Identification of the Privileged Position in the Imidazo[1,2-a]pyridine Ring of Phosphonocarboxylates for Development of Rab Geranylgeranyl Transferase (RGGT) Inhibitors

6533b858fe1ef96bd12b6472

RESEARCH PRODUCT

Identification of the Privileged Position in the Imidazo[1,2-a]pyridine Ring of Phosphonocarboxylates for Development of Rab Geranylgeranyl Transferase (RGGT) Inhibitors

Aleksandra Kaźmierczak Edyta Gendaszewska-darmach Damian Kusy Joanna Gmach Sanna Niinivehmas Olli T. Pentikäinen Olli T. Pentikäinen Katarzyna M. Błażewska ŁUkasz Joachimiak

subject

0301 basic medicine Molecular model Pyridines Organophosphonates Protein Prenylation Antineoplastic Agents GTPase 01 natural sciences HeLa 03 medical and health sciences Structure-Activity Relationship Geranylgeranylation Prenylation Drug Discovery Structure–activity relationship Humans Enzyme Inhibitors ta116 Cell Proliferation chemistry.chemical_classification Alkyl and Aryl Transferases biology 010405 organic chemistry rab geranylgeranyl transferase ta1182 biology.organism_classification 0104 chemical sciences Cell biology Molecular Docking Simulation 030104 developmental biology Enzyme chemistry Biochemistry rab GTP-Binding Proteins Molecular Medicine Rab HeLa Cells

description

Members of the Rab GTPase family are master regulators of vesicle trafficking. When disregulated, they are associated with a number of pathological states. The inhibition of RGGT, an enzyme responsible for post-translational geranylgeranylation of Rab GTPases represents one way to control the activity of these proteins. Because the number of molecules modulating RGGT is limited, we combined molecular modeling with biological assays to ascertain how modifications of phosphonocarboxylates, the first reported RGGT inhibitors, rationally improve understanding of their structure-activity relationship. We have identified the privileged position in the core scaffold of the imidazo[1,2-a]pyridine ring, which can be modified without compromising compounds' potency. Thus modified compounds are micromolar inhibitors of Rab11A prenylation, simultaneously being inactive against Rap1A/Rap1B modification, with the ability to inhibit proliferation of the HeLa cancer cell line. These findings were rationalized by molecular docking, which recognized interaction of phosphonic and carboxylic groups as decisive in phosphonocarboxylate localization in the RGGT binding site.

year	journal	country	edition	language
2017-01-01	Journal of Medicinal Chemistry

10.1021/acs.jmedchem.7b00811 https://doi.org/10.1021/acs.jmedchem.7b00811