Dataset Information

Lattice engineering enables definition of molecular features allowing for potent small-molecule inhibition of HIV-1 entry.

ABSTRACT: Diverse entry inhibitors targeting the gp120 subunit of the HIV-1 envelope (Env) trimer have been developed including BMS-626529, also called temsavir, a prodrug version of which is currently in phase III clinical trials. Here we report the characterization of a panel of small-molecule inhibitors including BMS-818251, which we show to be >10-fold more potent than temsavir on a cross-clade panel of 208-HIV-1 strains, as well as the engineering of a crystal lattice to enable structure determination of the interaction between these inhibitors and the HIV-1 Env trimer at higher resolution. By altering crystallization lattice chaperones, we identify a lattice with both improved diffraction and robust co-crystallization of HIV-1 Env trimers from different clades complexed to entry inhibitors with a range of binding affinities. The improved diffraction reveals BMS-818251 to utilize functional groups that interact with gp120 residues from the conserved ?20-?21 hairpin to improve potency.

SUBMITTER: Lai YT

PROVIDER: S-EPMC6318274 | biostudies-literature | 2019 Jan

REPOSITORIES: biostudies-literature

ACCESS DATA

Publications

Lattice engineering enables definition of molecular features allowing for potent small-molecule inhibition of HIV-1 entry.

Lai Yen-Ting YT Wang Tao T O'Dell Sijy S Louder Mark K MK Schön Arne A Cheung Crystal S F CSF Chuang Gwo-Yu GY Druz Aliaksandr A Lin Bob B McKee Krisha K Peng Dongjun D Yang Yongping Y Zhang Baoshan B Herschhorn Alon A Sodroski Joseph J Bailer Robert T RT Doria-Rose Nicole A NA Mascola John R JR Langley David R DR Kwong Peter D PD

Nature communications 20190103 1

Diverse entry inhibitors targeting the gp120 subunit of the HIV-1 envelope (Env) trimer have been developed including BMS-626529, also called temsavir, a prodrug version of which is currently in phase III clinical trials. Here we report the characterization of a panel of small-molecule inhibitors including BMS-818251, which we show to be >10-fold more potent than temsavir on a cross-clade panel of 208-HIV-1 strains, as well as the engineering of a crystal lattice to enable structure determinatio ...[more]

PMID: 30604750

Dataset Information

Lattice engineering enables definition of molecular features allowing for potent small-molecule inhibition of HIV-1 entry.

Publications

Lattice engineering enables definition of molecular features allowing for potent small-molecule inhibition of HIV-1 entry.

Similar Datasets

OmicsDI is part of the ELIXIR infrastructure

Similar Datasets

Identification of potent small molecule inhibitors of SARS-CoV-2 entry.
| S-EPMC8577999 | biostudies-literature

Force Field Optimization Guided by Small Molecule Crystal Lattice Data Enables Consistent Sub-Angstrom Protein-Ligand Docking.
| S-EPMC8218654 | biostudies-literature

Gene editing enables T-cell engineering to redirect antigen specificity for potent tumor rejection.
| S-EPMC6421629 | biostudies-literature

Lattice engineering through nanoparticle-DNA frameworks.
| S-EPMC5282967 | biostudies-literature

Small-Molecule CD4-Mimics: Structure-Based Optimization of HIV-1 Entry Inhibition.
| S-EPMC4789667 | biostudies-literature

Inhibition of Human Cytomegalovirus Entry into Host Cells Through a Pleiotropic Small Molecule.
| S-EPMC7084493 | biostudies-literature

Cell-cell transmission enables HIV-1 to evade inhibition by potent CD4bs directed antibodies.
| S-EPMC3320602 | biostudies-literature

Potent competitive inhibition of human ribonucleotide reductase by a nonnucleoside small molecule.
| S-EPMC5547592 | biostudies-literature

Engineering bacterial vortex lattice via direct laser lithography.
| S-EPMC6203773 | biostudies-literature

A small molecule approach to engineering vascularized tissue
2018-10-04 | E-MTAB-7209 | biostudies-arrayexpress