Webinar: Target X: An Unobstructed View of Pockets

About this session

Understanding how and where small molecules bind to protein pockets provides vital information for efficient design and establishing a defensible IP position. Having a complete picture of protein-ligand binding requires going beyond static structures, in which key pockets may not be apparent.

In this webinar, we introduce Target X, a method that combines enhanced sampling with data-driven modeling to provide a more complete view of protein pocket landscapes from a single apo structure.

Target X enables:

Identification of both known and previously unobserved binding sites
Reliable assessment of ligandability
Generation of conformations suitable for virtual screening

The approach demonstrates strong performance across diverse systems, along with improved robustness through the use of carefully curated, non-redundant training data. We will highlight applications in systems such as KRas and NKG2D and discuss how Target X supports structure-based drug design from early target understanding through screening.

Seeing where molecules can bind is no longer limited by static structures; with Target X, a more complete pocket landscape is within reach.