymptomatic and self-resolved, high-risk types, such as HPV-16 and HPV-18 are responsible for 99% of cervical cancers worldwide, whereas low-risk types, such as HPV-6 and HPV-11, are responsible for 90% of genital warts. While the different types of HPV and their varying oncogenicities have been studied extensively, it is still not clear what features of a HPV type make it more oncogenic than another. Two aspects which could affect the oncogenicity of HPV were studied: HPV variants and the E6 protein’s interaction with membrane associated guanylate kinase (MAGUK) proteins. Previous studies have shown that some HPV-16 variants may be more oncogenic than others. The first goal of this work was to characterise the HPV-16 variants in a Manitoba cervical cancer sample population to possibly identify mutations which could be associated with an increased risk of developing cervical cancer. Seventy-five samples from different individuals were sequenced in three distinct regions: the long control region and the E6 and E7 open reading frames. The DNA sequences obtained from these genomic regions were then compared between HPV-16 cervical cancer samples and Manitoba HPV-16 non cancer samples to identify any mutations that were exclusive to the cervical cancer samples. No specific mutations in any of the regions could be associated with cervical cancer. It is also proposed that HPV16 E6 protein’s interaction with MAGUK proteins contributes to its oncogenicity since low-risk E6 proteins lack this ability. The second goal of this work was to investigate which regions of high-risk HPV E6 proteins are needed in order to achieve MAGUK protein degradation, more specifically MAGI-1 degradation. Wild-type high-risk HPV16E6, low-risk HPV6E6, as well as mutants, were synthesized and cloned into vectors. In vitro translated proteins were used in MAGI-1 degradation assays. The ability of both wild-type HPV6 and HPV16 E6 proteins to degrade MAGI-1 was confirmed. Based on the performance of the different mutants in these degradation assays, it was determined that the PDZ-binding domain is necessary but not sufficient to induce E6-induced MAGI-1 degradation. In conclusion, it was determined that the entire HPV16 E6 protein is needed for the induction of MAGI-1 degradation.en_US
dc.description.noteMay 2014en_US
dc.identifier.urihttp://hdl.handle.net/1993/23340
dc.language.isoengen_US
dc.rightsopen accessen_US
dc.subjectHuman Papillomavirusen_US
dc.subjectHPVen_US
dc.subjectMAGUKen_US
dc.subjectMAGI-1en_US
dc.titleStudy of the carcinogenic potential of the E6 protein of human papillomavirus type 16en_US
dc.typemaster thesisen_US
local.subject.manitobayesen_US
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