| Literature DB >> 25016230 |
Fraser P Coxon1, Lukasz Joachimiak2, Arafath Kaja Najumudeen3, George Breen1, Joanna Gmach2, Christina Oetken-Lindholm3, Rebecca Way1, James E Dunford4, Daniel Abankwa3, Katarzyna M Błażewska5.
Abstract
Phosphonocarboxylate (PC) analogs of the anti-osteoporotic drugs, bisphosphonates, represent the first class of selective inhibitors of Rab geranylgeranyl transferase (RabGGTase, RGGT), an enzyme implicated in several diseases including ovarian, breast and skin cancer. Here we present the synthesis and biological characterization of an extended set of this class of compounds, including lipophilic derivatives of the known RGGT inhibitors. From this new panel of PCs, we have identified an inhibitor of RGGT that is of similar potency as the most active published phosphonocarboxylate, but of higher selectivity towards this enzyme compared to prenyl pyrophosphate synthases. New insights into structural requirements are also presented, showing that only PC analogs of the most potent 3rd generation bisphosphonates inhibit RGGT. In addition, the first phosphonocarboxylate-derived GGPPS inhibitor is reported.Entities:
Keywords: Bisphosphonates; GGPPS; Geranylgeranylation; Phosphonocarboxylates; RGGT
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Year: 2014 PMID: 25016230 DOI: 10.1016/j.ejmech.2014.06.062
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514