Complex of the herpes simplex virus type 1 origin binding protein UL9 with DNA as a platform for the design of a new type of antiviral drugs

Bazhulina, N. P.; Surovaya, A. N.; Gursky, Ya. G.; Андронова, В. Л.; Moiseeva, E. D.; Nikitin, Capital A Cyrillic M; Golovkin, M. V.; Ga, Galegov; Grokhovsky, S. L.; Gursky, G. V.

doi:10.1080/07391102.2013.820110

Cited by 6 publications

(1 citation statement)

References 63 publications

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“…таблицу и рис. 2) -с 14-16 АТ-парами оснований [18], благодаря чему обладает значительно большей DOI: http://dx.doi.org/10.18821/0507-4088-2018-63-4-149-159 RevIews лена безопасность ПТВ. Так как частый приём препарата не требуется (t 1/2 в плазме крови 80 ч.…”

Section: ингибиторы инициации репликации герпесвирусовunclassified

Modern Ethiotropic Chemotherapy of Herpesvirus Infections: Advances, New Trends and Perspectives. Alphaherpesviruses (Part Ii)

Андронова¹

2018

Problems of Virology

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A key role in the treatment of herpesviral infections is played by modified nucleosides and their predecessors - acyclovir, its L-valine ester (valaciclovir) and famciclovir (prodrug of penciclovir). The biological activity of compounds of this class is determined by their similarity to natural nucleosides. After phosphorylation by viral thymidine kinase and then cell enzymes to the triphosphate forms, acyclovir and penciclovir inhibit the activity of viral DNA polymerase and synthesis of viral DNA. The increasing role of herpesvirus infections in human infectious pathology, as well as the development of drug resistance in viruses, mainly in patients with immunodeficiencies of various origins, necessitate the search for new compounds possessing anti-herpesvirus activity, using as a biological target not DNA polymerase, but other viral proteins and enzymes, unique or different from cellular proteins, performing similar functions.

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Section: ингибиторы инициации репликации герпесвирусовunclassified

Modern Ethiotropic Chemotherapy of Herpesvirus Infections: Advances, New Trends and Perspectives. Alphaherpesviruses (Part Ii)

Андронова¹

2018

Problems of Virology

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Antiviral and synergistic effects of photo-energy with acyclovir on herpes simplex virus type 1 infection

Oh,

Han,

Lim

et al. 2024

Virology

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Targeting Holliday junctions by origin DNA-binding protein of herpes simplex virus type 1

Moiseeva

Bazhulina

Gursky

et al. 2016

Journal of Biomolecular Structure and Dynamics

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In the present paper, the interactions of the origin binding protein (OBP) of herpes simplex virus type 1 (HSV1) with synthetic four-way Holliday junctions (HJs) were studied using electrophoresis mobility shift assay and the FRET method and compared with the interactions of the protein with duplex and single-stranded DNAs. It has been found that OBP exhibits a strong preference for binding to four-way and three-way DNA junctions and possesses much lower affinities to duplex and single-stranded DNAs. The protein forms three types of complexes with HJs. It forms complexes I and II which are reminiscent of the tetramer and octamer complexes with four-way junction of HJ-specific protein RuvA of Escherichia coli. The binding approaches saturation level when two OBP dimers are bound per junction. In the presence of Mg ions (≥2 mM) OBP also interacts with HJ in the stacked arm form (complex III). In the presence of 5 mM ATP and 10 mM Mg ions OBP catalyzes processing of the HJ in which one of the annealed oligonucleotides has a 3'-terminal tail containing 20 unpaired thymine residues. The observed preference of OBP for binding to the four-way DNA junctions provides a basis for suggestion that OBP induces large DNA structural changes upon binding to Box I and Box II sites in OriS. These changes involve the bending and partial melting of the DNA at A+T-rich spacer and also include the formation of HJ containing Box I and Box II inverted repeats and flanking DNA sequences.

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Complex of the herpes simplex virus type 1 origin binding protein UL9 with DNA as a platform for the design of a new type of antiviral drugs

Cited by 6 publications

References 63 publications

Modern Ethiotropic Chemotherapy of Herpesvirus Infections: Advances, New Trends and Perspectives. Alphaherpesviruses (Part Ii)

Modern Ethiotropic Chemotherapy of Herpesvirus Infections: Advances, New Trends and Perspectives. Alphaherpesviruses (Part Ii)

Antiviral and synergistic effects of photo-energy with acyclovir on herpes simplex virus type 1 infection

Targeting Holliday junctions by origin DNA-binding protein of herpes simplex virus type 1

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