The tumor suppressing roles of tissue structure in cervical cancer development

dc.contributor.advisorQuilliam, Lawrence
dc.contributor.authorNguyen, Hoa Bich
dc.contributor.otherBrutkiewicz, Randy R.
dc.contributor.otherHarrington, Maureen A.
dc.contributor.otherKapur, Reuben
dc.contributor.otherWells, Clark D.
dc.date.accessioned2013-10-07T19:46:10Z
dc.date.available2014-10-08T09:30:25Z
dc.date.issued2012-12
dc.degree.date2012en_US
dc.degree.disciplineDepartment of Biochemistry & Molecular Biologyen
dc.degree.grantorIndiana Universityen_US
dc.degree.levelPh.D.en_US
dc.descriptionIndiana University-Purdue University Indianapolis (IUPUI)en_US
dc.description.abstractCervical cancer is caused by the persistent infection of human papilloma virus (HPV) in the cervix epithelium. Although effective preventative care is available, the widespread nature of infection and the variety of HPV strains unprotected by HPV vaccines necessitate a better understanding of the disease for development of new therapies. A major tumor suppressing mechanism is the inhibition of cell division by tissue structure; however, the underlining molecular circuitry for this regulation remains unclear. Recently, the Yap transcriptional co-activator has emerged as a key growth promoter that mediates contact growth arrest and limits organ size. Thus, we aimed to uncover upstream signals that connect tissue organization to Yap regulation in the inhibition of cervical cancer. Two events that disrupt tissue structure were examined including the loss of the tumor suppressor LKB1 and the expression of the viral oncogene HPV16-E6. We identified that Yap mediates cell growth regulation downstream of both LKB1 and E6. Restoration of LKB1 expression in HeLa cervical cancer cells, which lack this tumor suppressor, or shRNA knockdown of LKB1 in NTERT immortalized normal human dermal keratinocytes, demonstrated that LKB1 promotes Yap phosphorylation, nuclear exclusion, and proteasomal degradation. The ability of phosphorylation-defective Yap mutants to rescue LKB1 phenotypes, such as reduced cell proliferation and cell size, suggest that Yap inhibition contributes to LKB1 tumor suppressor function(s). Interestingly, LKB1’s suppression of Yap activity required neither the canonical Yap kinases, Lats1/2, nor metabolic downstream targets of LKB1, AMPK and mTORC1. Instead, the scaffolding protein NF2 was required for LKB1 to induce a specific actin cytoskeleton structure that associates with Yap suppression. Meanwhile, HPV16-E6 promoted Yap activation in all stages of keratinocyte differentiation. E6 activated the Rap1 small GTPase, which in turn promoted Yap activity. Since Rap1 does not mediate differentiation inhibition caused by E6, E6 may play a role in promoting cell growth through Rap1-Yap activation rather than preventing growth arrest through the disruption of differentiation. Altogether, the LKB1-NF2-Yap and E6-Rap1-Yap pathways represent two examples of a novel phenomenon, whereby the structure of a cell directly influences its gene expression and proliferation.en_US
dc.identifier.urihttps://hdl.handle.net/1805/3627
dc.identifier.urihttp://dx.doi.org/10.7912/C2/1868
dc.language.isoen_USen_US
dc.subjectCervical canceren_US
dc.subjectYapen_US
dc.subjectLKB1en_US
dc.subjectHPV-E6en_US
dc.subjectNF2en_US
dc.subjecttissue structureen_US
dc.subject.lcshPapillomaviruses -- Researchen_US
dc.subject.lcshCervix uteri -- Canceren_US
dc.subject.lcshTumor suppressor proteinsen_US
dc.subject.lcshCells -- Growth -- Regulationen_US
dc.subject.lcshCell proliferation -- Researchen_US
dc.subject.lcshPapillomavirus vaccinesen_US
dc.subject.lcshPhosphorylationen_US
dc.subject.lcshTranscription factorsen_US
dc.subject.lcshDysplasiaen_US
dc.subject.lcshKeratinocytes -- Differentiationen_US
dc.subject.lcshCancer cells -- Researchen_US
dc.titleThe tumor suppressing roles of tissue structure in cervical cancer developmenten_US
dc.typeThesisen
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