2024 ARCHIVES

Cambridge Healthtech Institute’s 19th Annual

Fragment-Based Drug Discovery

Fragment-Based Lead Design (FBLD) for New Small Molecule Therapeutic Candidates

APRIL 2 - 3, 2024

Fragment-based drug discovery (FBDD) approaches have proven fruitful for finding new drug candidates, especially against non-enzymatic intracellular targets such as protein-protein interactions (PPIs), including molecular glues, that lack a typical pocket for an inhibitor to bind within. Cambridge Healthtech Institute's Fragment-Based Drug Discovery conference covers the latest refinements to fragment libraries, innovations in biophysical approaches for screening fragment hits, and case studies of growing a fragment hit into a drug lead and beyond. The challenges of integrating information from other lead generation approaches like DNA-encoded libraries, and other timely topics, will also be on the agenda and/or part of discussions with fellow medicinal chemists.

6:00 pm MONDAY, APRIL 1: Dinner Short Course*

SC2: Fragment-Based Drug Design: Advancing Tools and Technologies

*Premium Pricing or separate registration required. See Short Courses page for details.

Tuesday, April 2

Registration Open and Morning Coffee7:00 am

Welcome Remarks8:00 am

8:05 am

Chairperson's Remarks

Matthew A. Marx, PhD, Senior Vice President, Drug Discovery, Mirati Therapeutics, Inc.

8:10 am

Assessing Highly Diverse Fragment Libraries by ¹⁹F NMR Enables Robust Identification of Chemical Starting Points for Challenging Drug Targets

Andreas Lingel, PhD, Associate Director, Global Discovery Chemistry, Novartis Institutes for Biomedical Research

Hit and lead generation by fragment-based methods has become an established approach which is now routinely applied alongside complementary methods in early drug discovery, with ¹⁹F NMR-based methods proven to be of particular utility as they offer unique advantages. In this presentation, recent developments which increase the feasibility of assessing large and chemically diverse libraries by ¹⁹F NMR as well as case studies of difficult-to-drug targets will be discussed.

8:40 am

Computational Hot-Spot Mapping for Fragment-Based Drug Discovery

Diane M. Joseph-McCarthy, PhD, Professor of the Practice, Biomedical Engineering, Boston University

Identification of fragment-binding positions on the surface of macromolecules is a key to locating druggable sites, assessing the druggability of novel targets, and developing starting points for finding new chemical entities. Computational hot-spot mapping was performed across a set of known or potential drug targets, and a novel approach for clustering was employed to select the top druggable sites, including those at active and allosteric sites. Within this context we assessed the utility of experimentally-determined vs. AlphaFold-generated models. Some of the latest techniques such as FTMove and its use with AlphaFold models (AI generated protein models) will be described.

9:10 am

Fragments to Leads: Accelerating Discovery by Rapid Screening of Giga-Scale On-Demand Chemical Spaces

Antonina Nazarova, PhD, Research Associate, Seva Katritch Lab, Quantitative & Computational Biology, University of Southern California

Rapid synthon-based screening approaches like V-SYNTHES have shown practical utility in hit and lead discovery for many clinically relevant targets, however, like any structure-based method it is limited to the structurally well-defined binding pockets. Here, we explore the new approaches to incorporate experimental information obtained in classical fragment screening into the V-SYNTHES pipeline to discover potent lead-like and drug-like ligands for cryptic pockets usually considered undruggable.

9:40 am

Exploring protein-protein interactions by Weak Affinity Chromatography (WAC™) - An IL-23 case study

Björn Walse, PhD, CEO, SARomics Biostructures AB

The advantage of WAC™ for FBS are the detection of weak binders by screening fragments at low concentrations (<5 μM) and its immediate ranking of hits. Here we present the result of a WAC™ screen towards IL-23 with hit validation by NMR, TSA and X-ray crystallography.

9:55 am

Site Directed Hit Discovery to Define the Mode of Action

Johan Veerman, PhD, Head of Chemistry, ZoBio

Allosteric inhibitors/activators, cryptic site binders, monofunctional degraders all require (not) binding at a specific site on the target. A generic binding screen is both inefficient and possibly misleading. A screen directed towards (or away from) a particular site on the target would be advantageous. Here biophysical approaches to accomplish this goal are presented. The complementary application of biochemical assays and structure elucidation increases confidence in promising chemotypes.

Networking Coffee Break10:10 am

10:35 am FEATURED PRESENTATION:

Integrating FBDD and DEL Approaches for Lead Generation

Chaohong Sun, PhD, Senior Director, Target Enabling Technologies, AbbVie, Inc.

In this presentation, I will discuss different hit generation approaches and highlight the opportunities of integrating FBDD and DEL for challenging target classes.

11:05 am

Beyond Affinity: Dissecting the Kinetic Landscape of Turnover Inhibitors of Nicotinamide N-Methyl Transferase (NNMT) and in vivo Verification of the Inhibitory Mechanism

Tomas Akerud, Associate Principal Scientist, Global Structural Chemistry, AstraZeneca R&D

A screen of 17k fragments identified 3 classes on NNMT inhibitors. One of the classes were turnover inhibitors which are substrates of the enzyme. We characterized this inhibitory mechanism in detail using a newly developed surface biosensor methodology that quantify enzymatic turnover. Systematic medicinal chemistry resulted in identification of more potent, extremely ligand efficient, inhibitors, for which we were able to verify the inhibitory mechanism in vivo.

11:35 am

Fragment-Based Discovery of Allosteric Probes of Protein Tyrosine Phosphatases

Virgil Woods, Senior Graduate Student, Laboratory of Daniel Keedy, Biochemistry, City University of New York

Fragment-based drug design presents a unique opportunity to identify allosteric footholds for therapeutic targets that have resisted conventional active-site-focused drug discovery. We leveraged crystallographic fragment screening and machine learning to discover binders and inhibitors at the allosteric L16 site of PTP1B. We characterized these and existing ligands using multiple biophysical assays, including HDX-MS. The results include a variety of responses in protein dynamics, including surprisingly diverse and widespread effects on conformational dynamics. Alongside complementary work on fragment screening with room-temperature crystallography, these results emphasize the powerful effects fragments and lead compounds have on protein structure and dynamics.

Enjoy Lunch on Your Own12:05 pm

1:30 pm

Chairperson's Remarks

Daniel A. Erlanson, PhD, Chief Innovation Officer, Innovation and Discovery, Frontier Medicines Corporation

1:35 pm

Covalent Discovery at AstraZeneca: Delivering the Next Generation of Irreversible Medicines

Henry Blackwell, PhD, Senior Scientist, Medicinal Chemistry, AstraZeneca

The rational search for covalent drugs has typically relied on the development of potent reversible binders, followed by the appending of an electrophilic warhead. Recently, a distinct approach involving the screening of covalent fragment-sized molecules has proved to be a viable method for the discovery of hits against previously intractable targets, including PPIs. This talk describes how AstraZeneca are pioneering the use of the electrophile-first approach for covalent drug discovery.

2:05 pm

Structure-Based Approaches Uncover Distinct Binding Modes for Covalent and Non-Covalent Ligands

Alex Berndt, PhD, Structural Biologist, Astex Pharmaceuticals Ltd

Astex has pioneered the application of structure-based approaches in drug discovery. I present a case study where crystal engineering was used to trap a therapeutic target protein kinase in distinct conformational states and deliver novel soakable crystal systems. This allowed the characterization of binding modes and mechanism-of-action of covalent and non-covalent compounds currently in the clinic. The combined results identified strategies to dial-out off-target effects and improve ligand selectivity.

2:35 pm

Identification of Unprecedented Binding Sites by Electrophilic MiniFrags

Gyorgy Keseru, PhD, Professor, Medicinal Chemistry, Research Centre for Natural Sciences (RCNS), Hungary

We developed the covalent alternatives of Astex's MiniFrags that allow mapping potential binding sites for covalent inhibitors. Covalent MiniFrags are 5- and 6-membered electrophilic heterocycles that covalently bond at their binding site. Screening hits can be identified by simple biochemical assay, and the binding site can be located by mass spectrometry. The utility of this methodology was demonstrated by discovering the first leadlike covalent inhibitor of HDAC8.

3:05 pm

Integrated Fragment-Based Drug Discovery (FBDD) studies at Selvita

Aleksandra Bebel, PhD, Team Leader, Crystallography Laboratory, Selvita S.A.

In this FBDD campaign, we searched for novel binders of VHL-EloB-EloC (VBC), a complex of an E3 ligase used as a targeted protein degrader. Fragment screening of VBC by SPR and X-ray crystallography resulted in identification of novel binders that were then evaluated and developed into an innovative series of compounds by computational chemistry and AI methods. The compounds are used for further development of PROTACs targeting therapeutic targets of interest.

Grand Opening Refreshment Break in the Exhibit Hall with Poster Viewing and Best of Show Voting Begins3:20 pm

4:20 pm

Plenary Welcome Remarks from Lead Content Director with Poster Finalists Announced

Anjani Shah, PhD, Senior Conference Director, Cambridge Healthtech Institute

4:30 pm

PLENARY KEYNOTE: Applications of SuFEx Click Chemistry for Drug Discovery and Chemical Biology

Barry Sharpless, PhD, Professor, Chemistry, Scripps Research Institute; 2022 and 2001 Nobel Laureate

My work has been guided by the modular simplicity of nature—the fact that all molecules of life are made from several dozen building blocks. Here I will discuss the Sulfur(VI) Fluoride Exchange (SuFEx), a second near-perfect click chemistry reaction pioneered here at Scripps. SuFEx allows reliable molecular connections to be made under metal-free conditions. I will include applications in drug discovery, chemical biology, and polymer chemistry.

Welcome Reception in the Exhibit Hall with Poster Viewing5:15 pm

Close of Day6:15 pm

Wednesday, April 3

Registration Open7:15 am

In-Person Breakouts with Continental Breakfast7:45 am

In-Person Breakouts are informal, moderated discussions, allowing participants to exchange ideas and experiences and develop future collaborations around a focused topic. Each breakout will be led by a facilitator who keeps the discussion on track and the group engaged. To get the most out of this format, please come prepared to share examples from your work, be a part of a collective, problem-solving session, and participate in active idea sharing. Please visit the Breakout Discussions page on the conference website for a complete listing of topics and descriptions.

IN-PERSON BREAKOUT 4:

FBDD against RNA Targets (SESSION ROOM)

Yaqiang Wang, PhD, Principal Scientist, Chemical Sciences & Structural Biology, Arrakis Therapeutics

Challenges for fragment screening against RNA targets vs. protein targets
How to decrease rate of false positive hits during fragment screening
Is high-resolution structure information required to evolve and optimize the hit?
Preferred fragment library for RNA

IN-PERSON BREAKOUT 5:

Covalent Fragments (FOYER)

Maurizio Pellecchia, PhD, Professor, Biomedical Sciences Division, University of California, Riverside

Which amino acids to target and with what chemistry?
Best methods/practices to screen for covalent fragments
How to optimize a covalent fragment

8:30 am

Chairperson's Remarks

Maricel Torrent, PhD, Principal Research Scientist, Computational Drug Discovery, AbbVie, Inc.

8:35 am

Exploring Hidden Pockets: Using Experimentally Driven MD Simulations for Structure-Based Drug Design

Benjamin Walters, PhD, Senior Principal Scientist, Genentech, Inc.

This study demonstrates a novel method employing data from HDX experiments to guide small molecules into cryptic pockets to crystallographic resolution with a success rate greater than 85%. A cryptic pocket is a binding site that requires the ligand in order to exist. These pockets elude successful interrogation by computational techniques, such as virtual screening and present a considerable challenge for drug discovery. The method will be described using a dynamic kinase with solved X-ray structures reflecting many binding modes before demonstrating its utility on a fragment-based drug discovery program, alongside critical aspects of the HDX experiments that enable this work.

9:05 am

Turning Cryptic Pockets into Drugs: Using (Bio)Synthetic Probes to Land in Drug-Like Chemical Space

Jerome M. Fox, PhD, CEO, Think Bioscience

I'll present how we program microbes to build small-molecule modulators that bind to cryptic pockets. We use these pockets to guide the discovery of novel hits in drug-like chemical space. Our pocket-finding probes are sp3-rich and largely nonpolar; our final hits are soluble, drug-like, and amenable to rapid chemical elaboration.

Coffee Break in the Exhibit Hall with Poster Awards Announced9:35 am

10:30 am

FEATURED PRESENTATION: Fragment-Based Screening for SARS-CoV Drug Discovery

Stephen W. Fesik, PhD, Professor of Biochemistry, Pharmacology & Chemistry; Orrin H. Ingram II Chair in Cancer Research, Vanderbilt University

Although vaccines can prevent SARS-CoV-2 infection, variants have emerged that produce resistance. New small-molecule anti-virals that inhibit COVID-19 are needed. Papain-like protease cleaves the polypeptide of the virus and is required for viral replication. Using an NMR-based fragment screen, we identified hits that bind to the protein, optimized these hits using structure-based design, and developed potent covalent and noncovalent inhibitors of the enzyme that block viral replication.

11:00 am

Fragment Hit-Finding Campaigns against Ubiquitin Ligases

Charles Wartchow, PhD, Associate Director, Global Discovery Chemistry, Novartis Institutes for BioMedical Research

An important challenge for ligase-based targeted protein degradation (TPD) is identifying new ligands for existing ligases. Because ubiquitin ligases are usually part of a multi-subunit protein that contains one or more binding partners, hit-finding assays need to differentiate binding locations. To identify new chemotypes for the VHL and cereblon ligases, we used various hit finding methods including fragment screening. I will describe our results and the complexities we encountered.

11:30 am

Search for Selective Inhibitors of Tau-Tubulin Kinase 1 (TTBK1) Using a Fragment-Based Lead-Discovery Approach

Sriram Tyagarajan, Associate Principal Scientist, Discovery Chemistry, Merck Sharp & Dohme LLC

A fragment-based screening strategy was employed to identify allosteric binders for tau tubulin kinase 1 (TTBK1). Several hit classes identified by leveraging biophysical, computational, and crystallographic approaches were prioritized based on the biophysical profile, potential ligandability, and potential of binding site for inhibitory selectivity. The identified allosteric pockets and corresponding fragment hits will be discussed with regard to their potential and early elaboration to provide kinome selectivity for TTBK1.

Close of Fragment-Based Drug Discovery Conference12:00 pm