Litcius/Paper detail

Incorporating Target-Specific Pharmacophoric Information into Deep Generative Models for Fragment Elaboration

Thomas E. Hadfield, Fergus Imrie, Andy Merritt, Kristian Birchall, Charlotte M. Deane

2022Journal of Chemical Information and Modeling25 citationsDOIOpen Access PDF

Abstract

Despite recent interest in deep generative models for scaffold elaboration, their applicability to fragment-to-lead campaigns has so far been limited. This is primarily due to their inability to account for local protein structure or a user's design hypothesis. We propose a novel method for fragment elaboration, STRIFE, that overcomes these issues. STRIFE takes as input fragment hotspot maps (FHMs) extracted from a protein target and processes them to provide meaningful and interpretable structural information to its generative model, which in turn is able to rapidly generate elaborations with complementary pharmacophores to the protein. In a large-scale evaluation, STRIFE outperforms existing, structure-unaware, fragment elaboration methods in proposing highly ligand-efficient elaborations. In addition to automatically extracting pharmacophoric information from a protein target's FHM, STRIFE optionally allows the user to specify their own design hypotheses.

Topics & Concepts

Fragment (logic)ElaborationComputer scienceGenerative grammarPharmacophoreArtificial intelligenceGenerative modelMachine learningChemistryAlgorithmStereochemistryPhilosophyHumanitiesComputational Drug Discovery MethodsMicrobial Natural Products and BiosynthesisChemical Synthesis and Analysis