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Genetic variations in the DNA replication origins of human papillomavirus family correlate with their oncogenic potential
Authors:Gulden Yilmaz  Esther E Biswas-Fiss  Subhasis B Biswas
Institution:1. Department of Molecular Biology, Rowan University, Stratford, NJ 08084, United States;2. Department of Medical Laboratory Sciences, College of Health Sciences, University of Delaware, Newark, DE 19716, United States
Abstract:Human papillomaviruses (HPVs) encompass a large family of viruses that range from benign to highly carcinogenic. The crucial differences between benign and carcinogenic types of HPV remain unknown, except that the two HPV types differ in the frequency of DNA replication. We have systematically analyzed the mechanism of HPV DNA replication initiation in low-risk and high-risk HPVs. Our results demonstrate that HPV-encoded E2 initiator protein and its four binding sites in the replication origin play pivotal roles in determining the destiny of the HPV-infected cell. We have identified strain-specific single nucleotide variations in E2 binding sites found only in the high-risk HPVs. We have demonstrated that these variations result in attenuated formation of the E2-DNA complex. E2 binding to these sites is linked to the activation of the DNA replication origin as well as initiation of DNA replication. Both electrophoretic mobility shift assay and atomic force microscopy studies demonstrated that binding of E2 from either low- or high-risk HPVs with variant binding sequences lacked multimeric E2-DNA complex formation in vitro. These results provided a molecular basis of differential DNA replication in the two types of HPVs and pointed to a correlation with the development of cancer.
Keywords:HPV  human papillomavirus  BS1  E2 binding site 1  BS2  E2 binding site 2  BS3  E2 binding site 3  BS4  E2 binding site 4  C1  complex 1  C2  complex 2  C3  complex 3  EMSA  electrophoretic mobility shift assay  D  dissociation constant  SNV  single nucleotide variation  DNA binding protein  DNA replication  Viral DNA replication  Viral protein  Single-nucleotide variation
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