Pharmacomodulation of a ligand targeting the HBV capsid hydrophobic pocket.
Mathilde BridayFrançois HalléLauriane LecoqSylvie RadixJuliette MartinRoland MontserretMarie DujardinMarie-Laure FogeronMichael NassalBeat H MeierThierry LombergetAnja BöckmannPublished in: Chemical science (2022)
Hepatitis B virus (HBV) is a small enveloped retrotranscribing DNA virus and an important human pathogen. Its capsid-forming core protein (Cp) features a hydrophobic pocket proposed to be central notably in capsid envelopment. Indeed, mutations in and around this pocket can profoundly modulate, and even abolish, secretion of enveloped virions. We have recently shown that Triton X-100, a detergent used during Cp purification, binds to the hydrophobic pocket with micromolar affinity. We here performed pharmacomodulation of pocket binders through systematic modifications of the three distinct chemical moieties composing the Triton X-100 molecule. Using NMR and ITC, we found that the flat aromatic moiety is essential for binding, while the number of atoms of the aliphatic chain modulates binding affinity. The hydrophilic tail, in contrast, is highly tolerant to changes in both length and type. Our data provide essential information for designing a new class of HBV antivirals targeting capsid-envelope interactions.
Keyphrases
- hepatitis b virus
- liver failure
- magnetic resonance
- ionic liquid
- endothelial cells
- cancer therapy
- healthcare
- high resolution
- amino acid
- aqueous solution
- dna binding
- magnetic resonance imaging
- computed tomography
- liquid chromatography
- drug delivery
- transcription factor
- capillary electrophoresis
- big data
- social media
- mass spectrometry
- artificial intelligence
- recombinant human
- data analysis