| Literature DB >> 27593112 |
Dario Diviani1, Francesco Raimondi2, Cosmo D Del Vescovo1, Elisa Dreyer1, Erica Reggi1, Halima Osman1, Lucia Ruggieri1, Cynthia Gonano1, Sabrina Cavin1, Clare L Box3, Marc Lenoir3, Michael Overduin4, Luca Bellucci2, Michele Seeber2, Francesca Fanelli5.
Abstract
Uncontrolled activation of Rho signaling by RhoGEFs, in particular AKAP13 (Lbc) and its close homologs, is implicated in a number of human tumors with poor prognosis and resistance to therapy. Structure predictions and alanine scanning mutagenesis of Lbc identified a circumscribed hot region for RhoA recognition and activation. Virtual screening targeting that region led to the discovery of an inhibitor of Lbc-RhoA interaction inside cells. By interacting with the DH domain, the compound inhibits the catalytic activity of Lbc, halts cellular responses to activation of oncogenic Lbc pathways, and reverses a number of prostate cancer cell phenotypes such as proliferation, migration, and invasiveness. This study provides insights into the structural determinants of Lbc-RhoA recognition. This is a successful example of structure-based discovery of a small protein-protein interaction inhibitor able to halt oncogenic Rho signaling in cancer cells with therapeutic implications.Entities:
Keywords: AKAP13 oncogene; Ras GTPases; RhoGEFs; comparative modeling; virtual screening
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Year: 2016 PMID: 27593112 DOI: 10.1016/j.chembiol.2016.07.015
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116