Inhibition of Human Cytomegalovirus pUL89 Terminase Subunit Blocks Virus Replication and Genome Cleavage

Wang, Yan; Mao, Lili; Kankanala, Jayakanth; Wang, Zhengqiang; Geraghty, Robert J.

doi:10.1128/jvi.02152-16

Cited by 23 publications

(43 citation statements)

References 31 publications

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“…Colored residues 463, 534, and 651 in the nuclease domain are involved in metal ion coordination (12). molecules may effectively target the UL89 nuclease domain independently of the terminase inhibitors studied here (15,16).…”

Section: Discussionmentioning

confidence: 99%

Comparison of Cytomegalovirus Terminase Gene Mutations Selected after Exposure to Three Distinct Inhibitor Compounds

Chou

2017

Antimicrob Agents Chemother

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Letermovir, GW275175X (a benzimidazole), and tomeglovir (Bay38-4766) are chemically unrelated human cytomegalovirus (CMV) terminase complex inhibitors that have been tested in human subjects. UL56 gene mutations are the dominant pathway of letermovir resistance, while UL89 and UL56 mutations are known to confer benzimidazole resistance. This study compares the mutations elicited by the three inhibitors during CMV propagation. GW275175X consistently selected for UL89 D344E and sometimes selected for UL89 C347S, UL89 R351H, or UL56 Q204R. Tomeglovir consistently selected for UL89 V362M and sometimes selected for UL89 N329S, T350M, H389N, or N405D or UL56 L208M, E407D, H637Q, or V639M. Adding to known and novel UL56 mutations, letermovir occasionally selected for UL89 N320H, D344E, or M359I. Recombinant phenotyping confirmed that UL89 D344E conferred 9-fold resistance (an increased 50% effective concentration [EC]) for GW275175X and increased the letermovir and tomeglovir ECs by 1.7- to 2.1-fold for the baseline virus and the UL56 Q204R, E237D, F261L, and M329T mutants. UL89 N320H and M359I conferred <2-fold letermovir resistance but 7-fold tomeglovir resistance; the N320H mutant was also 4-fold resistant to GW275175X. UL89 N329S conferred tomeglovir and letermovir cross-resistance. UL89 T350M conferred resistance to all three inhibitors. UL89 C347S conferred 27-fold GW275175X resistance. UL89 V362M and H389N conferred 98-fold and 29-fold tomeglovir resistance, respectively, without conferring cross-resistance. Thus, characteristic UL89 mutations confer substantial resistance to GW275175X and tomeglovir and are an uncommon accessory pathway of letermovir resistance. Instances of moderate cross-resistance and the proximity of the selected UL89 and UL56 mutations suggest targeting of a similar terminase functional locus involving UL56 and UL89 interaction.

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Section: Discussionmentioning

confidence: 99%

Comparison of Cytomegalovirus Terminase Gene Mutations Selected after Exposure to Three Distinct Inhibitor Compounds

Chou

2017

Antimicrob Agents Chemother

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“…WAY‐150138 showed modest activity (13 μM) against HCMV (Table ), but the CMV portal was not experimentally confirmed to be the target. Although no compounds currently target pUL104, several compounds have been described that prevent encapsidation by inhibiting the viral terminase . Letermovir, a CMV‐specific terminase inhibitor in late stage development, showed no cross resistance with viral strains resistant to currently available drugs and few side effects in clinical trials .…”

Section: Human Cytomegalovirusmentioning

confidence: 99%

“…The portal oligomer serves as a docking site for the encapsidation motor or terminase complex. Viral terminases possess ATPase and endonuclease activities and provide the necessary force to pack the increasingly rigid dsDNA into the capsid under pressure . DNA, though initially flexible, becomes semicrystalline as it fills the capsid .…”

Section: Introductionmentioning

confidence: 99%

Human herpesvirus portal proteins: Structure, function, and antiviral prospects

Kornfeind

Visalli

2018

Reviews in Medical Virology

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Herpesviruses (Herpesvirales) and tailed bacteriophages (Caudovirales) package their dsDNA genomes through an evolutionarily conserved mechanism. Much is known about the biochemistry and structural biology of phage portal proteins and the DNA encapsidation (viral genome cleavage and packaging) process. Although not at the same level of detail, studies on HSV-1, CMV, VZV, and HHV-8 have revealed important information on the function and structure of herpesvirus portal proteins. During dsDNA phage and herpesviral genome replication, concatamers of viral dsDNA are cleaved into single length units by a virus-encoded terminase and packaged into preformed procapsids through a channel located at a single capsid vertex (portal). Oligomeric portals are formed by the interaction of identical portal protein monomers. Comparing portal protein primary aa sequences between phage and herpesviruses reveals little to no sequence similarity. In contrast, the secondary and tertiary structures of known portals are remarkable. In all cases, function is highly conserved in that portals are essential for DNA packaging and also play a role in releasing viral genomic DNA during infection. Preclinical studies have described small molecules that target the HSV-1 and VZV portals and prevent viral replication by inhibiting encapsidation. This review summarizes what is known concerning the structure and function of herpesvirus portal proteins primarily based on their conserved bacteriophage counterparts and the potential to develop novel portal-specific DNA encapsidation inhibitors.

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“…В структуре рUL86 установлен домен, имеющий близкую структуру с РНКазаН-каталитическим сайтом обратной транскриптазы (ОТ) ВИЧ-1 и проявляющий РНКазаН/ интегразаподобную активность. РНКазный каталитический сайт ВИЧ-1 включает 4 аминокислотных остатка Asp443, Asp498, Glu478 и Asp549, координирующих 2 катиона Mg 2+ , а эндонуклеазный каталитический сайт pUL86 сформирован Asp463, Asp651, Glu534 и Ala465, которые координируют 2 катиона Mn 2+ [47,48]. Поэтому представляет очевидный интерес поиск структурных аналогов РТВ с более высокой антивирусной активностью.…”

Section: S 4as 8as)-n-трет-бутил-2-[(2r 3r)-2-гидрокси-3-[(3-гидрunclassified

“…3). Показано, что биомишенью для 10k является pUL86: в присутствии 10k ингибируется эндонуклеазная активность pUL86 и нарезание вирусной конкатемерной ДНК на единичные геномы [48].…”

Section: S 4as 8as)-n-трет-бутил-2-[(2r 3r)-2-гидрокси-3-[(3-гидрunclassified

Modern Ethiotropic Chemotherapy of Human Cytomegalovirus Infection: Clinical Effectiveness, Molecular Mechanism of Action, Drug Resistance, New Trends and Prospects. Part 1

Андронова¹

2018

Problems of Virology

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Modern chemotherapy of cytomegalovirus (CMV) infections has a very limited arsenal of first-line drugs. These are preparations of ganciclovir (GCV) belonging to the class of modified nucleosides and its metabolic precursor ganciclovir valine ester. After three-step phosphorylation, GCV, as a structural analogue of the natural nucleotide, competes with it for binding to DNA polymerase and, due to its structural features, inhibits its activity. However, with prolonged use of GCV, mainly under conditions of immunosuppression, the virus develops drug resistance associated in most cases with changes in pUL97 catalyzing the first stage of GCV phosphorylation, as well as in the catalytic subunit of DNA polymerase. When variants of viruses resistant to GCV appear, second-line drugs are used: pyrophosphate analog of foscarnet and nucleotide cidofovir. Resistance to second-line drugs is due to mutations in the pol-gene and in a number of cases leads to multiresistance, which makes it impossible to use traditional anti-CMV drugs. In addition, the use of all of the above drugs is accompanied by the development of severe side effects. All of the above determines the need to search for new compounds that can effectively inhibit the reproduction of the virus, harmless to the macroorganism, convenient to use, overcoming the drug resistance barrier in viruses. As a result of the search in international databases (PubMed, MedLine, eLIBRARY.RU, ClinicalTrials.gov, etc.), the main trends in the search for new anti-CMV agents were identified. In the first part of the review, we concentrated on compounds that are modifications of known antiviral agents currently used in clinical practice, the most promising for the development of drug anti-CMV drugs.

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Inhibition of Human Cytomegalovirus pUL89 Terminase Subunit Blocks Virus Replication and Genome Cleavage

Cited by 23 publications

References 31 publications

Comparison of Cytomegalovirus Terminase Gene Mutations Selected after Exposure to Three Distinct Inhibitor Compounds

Comparison of Cytomegalovirus Terminase Gene Mutations Selected after Exposure to Three Distinct Inhibitor Compounds

Human herpesvirus portal proteins: Structure, function, and antiviral prospects

Modern Ethiotropic Chemotherapy of Human Cytomegalovirus Infection: Clinical Effectiveness, Molecular Mechanism of Action, Drug Resistance, New Trends and Prospects. Part 1

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