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CK2 Phosphorylation of Human Papillomavirus 16 E2 on Serine 23 Promotes Interaction with TopBP1 and Is Critical for E2 Interaction with Mitotic Chromatin and the Viral Life Cycle

MBio. 2021-09; 
Apurva T Prabhakar, Claire D James, Dipon Das, Raymonde Otoa, Matthew Day, John Burgner, Christian T Fontan, Xu Wang, Sarah H Glass, Andreas Wieland, Mary M Donaldson, Molly L Bristol, Renfeng Li, Anthony W Oliver, Laurence H Pearl, Brian O Smith, Iain M Morgan
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Gene Synthesis pS23-Ab (1:10,000) (custom generated by GenScript Get A Quote

摘要

During the human papillomavirus 16 (HPV16) life cycle, the E2 protein interacts with host factors to regulate viral transcription, replication, and genome segregation/retention. Our understanding of host partner proteins and their roles in E2 functions remains incomplete. Here we demonstrate that CK2 phosphorylation of E2 on serine 23 promotes interaction with TopBP1 and and that E2 is phosphorylated on this residue during the HPV16 life cycle. We investigated the consequences of mutating serine 23 on E2 functions. E2-S23A (E2 with serine 23 mutated to alanine) activates and represses transcription identically to E2-WT (wild-type E2), and E2-S23A is as efficient as E2-WT in transient replication assays. Howev... More

關(guān)鍵詞

BRD4, CK2, E2, TopBP1, assay, cervical cancer, head and neck cancer, human papillomavirus, life cycle, papillomavirus, phosphorylation
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