A combined in silico / in vitro approach unveils common molecular requirements for efficient BVDV RdRp binding of linear aromatic N-polycyclic systems

Carta, Antonio; Briguglio, Irene; Piras, Sandra; Corona, Paola; Ibba, Roberta; Laurini, Erik; Fermeglia, Maurizio; Pricl, Sabrina; Desideri, N.; Atzori, Elena Maria; Colla, Paolo La; Collu, Gabriella; Delogu, Ilenia; Loddo, Roberta

doi:10.1016/j.ejmech.2016.03.080

Cited by 23 publications

(13 citation statements)

References 34 publications

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“…As described above, the driven idea for this project is the isosteric substitution of a nitrogen atom with a carbon atom and evaluate the antiviral activity of the resulted molecules compared with the parental compounds. Naphthoimidazole derivatives ( 3a -j ) were designed and synthesised in order to confirm the relevance of nitrogen atom in position 5 of the imidazoquinoline derivatives for the interaction with the target, these molecule's antiviral results confirmed the predicted affinity data previously published since they showed a consistent loss of antiviral activity with respect to parental compounds [32]. Derivative 3a still maintains a weak antiviral activity, EC 50 at 16 µM, but related at cytotoxicity CC 50 value of 37 µM.…”

Section: Resultssupporting

confidence: 60%

“…In detail, arginine 295 interacts with N5 of the lead compound as H-bond donor, while N1 resulted as H-bond acceptor in the interaction with tyrosine 674 and the nitrogen of the benzonitrile moiety gives H-bond with serine 411. Has also been predicted the decrease of affinity of some molecules with the substrate when R295 and Y674 -critical residues for compound binding -are mutated into alanine and the prediction has been confirmed by in vitro assays on the mutant RdRp [32]. In order to have a further negative control for these simulations, we now designed some chemical modification on the lead compounds and parent compounds similarly active in BVDV RdRp inhibition, and we synthesised the designed compounds.…”

Section: Introductionmentioning

confidence: 95%

“…In the framework of a long-lasting antiviral research program, our group designed and synthesised a series of angular and linear N-polycyclic derivatives active against BVDV, YFV, HCV and other related viruses [23 -30]. The molecular target for BVDV inhibition was identified in the viral RNA dependent RNA polymerase (RdRp) [24,28,31,32]. Imidazo[4,5-g]quinoline derivatives were published as interesting BVDV inhibitors and the most active derivative of that series, 4-(4-chloro-3H-imidazo[4,5-g]quinolin-2yl)benzonitrile (A) (EC 50 0.3µM; CC 50 >100 µM) [32,33] was docked and scored for affinity towards the binding site of the BVDV RdRp, the resulting receptor/ligand complex was relaxed by energy minimisation, followed by MD simulation.…”

Section: Introductionmentioning

confidence: 99%

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Anti-BVDV Activity Evaluation of Naphthoimidazole Derivatives Compared with Parental Imidazoquinoline Compounds

Ibba¹,

Piras²,

Delogu³

et al. 2020

TOMCJ

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Background: Pestivirus genus includes animal pathogens which are involved in economic impact for the livestock industry. Among others, Bovine Viral Diarrhoea Virus (BVDV) establish a persistent infection in cattle causing a long list of symptoms and a high mortality rate. In the last decades, we synthesised and reported a certain number of anti-BVDV compounds. Methods: In them, imidazoquinoline derivatives turned out as the most active. Their mechanism of actions has been deeply investigated, BVDV RNA-dependent RNA polymerase (RpRd) resulted as target and the way of binding was predicted in silico through three main H-bond interaction with the target. The prediction could be confirmed by target or ligand mutation. The first approach has already been performed and published confirming the in silico prediction. Results: Here, we present how the ligand chemical modification affects the anti-BVDV activity. The designed compounds were synthesised and tested against BVDV as in silico assay negative control. Conclusion: The antiviral results confirmed the predicted mechanism of action, as the newly synthesised compounds resulted not active in the in vitro BVDV infection inhibition.

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Section: Resultssupporting

confidence: 60%

Section: Introductionmentioning

confidence: 95%

Section: Introductionmentioning

confidence: 99%

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Anti-BVDV Activity Evaluation of Naphthoimidazole Derivatives Compared with Parental Imidazoquinoline Compounds

Ibba¹,

Piras²,

Delogu³

et al. 2020

TOMCJ

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“…As a part of our researches on heterocyclic compounds with antiviral activity (Conti et al, 2014, 2017; Carta et al, 2016; Fioravanti et al, 2017), we recently identified ( N -(1,3-diphenyl-1 H -pyrazol-4-yl)methyl)anilines ( 1a-v ) as a new class of potent and selective inhibitors of human respiratory syncytial virus (RSV) replication (Fioravanti et al, 2015). Some derivatives were also endowed with a moderate activity against YFV and BVDV representative type members of the Flavivirus genus and the Pestivirus genus, respectively, within the Flaviviridae family (Fioravanti et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

Design, Synthesis, Antiviral Evaluation, and SAR Studies of New 1-(Phenylsulfonyl)-1H-Pyrazol−4-yl-Methylaniline Derivatives

et al. 2019

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A series of N -((3-phenyl-1-(phenylsulfonyl)-1 H -pyrazol-4-yl)methyl)anilines 7a-p and 8a-l , structurally related to previously synthesized and tested ( N -(1,3-diphenyl-1 H -pyrazol-4-yl)methyl)anilines ( 1a-v ), were designed and synthesized. The new derivatives were evaluated in cell-based assays for their cytotoxicity and antiviral activity against a large panel of RNA and DNA viruses of public health significance. Generally, the tested compounds did not display cytotoxicity toward the cell lines used. The majority of derivatives 7a - p were able to interfered with YFV and RSV replication in the micromolar range showing a marked improvement in potency and selectivity with respect to the reference inhibitors 6-azauridine and ribavirin, respectively. The introduction of a p -methoxy substituent on the phenylsulfonyl group (compounds 8a-l ) completely abolished the anti-RSV activity and reduced or eliminated the potency against YFV. On the contrary, several p -methoxy analogs were able to interfere with BVDV replication with a comparable ( 8b, 8c, 8g , and 8k ) or better ( 8a and 8f ) potency than the reference inhibitor, ribavirin. Compound 7e , selected for time of addition experiments on BHK-21 cell cultures infected with YFV, achieved the highest reduction of virus titer when added 2 h post infection and maintained up to 4 h post infection.

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“…Bovine viral diarrhea-mucosal disease (BVD-MD), also known as bovine viral diarrhea-mucosal disease virus or mucosal virus, is a contagious disease that often occurs in domestic animals[1, 2]. BVD-MD is caused by BVDV viral infection from viruses in the Pestivirus genus of the Flaviviridae family.…”

Section: Introductionmentioning

confidence: 99%

Selection and characterization of specific nanobody against bovine virus diarrhea virus (BVDV) E2 protein

Huang

Xiao

et al. 2017

PLoS ONE

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Bovine viral diarrhea-mucosal disease (BVD-MD) is caused by bovine viral diarrhea virus (BVDV), and results in abortion, stillbirth, and fetal malformation in cows. Here, we constructed the phage display vector pCANTAB 5E-VHH and then transformed it into Escherichia coli TG1-competent cells, to construct an initial anti-BVDV nanobody gene library. We obtained a BVDV-E2 antigen epitope bait protein by prokaryotic expression using the nucleotide sequence of the E2 gene of the BVDV-NADL strain published in GenBank. Phage display was used to screen the anti-BVDV nanobody gene library. We successfully constructed a high quality phage display nanobody library, with an initial library capacity of 4.32×105. After the rescue of helper phage, the titer of the phage display nanobody library was 1.3×1011. The BVDV-E2 protein was then expressed in Escherichia coli (DE3), and a 49.5 kDa band was observed with SDS-PAGE analysis that was consistent with the expected nanobody size. Thus, we were able to isolate one nanobody that exhibits high affinity and specificity against BVDV using phage display techniques. This isolated nanobody was then used in Enzyme Linked Immunosorbent Assay and qRT-PCR, and ELISA analyses of BVDV infection of MDBK cells indicated that the nanobodies exhibited good antiviral effect.

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A combined in silico / in vitro approach unveils common molecular requirements for efficient BVDV RdRp binding of linear aromatic N-polycyclic systems

Cited by 23 publications

References 34 publications

Anti-BVDV Activity Evaluation of Naphthoimidazole Derivatives Compared with Parental Imidazoquinoline Compounds

Anti-BVDV Activity Evaluation of Naphthoimidazole Derivatives Compared with Parental Imidazoquinoline Compounds

Design, Synthesis, Antiviral Evaluation, and SAR Studies of New 1-(Phenylsulfonyl)-1H-Pyrazol−4-yl-Methylaniline Derivatives

Selection and characterization of specific nanobody against bovine virus diarrhea virus (BVDV) E2 protein

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