Herpes ICP8 protein stimulates homologous recombination in human cells

Valledor, Melvys; Myers, Richard S.; Schiller, Paul C.

doi:10.1101/259739

2018

DOI: 10.1101/259739

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Herpes ICP8 protein stimulates homologous recombination in human cells

Melvys Valledor

Richard S. Myers

Paul C. Schiller

Abstract: Recombineering has transformed functional genomic analysis. Genome modification by recombineering using the phage lambda Red SynExo homologous recombination proteins Beta in Escherichia coli has approached 100% efficiency. While highly efficient in E. coli, recombineering using the Red SynExo in other organisms declines in efficiency roughly correlating with phylogenetic distance from E. coli. SynExo recombinases are common to double-stranded DNA viruses infecting a variety of organisms, including humans. Huma… Show more

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“…The HSV exo/SSAP, composed of a 5′-to-3′ exonuclease (UL12) and an SSAP (ICP8), is capable of promoting strand exchange in vitro (25,26). More recently, we have shown that HSV infection stimulates single-strand annealing (27), and ICP8 has been reported to promote recombineering in transfected cells (28). However, these assays do not directly address the importance of the exo/SSAP during viral replication.…”

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Herpes simplex virus 1 ICP8 mutant lacking annealing activity is deficient for viral DNA replication

Weerasooriya

DiScipio

Darwish

et al. 2018

Proc. Natl. Acad. Sci. U.S.A.

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Most DNA viruses that use recombination-dependent mechanisms to replicate their DNA encode a single-strand annealing protein (SSAP). The herpes simplex virus (HSV) single-strand DNA binding protein (SSB), ICP8, is the central player in all stages of DNA replication. ICP8 is a classical replicative SSB and interacts physically and/or functionally with the other viral replication proteins. Additionally, ICP8 can promote efficient annealing of complementary ssDNA and is thus considered to be a member of the SSAP family. The role of annealing during HSV infection has been difficult to assess in part, because it has not been possible to distinguish between the role of ICP8 as an SSAP from its role as a replicative SSB during viral replication. In this paper, we have characterized an ICP8 mutant, Q706A/F707A (QF), that lacks annealing activity but retains many other functions characteristic of replicative SSBs. Like WT ICP8, the QF mutant protein forms filaments in vitro, binds ssDNA cooperatively, and stimulates the activities of other replication proteins including the viral polymerase, helicase–primase complex, and the origin binding protein. Interestingly, the QF mutant does not complement an ICP8-null virus for viral growth, replication compartment formation, or DNA replication. Thus, we have been able to separate the activities of ICP8 as a replicative SSB from its annealing activity. Taken together, our data indicate that the annealing activity of ICP8 is essential for viral DNA replication in the context of infection and support the notion that HSV-1 uses recombination-dependent mechanisms during DNA replication.

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mentioning

confidence: 99%

Herpes simplex virus 1 ICP8 mutant lacking annealing activity is deficient for viral DNA replication

Weerasooriya

DiScipio

Darwish

et al. 2018

Proc. Natl. Acad. Sci. U.S.A.

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Herpes ICP8 protein stimulates homologous recombination in human cells

Cited by 1 publication

References 45 publications

Herpes simplex virus 1 ICP8 mutant lacking annealing activity is deficient for viral DNA replication

Herpes simplex virus 1 ICP8 mutant lacking annealing activity is deficient for viral DNA replication

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