We examined how well the human papillomavirus (HPV) E6 oncogene can function in the absence of the E7 oncogene during the carcinogenic process in human keratinocytes using a common HPV variant strongly associated with cervical cancer: the AsianAmerican E6 variant (AAE6). This E6 variant is 20 times more frequently detected in cervical cancer than the prototype European E6 variant, as evidenced by independent epidemiological data. Using cell culture and cell-based functional assays, we assessed how this variant can perform crucial carcinogenesis steps compared to the prototype E6 variant. The ability to immortalize and transform primary human foreskin keratinocytes (PHFKs) to acquire resilient phenotypes and the ability to promote cell migration were evaluated. The immortalization capability was assayed based on population doublings, number of passages, surpassing mortality stages 1 and 2, human telomerase reverse transcriptase (hTERT) expression, and the ability to overcome G 1 arrest via p53 degradation. Transformation and migration efficiency were analyzed using a combination of functional cell-based assays. We observed that either AAE6 or prototype E6 proteins alone were sufficient to immortalize PHFKs, although AAE6 was more potent in doing so. The AAE6 variant protein alone pushed PHFKs through transformation and significantly increased their migration ability over that of the E6 prototype. Our findings are in line with epidemiological data that the AA variant of HPV16 confers an increased risk over the European prototype for cervical cancer, as evidenced by a superior immortalization, transformation, and metastatic potential.H uman papillomavirus (HPV) is a double-stranded DNA virus that infects epithelial keratinocytes. It is implicated in virtually all cervical cancers worldwide, with HPV16 being the most common high-risk type (76). Within the HPV16 type, variation occurs among the genomes, resulting in variants such as the European prototype (E), Asian-American (AA), African (Af), or Asian (As) (72). Epidemiological evidence suggests that the AA variant is more aggressive than other variants (3,6,63,70,71,75), particularly in the presence of the HPV16 E7 oncogene (51).Over the years, cellular immortalization has been defined in numerous ways. Landmark publications in 1989 defined immortalization as simply an extension of life span (21,29,43). On this basis, they showed that both the E6 and E7 oncogenes cooperated to accomplish immortalization of keratinocytes. This established that the E6 and E7 oncogenes were the cause of cellular immortalization in HPV16-positive primary human keratinocytes (PHKs) (21,29,43).Experimental methods in the late 1980s were suboptimal as gene technology was rudimentary, but they have quickly evolved since then. In 1990, amphotropic, high-titer virus technology was developed for the purpose of transducing PHKs (42); this mimicked conditions occurring in vivo through the natural infection process. As more research was conducted over the course of time, the process of cell imm...
