A Conserved Pocket in the Dengue Virus Polymerase Identified through Fragment-based Screening

Noble, Christian G.; Lim, Siew Pheng; Arora, Rishi; Yokokawa, Fumiaki; Nilar, Shahul; Seh, Cheah Chen; Wright, S. Kirk; Benson, Timothy E.; Smith, Paul W.; Shi, Pei Yong

doi:10.1074/jbc.m115.710731

Cited by 64 publications

(74 citation statements)

References 20 publications

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“…The priming loop locates between α19 and α20 in the subthumb domain, which is deployed inside the catalytic chamber to promote formation of the initiation complex. This loop is well‐ordered and inserting into a narrow RNA binding tunnel in our structure, implying that our ZIKV RdRp adopts a “closed” pre‐initiation state conformation (Noble et al , , ; Lim et al , ).…”

Section: Resultsmentioning

confidence: 66%

“…Previously, two conserved inhibitor‐binding sites have been identified for DENV RdRp (Noble et al , , ; Lim et al , ; Yokokawa et al , ). One is targeting the RNA template entry tunnel (Noble et al , ), and the other pocket, called as the “N pocket”, located in the thumb subdomain, close to the enzyme active site (Lim et al , ; Noble et al , ; Yokokawa et al , ). By targeting the RNA tunnel, the compound NITD107 was first identified by enzyme activity‐based screening and the binding site was defined by complex structure (Noble et al , ).…”

Section: Resultsmentioning

confidence: 99%

“… Superimposition of ZIKV RdRp with DENV3 RdRp apo structure (gray) (PDB: 4HHJ) or DENV3 RdRp (light pink) bound to NTTD107 molecule (purple) (PDB: 3VWS) (Niyomrattanakit et al , ; Noble et al , ). The detailed interactions are shown in the panel on the right side. Superimposition of ZIKV RdRp with DENV3 RdRp (gray) bound to JF‐31‐MG46 molecule (orange) (PDB: 5F3T) (Noble et al , ). The detailed interactions are shown in the panel on the right side. Superimposition of ZIKV RdRp with DENV3 RdRp (gray) bound to 29 compound (gold) (PDB: 5I3Q) (Lim et al , ; Yokokawa et al , ).…”

Section: Resultsmentioning

confidence: 99%

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The crystal structure of Zika virus NS 5 reveals conserved drug targets

et al. 2017

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Zika virus (ZIKV) has emerged as major health concern, as ZIKV infection has been shown to be associated with microcephaly, severe neurological disease and possibly male sterility. As the largest protein component within the ZIKV replication complex, NS5 plays key roles in the life cycle and survival of the virus through its N-terminal methyltransferase (MTase) and C-terminal RNAdependent RNA polymerase (RdRp) domains. Here, we present the crystal structures of ZIKV NS5 MTase in complex with an RNA cap analogue ( m7 GpppA) and the free NS5 RdRp. We have identified the conserved features of ZIKV NS5 MTase and RdRp structures that could lead to development of current antiviral inhibitors being used against flaviviruses, including dengue virus and West Nile virus, to treat ZIKV infection. These results should inform and accelerate the structure-based design of antiviral compounds against ZIKV.

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Section: Resultsmentioning

confidence: 66%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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The crystal structure of Zika virus NS 5 reveals conserved drug targets

et al. 2017

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“…31,32 Fragments are small molecular weight compounds (MW < 300 Da) that are frequently used for the discovery of novel drugs. They generally possess good drug-like properties, high ligand efficiency (a measure of affinity corrected by size), and good coverage of available chemical space.…”

Section: Introductionmentioning

confidence: 99%

Identification of allosteric binding sites for PI3Kα oncogenic mutant specific inhibitor design

Miller

Maheshwari

McRobb

et al. 2017

Bioorganic & Medicinal Chemistry

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PIK3CA , the gene that encodes the catalytic subunit of phosphatidylinositol 3-kinase α (PI3Kα), is frequently mutated in breast and other types of cancer. A specific inhibitor that targets the mutant forms of PI3Kα could maximize treatment efficiency while minimizing side-effects. Herein we describe the identification of novel binding pockets that may provide an opportunity for the design of mutant selective inhibitors. Using a fragment-based approach, we screened a library of 352 fragments (MW <300 Da) for binding to PI3Kα by X-ray crystallography. Five novel binding pockets were identified, each providing potential opportunities for inhibitor design. Of particular interest was a binding pocket near Glu542, which is located in one of the two most frequently mutated domains.

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“…The structural information could be used for rational design, as previously shown for dengue RdRp inhibitors. 13 In addition, compounds with improved potency could also be tested in a pregnant mouse model for prevention of maternal-to-fetal viral transmission. 14 Collectively, the study by Sariyer et al 2 reinforces the potential of drug repurposing for therapeutic development against emerging and re-emerging pathogens.…”

mentioning

confidence: 99%