Abstract
BackgroundCidofovir (CDV) proved efficacious in treatment of human papillomaviruses (HPVs) hyperplasias. Antiproliferative effects of CDV have been associated with apoptosis induction, S-phase accumulation, and increased levels of tumor suppressor proteins. However, the molecular mechanisms for the selectivity and antitumor activity of CDV against HPV-transformed cells remain unexplained.MethodsWe evaluated CDV drug metabolism and incorporation into cellular DNA, in addition to whole genome gene expression profiling by means of microarrays in two HPV+ cervical carcinoma cells, HPV- immortalized keratinocytes, and normal keratinocytes.ResultsDetermination of the metabolism and drug incorporation of CDV into genomic DNA demonstrated a higher rate of drug incorporation in HPV+ tumor cells and immortalized keratinocytes compared to normal keratinocytes. Gene expression profiling clearly showed distinct and specific drug effects in the cell types investigated. Although an effect on inflammatory response was seen in all cell types, different pathways were identified in normal keratinocytes compared to immortalized keratinocytes and HPV+ tumor cells. Notably, Rho GTPase pathways, LXR/RXR pathways, and acute phase response signaling were exclusively activated in immortalized cells. CDV exposed normal keratinocytes displayed activated cell cycle regulation upon DNA damage signaling to allow DNA repair via homologous recombination, resulting in genomic stability and survival. Although CDV induced cell cycle arrest in HPV- immortalized cells, DNA repair was not activated in these cells. In contrast, HPV+ cells lacked cell cycle regulation, leading to genomic instability and eventually apoptosis.ConclusionsTaken together, our data provide novel insights into the mechanism of action of CDV and its selectivity for HPV-transformed cells. The proposed mechanism suggests that this selectivity is based on the inability of HPV+ cells to respond to DNA damage, rather than on a direct anti-HPV effect. Since cell cycle control is deregulated by the viral oncoproteins E6 and E7 in HPV+ cells, these cells are more susceptible to DNA damage than normal keratinocytes. Our findings underline the therapeutic potential of CDV for HPV-associated malignancies as well as other neoplasias.
Highlights
Cidofovir (CDV) proved efficacious in treatment of human papillomaviruses (HPVs) hyperplasias
Metabolism and incorporation Since CDV has been suggested to be preferentially converted to its active diphosphate form (CDVpp) in HPV16+ cells [24], we investigated the metabolism of [5-3H]-CDV in HPV+ cervical carcinoma cells compared to HPV- immortalized keratinocytes and normal keratinocytes
No significant differences in the levels of the active metabolite (CDVpp), CDV-phosphocholine or CDV were observed between primary human keratinocytes (PHKs) and HPV+ tumor cells
Summary
Cidofovir (CDV) proved efficacious in treatment of human papillomaviruses (HPVs) hyperplasias. Human papillomaviruses (HPVs) are small doublestranded DNA viruses with a strict epithelial tropism. HPVs infect either mucosal or cutaneous surfaces causing a variety of diseases ranging from benign warts (lowrisk types) to malignant neoplasms, including cervical carcinoma and other anogenital cancers (high-risk types) [1]. Development of HPV-induced cancerous lesions is often accompanied by partial integration of the viral genome in the host cell DNA, resulting in conservation and stabilized expression of E6 and E7 oncoproteins [3]. Cell lines derived from cervical carcinomas do not produce HPV virions and only express the E6 and E7 oncoproteins [5,6]
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