Synthesis and Evaluation of N-Phenyl-3-sulfamoyl-benzamide Derivatives as Capsid Assembly Modulators Inhibiting Hepatitis B Virus (HBV)

Koen Vandyck,Geert Rombouts,Bart Stoops,Abdellah Tahri,Ann Vos,Wim G. Verschueren,Yiming Wu,Jingmei Yang,Fuliang Hou,Bing Huang,Karen Vergauwen,Pascale Dehertogh,Jan Martin Berke,Pierre Raboisson

Synthesis and Evaluation of N-Phenyl-3-sulfamoyl-benzamide Derivatives as Capsid Assembly Modulators Inhibiting Hepatitis B Virus (HBV)

2018

Koen Vandyck
Geert Rombouts
Bart Stoops
Abdellah Tahri
Ann Vos
Wim G. Verschueren
Yiming Wu
Jingmei Yang
Fuliang Hou
Bing Huang
Karen Vergauwen
Pascale Dehertogh
Jan Martin Berke
Pierre Raboisson

Small molecule induced hepatitis B virus (HBV) capsid assembly modulation is considered an attractive approach for new antiviral therapies against HBV. Here we describe efforts toward the discovery of a HBV capsid assembly modulator in a hit-to-lead optimization, resulting in JNJ-632, a tool compound used to further profile the mode of action. Administration of JNJ-632 (54) in HBV genotype D infected chimeric mice resulted in a 2.77 log reduction of the HBV DNA viral load.

Keywords:

Small molecule
Hepatitis B virus HBV
Virology
Benzamide
Biochemistry
Capsid
DNA
Genotype
Chemistry
Hepatitis B virus
Viral load
Protein structure

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