Use of AD Informer Set compounds to explore validity of novel targets in Alzheimer's disease pathology

Frances M Potjewyd; Joel K Annor-Gyamfi; Jeffrey Aubé; Shaoyou Chu; Ivie L Conlon; Kevin J Frankowski; Shiva K R Guduru; Brian P Hardy; Megan D Hopkins; Chizuru Kinoshita; Dmitri B Kireev; Emily R Mason; Charles T Moerk; Felix Nwogbo; Kenneth H Pearce Jr; Timothy I Richardson; David A Rogers; Disha M Soni; Michael Stashko; Xiaodong Wang; Carrow Wells; Timothy M Willson; Stephen V Frye; Jessica E Young; Alison D Axtman

doi:10.1002/trc2.12253

Use of AD Informer Set compounds to explore validity of novel targets in Alzheimer's disease pathology

Alzheimers Dement (N Y). 2022 Apr 12;8(1):e12253. doi: 10.1002/trc2.12253. eCollection 2022.

Authors

Frances M Potjewyd¹, Joel K Annor-Gyamfi¹, Jeffrey Aubé², Shaoyou Chu³, Ivie L Conlon², Kevin J Frankowski², Shiva K R Guduru², Brian P Hardy², Megan D Hopkins², Chizuru Kinoshita^{3

4}, Dmitri B Kireev², Emily R Mason⁵, Charles T Moerk^{3

4}, Felix Nwogbo², Kenneth H Pearce Jr², Timothy I Richardson⁵, David A Rogers², Disha M Soni⁵, Michael Stashko², Xiaodong Wang², Carrow Wells¹, Timothy M Willson¹, Stephen V Frye², Jessica E Young^{3

4}, Alison D Axtman¹

Affiliations

¹ UNC Eshelman School of Pharmacy Division of Chemical Biology and Medicinal Chemistry Structural Genomics Consortium Chapel Hill North Carolina USA.
² UNC Eshelman School of Pharmacy Division of Chemical Biology and Medicinal Chemistry Center for Integrative Chemical Biology and Drug Discovery Chapel Hill North Carolina USA.
³ Department of Laboratory Medicine and Pathology University of Washington Seattle Washington USA.
⁴ Institute for Stem Cell and Regenerative Medicine University of Washington Seattle Washington USA.
⁵ Department of Medicine Division of Clinical Pharmacology Indiana University School of Medicine Indianapolis Indiana USA.

Abstract

Introduction: A chemogenomic set of small molecules with annotated activities and implicated roles in Alzheimer's disease (AD) called the AD Informer Set was recently developed and made available to the AD research community: https://treatad.org/data-tools/ad-informer-set/.

Methods: Small subsets of AD Informer Set compounds were selected for AD-relevant profiling. Nine compounds targeting proteins expressed by six AD-implicated genes prioritized for study by Target Enablement to Accelerate Therapy Development for Alzheimer's Disease (TREAT-AD) teams were selected for G-protein coupled receptor (GPCR), amyloid beta (Aβ) and tau, and pharmacokinetic (PK) studies. Four non-overlapping compounds were analyzed in microglial cytotoxicity and phagocytosis assays.

Results: The nine compounds targeting CAPN2, EPHX2, MDK, MerTK/FLT3, or SYK proteins were profiled in 46 to 47 primary GPCR binding assays. Human induced pluripotent stem cell (iPSC)-derived neurons were treated with the same nine compounds and secretion of Aβ peptides (Aβ40 and Aβ42) as well as levels of phosphophorylated tau (p-tau, Thr231) and total tau (t-tau) peptides measured at two concentrations and two timepoints. Finally, CD1 mice were dosed intravenously to determine preliminary PK and/or brain-specific penetrance values for these compounds. As a final cell-based study, a non-overlapping subset of four compounds was selected based on single-concentration screening for analysis of both cytotoxicity and phagocytosis in murine and human microglia cells.

Discussion: We have demonstrated the utility of the AD Informer Set in the validation of novel AD hypotheses using biochemical, cellular (primary and immortalized), and in vivo studies. The selectivity for their primary targets versus essential GPCRs in the brain was established for our compounds. Statistical changes in tau, p-tau, Aβ40, and/or Aβ42 and blood-brain barrier penetrance were observed, solidifying the utility of specific compounds for AD. Single-concentration phagocytosis results were validated as predictive of dose-response findings. These studies established workflows, validated assays, and illuminated next steps for protein targets and compounds.

Keywords: AD Informer Set; Alzheimer's disease; Target Enablement to Accelerate Therapy Development for Alzheimer's Disease; chemogenomic set; chemogenomics; target validation.

Abstract

Grants and funding