Inhibition of endoplasmic reticulum glucosidases is required for in vitro and in vivo dengue antiviral activity by the iminosugar UV-4.

Warfield KL, Plummer EM, Sayce AC, Alonzi DS, Tang W, Tyrrell BE, Hill ML, Caputo AT, Killingbeck SS, Beatty PR, Harris E, Iwaki R
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et al

The antiviral activity of UV-4 was previously demonstrated against dengue virus serotype 2 (DENV2) in multiple mouse models. Herein, step-wise minimal effective dose and therapeutic window of efficacy studies of UV-4B (UV-4 hydrochloride salt) were conducted in an antibody-dependent enhancement (ADE) mouse model of severe DENV2 infection in AG129 mice lacking types I and II interferon receptors. Significant survival benefit was demonstrated with 10-20 mg/kg of UV-4B administered thrice daily (TID) for seven days with initiation of treatment up to 48 h after infection. UV-4B also reduced infectious virus production in in vitro antiviral activity assays against all four DENV serotypes, including clinical isolates. A set of purified enzyme, in vitro, and in vivo studies demonstrated that inhibition of endoplasmic reticulum (ER) α-glucosidases and not the glycosphingolipid pathway appears to be responsible for the antiviral activity of UV-4B against DENV. Along with a comprehensive safety package, these and previously published data provided support for an Investigational New Drug (IND) filing and Phases 1 and 2 clinical trials for UV-4B with an indication of acute dengue disease.

Keywords:

Antibody-dependent enhancement

,

Antiviral

,

Dengue

,

Glucosidase

,

Iminosugar

,

UV-4B

,

1-Deoxynojirimycin

,

Animals

,

Antibodies, Viral

,

Antibody-Dependent Enhancement

,

Antiviral Agents

,

Cells, Cultured

,

Chlorocebus aethiops

,

Clinical Trials as Topic

,

Dengue Virus

,

Disease Models, Animal

,

Drugs, Investigational

,

Endoplasmic Reticulum

,

Glycoside Hydrolase Inhibitors

,

Humans

,

Inhibitory Concentration 50

,

Mice

,

Monocytes

,

Receptors, Interferon

,

Serogroup

,

Severe Dengue

,

Vero Cells

,

alpha-Glucosidases