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Literature DB >> 26912611

Domain Organization of Vaccinia Virus Helicase-Primase D5.

Stephanie Hutin¹, Wai Li Ling¹, Adam Round^2,3, Gregory Effantin¹, Stefan Reich², Frédéric Iseni⁴, Nicolas Tarbouriech¹, Guy Schoehn¹, Wim Pascal Burmeister⁵.

Abstract

UNLABELLED: Poxviridae are viruses with a large linear double-stranded DNA genome coding for up to 250 open reading frames and a fully cytoplasmic replication. The double-stranded DNA genome is covalently circularized at both ends. Similar structures of covalently linked extremities of the linear DNA genome are found in the African swine fever virus (asfarvirus) and in the Phycodnaviridae We are studying the machinery which replicates this peculiar genome structure. From our work with vaccinia virus, we give first insights into the overall structure and function of the essential poxvirus virus helicase-primase D5 and show that the active helicase domain of D5 builds a hexameric ring structure. This hexamer has ATPase and, more generally, nucleoside triphosphatase activities that are indistinguishable from the activities of full-length D5 and that are independent of the nature of the base. In addition, hexameric helicase domains bind tightly to single- and double-stranded DNA. Still, the monomeric D5 helicase construct truncated within the D5N domain leads to a well-defined structure, but it does not have ATPase or DNA-binding activity. This shows that the full D5N domain has to be present for hexamerization. This allowed us to assign a function to the D5N domain which is present not only in D5 but also in other viruses of the nucleocytoplasmic large DNA virus (NCLDV) clade. The primase domain and the helicase domain were structurally analyzed via a combination of small-angle X-ray scattering and, when appropriate, electron microscopy, leading to consistent low-resolution models of the different proteins. IMPORTANCE: Since the beginning of the 1980s, research on the vaccinia virus replication mechanism has basically stalled due to the absence of structural information. As a result, this important class of pathogens is less well understood than most other viruses. This lack of information concerns in general viruses of the NCLDV clade, which use a superfamily 3 helicase for replication, as do poxviruses. Here we provide for the first time information about the domain structure and DNA-binding activity of D5, the poxvirus helicase-primase. This result not only refines the current model of the poxvirus replication fork but also will lead in the long run to a structural basis for antiviral drug design.

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Year: 2016 PMID： 26912611 PMCID： PMC4836322 DOI： 10.1128/JVI.00044-16

Source DB: PubMed Journal: J Virol ISSN： 0022-538X Impact factor: 5.103

34 in total

1. EMAN: semiautomated software for high-resolution single-particle reconstructions.

Authors: S J Ludtke; P R Baldwin; W Chiu
Journal: J Struct Biol Date: 1999-12-01 Impact factor: 2.867

2. Genome-wide analysis of vaccinia virus protein-protein interactions.

Authors: S McCraith; T Holtzman; B Moss; S Fields
Journal: Proc Natl Acad Sci U S A Date: 2000-04-25 Impact factor: 11.205

3. Accurate determination of local defocus and specimen tilt in electron microscopy.

Authors: Joseph A Mindell; Nikolaus Grigorieff
Journal: J Struct Biol Date: 2003-06 Impact factor: 2.867

4. UCSF Chimera--a visualization system for exploratory research and analysis.

Authors: Eric F Pettersen; Thomas D Goddard; Conrad C Huang; Gregory S Couch; Daniel M Greenblatt; Elaine C Meng; Thomas E Ferrin
Journal: J Comput Chem Date: 2004-10 Impact factor: 3.376

5. The 1.2-megabase genome sequence of Mimivirus.

Authors: Didier Raoult; Stéphane Audic; Catherine Robert; Chantal Abergel; Patricia Renesto; Hiroyuki Ogata; Bernard La Scola; Marie Suzan; Jean-Michel Claverie
Journal: Science Date: 2004-10-14 Impact factor: 47.728

6. Mechanism of DNA translocation in a replicative hexameric helicase.

Authors: Eric J Enemark; Leemor Joshua-Tor
Journal: Nature Date: 2006-07-20 Impact factor: 49.962

Review 7. Evolutionary genomics of nucleo-cytoplasmic large DNA viruses.

Authors: Lakshminarayan M Iyer; S Balaji; Eugene V Koonin; L Aravind
Journal: Virus Res Date: 2006-02-21 Impact factor: 3.303

8. Structure of the replicative helicase of the oncoprotein SV40 large tumour antigen.

Authors: Dawei Li; Rui Zhao; Wayne Lilyestrom; Dahai Gai; Rongguang Zhang; James A DeCaprio; Ellen Fanning; Andrzej Jochimiak; Gerda Szakonyi; Xiaojiang S Chen
Journal: Nature Date: 2003-05-29 Impact factor: 49.962

Review 9. Phycodnaviridae--large DNA algal viruses.

Authors: J L Van Etten; M V Graves; D G Müller; W Boland; N Delaroque
Journal: Arch Virol Date: 2002-08 Impact factor: 2.574

10. Origin and evolution of the archaeo-eukaryotic primase superfamily and related palm-domain proteins: structural insights and new members.

Authors: Lakshminarayan M Iyer; Eugene V Koonin; Detlef D Leipe; L Aravind
Journal: Nucleic Acids Res Date: 2005-07-15 Impact factor: 16.971

12 in total

10. Global ubiquitination analysis reveals extensive modification and proteasomal degradation of cowpox virus proteins, but preservation of viral cores.

Authors: Marica Grossegesse; Joerg Doellinger; Annemarie Fritsch; Michael Laue; Janett Piesker; Lars Schaade; Andreas Nitsche
Journal: Sci Rep Date: 2018-01-29 Impact factor: 4.379

Domain Organization of Vaccinia Virus Helicase-Primase D5.

1. EMAN: semiautomated software for high-resolution single-particle reconstructions.

2. Genome-wide analysis of vaccinia virus protein-protein interactions.

3. Accurate determination of local defocus and specimen tilt in electron microscopy.

4. UCSF Chimera--a visualization system for exploratory research and analysis.

5. The 1.2-megabase genome sequence of Mimivirus.

6. Mechanism of DNA translocation in a replicative hexameric helicase.

Review 7. Evolutionary genomics of nucleo-cytoplasmic large DNA viruses.

8. Structure of the replicative helicase of the oncoprotein SV40 large tumour antigen.

Review 9. Phycodnaviridae--large DNA algal viruses.

10. Origin and evolution of the archaeo-eukaryotic primase superfamily and related palm-domain proteins: structural insights and new members.

Review 1. Poxvirus uracil-DNA glycosylase-An unusual member of the family I uracil-DNA glycosylases.

2. An in vitro fluorescence based study of initiation of RNA synthesis by influenza B polymerase.

3. Online ion-exchange chromatography for small-angle X-ray scattering.

Review 4. The French Armed Forces Virology Unit: A Chronological Record of Ongoing Research on Orthopoxvirus.

5. The vaccinia virus DNA polymerase structure provides insights into the mode of processivity factor binding.

6. Online Size-exclusion and Ion-exchange Chromatography on a SAXS Beamline.

Review 7. In vitro methods for testing antiviral drugs.

8. A novel DNA primase-helicase pair encoded by SCCmec elements.

9. Replication and transcription machinery for ranaviruses: components, correlation, and functional architecture.

10. Global ubiquitination analysis reveals extensive modification and proteasomal degradation of cowpox virus proteins, but preservation of viral cores.