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Design of gp120 HIV-1 entry inhibitors by scaffold hopping via isosteric replacements.


ABSTRACT: We present the development of alternative scaffolds and validation of their synthetic pathways as a tool for the exploration of new HIV gp120 inhibitors based on the recently discovered inhibitor of this class, NBD-14136. The new synthetic routes were based on isosteric replacements of the amine and acid precursors required for the synthesis of NBD-14136, guided by molecular modeling and chemical feasibility analysis. To ensure that these synthetic tools and new scaffolds had the potential for further exploration, we eventually tested few representative compounds from each newly designed scaffold against the gp120 inhibition assay and cell viability assays.

SUBMITTER: Iusupov IR 

PROVIDER: S-EPMC8511295 | biostudies-literature | 2021 Nov

REPOSITORIES: biostudies-literature

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Design of gp120 HIV-1 entry inhibitors by scaffold hopping via isosteric replacements.

Iusupov Ildar R IR   Curreli Francesca F   Spiridonov Evgeniy A EA   Markov Pavel O PO   Ahmed Shahad S   Belov Dmitry S DS   Manasova Ekaterina V EV   Altieri Andrea A   Kurkin Alexander V AV   Debnath Asim K AK  

European journal of medicinal chemistry 20210707


We present the development of alternative scaffolds and validation of their synthetic pathways as a tool for the exploration of new HIV gp120 inhibitors based on the recently discovered inhibitor of this class, NBD-14136. The new synthetic routes were based on isosteric replacements of the amine and acid precursors required for the synthesis of NBD-14136, guided by molecular modeling and chemical feasibility analysis. To ensure that these synthetic tools and new scaffolds had the potential for f  ...[more]

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