| Literature DB >> 32614585 |
Kenneth V Lawson1, Jaroslaw Kalisiak1, Erick A Lindsey1, Eric T Newcomb1, Manmohan Reddy Leleti1, Laurent Debien1, Brandon R Rosen1, Dillon H Miles1, Ehesan U Sharif1, Jenna L Jeffrey1, Joanne B L Tan1, Ada Chen1, Sharon Zhao1, Guifen Xu1, Lijuan Fu1, Lixia Jin1, Tim W Park1, Wade Berry1, Susanne Moschütz2, Emma Scaletti2, Norbert Sträter2, Nigel P Walker1, Stephen W Young1, Matthew J Walters1, Uli Schindler1, Jay P Powers1.
Abstract
Extracellular adenosine (ADO), present in high concentrations in the tumor microenvironment (TME), suppresses immune function via inhibition of T cell and NK cell activation. Intratumoral generation of ADO depends on the sequential catabolism of ATP by two ecto-nucleotidases, CD39 (ATP → AMP) and CD73 (AMP → ADO). Inhibition of CD73 eliminates a major pathway of ADO production in the TME and can reverse ADO-mediated immune suppression. Extensive interrogation of structure-activity relationships (SARs), structure-based drug design, and optimization of pharmacokinetic properties culminated in the discovery of AB680, a highly potent (Ki = 5 pM), reversible, and selective inhibitor of CD73. AB680 is further characterized by very low clearance and long half-lives across preclinical species, resulting in a PK profile suitable for long-acting parenteral administration. AB680 is currently being evaluated in phase 1 clinical trials. Initial data show AB680 is well tolerated and exhibits a pharmacokinetic profile suitable for biweekly (Q2W) iv-administration in human.Entities:
Year: 2020 PMID: 32614585 DOI: 10.1021/acs.jmedchem.0c00525
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446