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2.0 BACKGROUND AND RATIONALE 2.1 Cervical Cancer Etiology and Targets for Intervention Cervical cancer is one of the most common causes of cancer-related deaths in women worldwide. Implementation of widespread screening has created drastic improvements in the incidence of cervical cancer as well as significant decreases in mortality over the last 30 years. It is estimated that in 2011, there will be 12,710 women in the US diagnosed with cervical cancer and ultimately 4,290 women will die from the disease. Cervical cancer is unique in that there exists a well-defined pre-malignant phase, referred to as cervical dysplasia, which can be suspected on cytological examination (pap smear) of exfoliated cervical cells and confirmed on histological examination of cervical biopsy material. The pre-cancerous changes represent a spectrum of histological abnormalities or cervical intraepithelial neoplasia (CIN) ranging from CIN 1 (mild dysplasia) to CIN2 (moderate dysplasia) to CIN3 (severe dysplasia/ carcinoma in situ). The timeline of progression for CIN 3 to invasive cancer in untreated women averages between 8.1 and 12.6 years.The surgical treatment of cervical pre-cancerous is therapeutically efficacious. However, it is an invasive procedure which has been associated with fertility and obstetrical complications in reproductive aged women. An attractive alternative to an excisional or ablative procedure would be to utilize an agent which could be applied topically or taken by mouth to foster regression of cervical dysplasia. The use of natural, synthetic, or biologic chemical agents to reverse, suppress, or prevent carcinogenic progression is called chemoprevention. A prerequisite for cervical cancer is persistent infection by a high-risk human papillomavirus allowing viral gene products sufficient time with which to induce carcinogenesis through a generally well understood natural history. Cancer-associated HPV types encode three oncogenes, E5, E6 and E7, and the E6 and E7 proteins have a significant role in malignant transformation. E6 and E7 stimulate cell proliferation by interfering with the function of regulatory proteins in cells, including the tumor suppressors p53 and pRB. Co-expression of both E6 and E7 leads to indefinite proliferation and immortalization of keratinocytes and induces premalignant neoplasms. HPV-E5, a transmembrane protein, can activate PI3K-Akt signalling. The up-regulation of PI3K-Akt survival signaling protects HPV-16 E5-expressing cells from apoptosis induced by ultraviolet irradiation. The major transforming capability of HPV is dependent on E6 and E7. However, E5 is necessary for full activation of E7, and the induction of PI3K-Akt-dependent apoptotic inhibition by E5 contributes to E7-mediated oncogenesis. The work done to evaluate PI3K activity as a potential marker of CIN progression further supports the idea that this pathway is also up-regulated in pre-cancerous lesions. The catalytic subunit alpha of PI3K is expressed in non-invasive cervical lesions and has shown potential as a carcinogenesis-related marker for early intraepithelial lesion of the uterine cervix in cytology samples. Among other potential markers, PIK3CA showed a superior specificity to distinguish CIN3 from other groups. Yao et al 2008 showed that positive rates of PI3K and Akt were significantly lower in normal cervical epithelium and cervical intraepithelial neoplasia than in cervical carcinoma (0.0% and 42.9% vs. 69.7%, P<0.01; 10.0% and 52.4% vs. 75.0%,P<0.01). Specifically, PI3K/Akt activation increased with grade of dysplasia with invasive carcinoma having the highest activity. They also showed that expression of PI3K protein positively correlated to the expression of Akt protein(r=0.425, P<0.01). 2.2 Nelfinavir (NFV) Background Nelfinavir (NFV) induces cell cycle arrest, endoplasmic reticulum stress, autophagy, and apoptosis is cancer cells. As a protease inhibitor used in patients with HIV, NFV predominately targets proteases 1 and 2, but it is also known that part of the efficacy is due to selective inhibition of the proteosome. The pathogenecity of high risk HPV is dependent on expression of viral E6 proteins which inappropriately activate the 26S proteosome to degrade p53 and other cellular proteins that are detrimental to viral replication; specific HIV protease inhibitors can block the ability of HPV16 E6 to degrade p53 and selectively kill E6-dependent cervical carcinoma cells. Furthermore, HIV protease inhibitors have been shown to inhibit the PI3K/Akt signaling pathway with NFV being the most potent. NFV's mechanism of action involves decreasing Akt phosphorylation. In addition, at concentrations (micromolar) achievable in the serum of patients taking usual dosing of the drug (1250mg PO BID), Akt phosphorylation is inhibited. At our institution, we have shown that HPV-infected cervical cancer cells lines treated with NFV underwent apoptosis and decreased cell proliferation in a dose dependent manner. Furthermore, we have shown through a recent retrospective study that HIV-infected women with cervical dysplasia who were treated with protease inhibitors (PI), including NFV were more likely to regress than those not on a PI-containing regimen. Because PI3K/Akt is up-regulated in CIN2/3 and NFV has been shown to inhibit this pathway in HPV-infected cervical cancer cell lines, we aim to further evaluate the effectiveness of NFV as an intervention for CIN2/3 and correlate these findings with phospho-Akt levels in cervical tissue. Several intervention trials have been conducted in women with CIN using retinoids, ß-carotene, difluoromethylornithine, and indole-3- carbinol and over 300 women with CIN 3 were followed in these trials for one to 15 months while none of them developed invasive cervical cancer. Therefore, this proposed intervention trial of 24 weeks (6 months) duration should allow a safe evaluation of NFV as a potential agent for a future randomized Phase III trial. Development of a new drug for cancer treatment is expensive and time consuming. Repositioning of a drug which is already FDA approved for another indication allows for more rapid evaluation and potential implementation of a novel cancer therapy. NFV has been identified to have anti-cancer effects in vitro, and compared to other protease inhibitors it is more potent in causing cell death. NFV has over 10 years of safety and pharmacokinetic data in HIV-infected individuals. Standard dosing for the treatment of HIV is 1,250 mg PO BID, and this dose has demonstrated plasma concentrations in vivo which correlate with necessary concentrations of successful in vitro studies. Furthermore, evaluation of the standard dose offers the availability of commercially produced tablets, the known and acceptable side effect profile, and the ease of twice daily dosing. For these reasons NFV is an excellent candidate for repositioning as an intervention for cervical dysplasia, which can be quickly evaluated in this phase II clinical trial.