Synthesis, Biochemical, and Cellular Evaluation of Farnesyl Monophosphate Prodrugs As Farnesyltransferase Inhibitors
Overview
Authors
Affiliations
Certain farnesyl diphosphate (FPP) analogs are potent inhibitors of the potential anticancer drug target protein farnesyltransferase (FTase), but these compounds are not suitable as drug candidates. Thus, phosphoramidate prodrug derivatives of the monophosphate precursors of FPP-based FTase inhibitors have been synthesized. The monophosphates themselves were significantly more potent inhibitors of FTase than the corresponding FPP analogs. The effects of the prodrug 5b (a derivative of 3-allylfarnesyl monophosphate) have been evaluated on prenylation of RhoB and on the cell cycle in a human malignant schwannoma cell line (STS-26T). In combination treatments, 1-3 microM 5b plus 1 microM lovastatin induced a significant inhibition of RhoB prenylation, and a combination of these drugs at 1 microM each also resulted in significant cell cycle arrest in G1. Indeed, combinations as low as 50 nM lovastatin + 1 microM 5c or 250 nM lovastatin + 50 nM 5c were highly cytostatic in STS-26T cell culture.
Reiners Jr J, Mathieu P, Gargano M, George I, Shen Y, Callaghan J Cancers (Basel). 2024; 16(1).
PMID: 38201517 PMC: 10778372. DOI: 10.3390/cancers16010089.
Ras and Rap1: A tale of two GTPases.
Shah S, Brock E, Ji K, Mattingly R Semin Cancer Biol. 2018; 54:29-39.
PMID: 29621614 PMC: 6170734. DOI: 10.1016/j.semcancer.2018.03.005.
How to Target Activated Ras Proteins: Direct Inhibition vs. Induced Mislocalization.
Brock E, Ji K, Reiners J, Mattingly R Mini Rev Med Chem. 2015; 16(5):358-69.
PMID: 26423696 PMC: 4955559. DOI: 10.2174/1389557515666151001154002.
Prodrugs of phosphonates and phosphates: crossing the membrane barrier.
Wiemer A, Wiemer D Top Curr Chem. 2014; 360:115-60.
PMID: 25391982 PMC: 4774048. DOI: 10.1007/128_2014_561.
Mattingly R ISRN Oncol. 2013; 2013:536529.
PMID: 24294527 PMC: 3833460. DOI: 10.1155/2013/536529.