Exploring Human Parainfluenza Virus Type-1 Hemagglutinin–Neuraminidase as a Target for Inhibitor Discovery

El‐Deeb, Ibrahim M.; Guillon, Patrice; Winger, Moritz; Eveno, Tanguy; Haselhorst, Thomas; Dyason, Jeffrey Clifford; Itzstein, Mark von

doi:10.1021/jm500759v

Cited by 21 publications

(63 citation statements)

References 35 publications

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“…Along this line, we planned the synthesis of sulfonamide 2 a , via an azido intermediate. However, considering that some azido derivatives, such as BCX‐2798 1 b , have been reported among the most promising inhibitors against hPIVs, we also planned to synthesize the free azido compound 3 a . Additionally, we designed the synthesis of some unreported inhibitors, 2 b – d and 3 b – d , by combining the new selected C4 substituents ( p ‐toluenesulfonyl amido and azido) with the linear homologues perfluoracylamides at C5, from trifluoroacetic to heptafluorobutyric, that we previously reported .…”

Section: Figurementioning

confidence: 99%

“…After these preliminary considerations, we synthesized the p ‐toluenesulfonyl amido derivative 2 a and the azido compound 3 a . These selected molecules were achieved, according to the previously reported literature . However, the final hydrolytic step was performed with K 2 CO 3 in methanol/water (10:1) mixture, affording the desired inhibitors 2 a and 3 a in acidic form.…”

Section: Figurementioning

confidence: 99%

“…To this purpose, we synthesized some new analogues 2 b – d and 3 b – d . The key azido derivatives 8 b – d were obtained, as reported in Scheme , starting from compound 7 by direct N ‐transacylation of the amidic function at C5. Notably, these results highlighted that the N ‐transacylation reaction works well even in the presence of a relatively unstable azido group.…”

Section: Figurementioning

confidence: 99%

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Potent Inhibitors against Newcastle Disease Virus Hemagglutinin‐Neuraminidase

et al. 2018

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Neuraminidase activity is essential for the infection and propagation of paramyxoviruses, including human parainfluenza viruses (hPIVs) and the Newcastle disease virus (NDV). Thus, many inhibitors have been developed based on the 2-deoxy-2,3-didehydro-d-N-acetylneuraminic acid inhibitor (DANA) backbone. Along this line, herein we report a series of neuraminidase inhibitors, having C4 (p-toluenesulfonamido and azido substituents) and C5 (N-perfluorinated chains) modifications to the DANA backbone, resulting in compounds with 5- to 15-fold greater potency than the currently most active compound, the N-trifluoroacetyl derivative of DANA (FANA), toward the NDV hemagglutinin-neuraminidase (NDV-HN). Remarkably, these inhibitors were found to be essentially inactive against the human sialidase NEU3, which is present on the outer layer of the cell membrane and is highly affected by the current NDV inhibitor FANA.

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Section: Figurementioning

confidence: 99%

Section: Figurementioning

confidence: 99%

Section: Figurementioning

confidence: 99%

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Potent Inhibitors against Newcastle Disease Virus Hemagglutinin‐Neuraminidase

et al. 2018

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“…1-4 Modification of the amido group at the 5-position of N -amidoneuraminic acid derivatives has proved to be beneficial in the development of sialidase inhibitors and of carbohydrate antigens with greater antigenicity. 5-9 Such modifications have typically been achieved by N -deacetylation, its glycosides and derivatives, followed by reinstallation of different acyl groups, 6-7,10-12 or by use of the biosynthetic machinery when various N -acyl mannosamines are converted enzymatically to the corresponding N -acyl neuraminic acids 13 and eventually their glycosides, 14-15 or by a combination of the biosynthetic and chemical methods. 16 Consequently, modifications are typically limited to amide derivatives or other simple substitutions that are compatible with the biosynthetic machinery such as the conversion of 2-deoxy glucose to 5-desacetamido neuraminic acid.…”

Section: Introductionmentioning

confidence: 99%

Oxidative Deamination ofN-Acetyl Neuraminic Acid: Substituent Effects and Mechanism

Buda

Crich

2016

J. Am. Chem. Soc.

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A study of the mechanism of the oxidative deamination of the N-nitroso-N-acetyl sialyl glycosides leading with overall retention of configuration to the corresponding 2-keto-3-deoxy-d-glycero-d-galacto-nonulopyranosidonic acid (KDN) glycosides is described, making use of a series of differentially O-protected N-nitroso-N-acetyl sialyl glycosides and of isotopic labelling studies. No evidence is found for stereodirecting participation by ester groups at the 4- and 7-positions. Comparisons are drawn with oxidative deamination reactions of 4-amino-4-deoxy and 2-amino-2-deoxy hexopyranosides and a common mechanism is formulated involving the intermediacy of 1-oxabicyclo[3.1.0]hexyl oxonium ions following participation by the pyranoside ring oxygen. A minor reaction pathway has been uncovered by labelling studies in the β-thiosialosides that results in the exchange of the 4-O-acetyl group by the glacial acetic acid that serves as external nucleophile in the general oxidative deamination process. A mechanism is proposed for this exchange involving participation by the thioglycoside at the level of an intermediate diazoalkane.

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“…To investigate the catalytic mechanism of hPIV-3 HN, the 2,3-difluoro analogues (3-5) of the previously reported potent hPIV inhibitor BCX2798 (2), have been synthesized following the procedures illustrated in Figure 1 b. The synthesis of the target compounds started with the known [21,22] 4-azido-4deoxy-5-isobutyramido-Neu2en intermediate 6. The halohydrins 7 and 8 were obtained in very good overall yields of 58 % and 35 %, respectively, and in a short period of time by heating intermediate 6 with Selectfluor in an aqueous nitromethane solution by microwave (MW) irradiation for 2 h at 80 8C.…”

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confidence: 99%

The Catalytic Mechanism of Human Parainfluenza Virus Type 3 Haemagglutinin‐Neuraminidase Revealed

et al. 2015

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Human parainfluenza virus type 3 (hPIV-3) is one of the leading causes for lower respiratory tract disease in children, with neither an approved antiviral drug nor vaccine available to date. Understanding the catalytic mechanism of human parainfluenza virus haemagglutinin-neuraminidase (HN) protein is key to the design of specific inhibitors against this virus. Herein, we used (1) H NMR spectroscopy, X-ray crystallography, and virological assays to study the catalytic mechanism of the HN enzyme activity and have identified the conserved Tyr530 as a key amino acid involved in catalysis. A novel 2,3-difluorosialic acid derivative showed prolonged enzyme inhibition and was found to react and form a covalent bond with Tyr530. Furthermore, the novel derivative exhibited enhanced potency in virus blockade assays relative to its Neu2en analogue. These outcomes open the door for a new generation of potent inhibitors against hPIV-3 HN.

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Exploring Human Parainfluenza Virus Type-1 Hemagglutinin–Neuraminidase as a Target for Inhibitor Discovery

Cited by 21 publications

References 35 publications

Potent Inhibitors against Newcastle Disease Virus Hemagglutinin‐Neuraminidase

Potent Inhibitors against Newcastle Disease Virus Hemagglutinin‐Neuraminidase

Oxidative Deamination ofN-Acetyl Neuraminic Acid: Substituent Effects and Mechanism

The Catalytic Mechanism of Human Parainfluenza Virus Type 3 Haemagglutinin‐Neuraminidase Revealed

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