| Literature DB >> 33658076 |
Leen Kalash1,2, Ian Winfield1,3, Dewi Safitri3,4, Marcel Bermudez1,5, Sabrina Carvalho3, Robert Glen1,6, Graham Ladds7, Andreas Bender8.
Abstract
Enhanced/prolonged cAMP signalling has been suggested as a suppressor of cancer proliferation. Interestingly, two key modulators that elevate cAMP, the A2A receptor (A2AR) and phosphodiesterase 10A (PDE10A), are differentially co-expressed in various types of non-small lung cancer (NSCLC) cell-lines. Thus, finding dual-target compounds, which are simultaneously agonists at the A2AR whilst also inhibiting PDE10A, could be a novel anti-proliferative approach. Using ligand- and structure-based modelling combined with MD simulations (which identified Val84 displacement as a novel conformational descriptor of A2AR activation), a series of known PDE10A inhibitors were shown to dock to the orthosteric site of the A2AR. Subsequent in-vitro analysis confirmed that these compounds bind to the A2AR and exhibit dual-activity at both the A2AR and PDE10A. Furthermore, many of the compounds exhibited promising anti-proliferative effects upon NSCLC cell-lines, which directly correlated with the expression of both PDE10A and the A2AR. Thus, we propose a structure-based methodology, which has been validated in in-vitro binding and functional assays, and demonstrated a promising therapeutic value.Entities:
Keywords: A2AR; Anti‐proliferative; Docking; Dual target; Lung cancer; MD simulations; NSCLC; PDE10A; Structure‐based design; Triazoloquinazolines; Virtual screening
Year: 2021 PMID: 33658076 PMCID: PMC7927403 DOI: 10.1186/s13321-021-00492-5
Source DB: PubMed Journal: J Cheminform ISSN: 1758-2946 Impact factor: 5.514