2006
DOI: 10.1016/j.bmcl.2006.01.039
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Factor VIIa inhibitors: A prodrug strategy to improve oral bioavailability

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Cited by 28 publications
(19 citation statements)
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“…Researchers at Celera Genomics attempted to improve oral bioavailability of compounds containing a biaryl P1 moiety, 5-amidinoindole. 37 A series of hydroxyl-, alkoxy-, and carbamate-amidine prodrugs were synthesized that showed moderate to good oral absorption of the prodrug in rat (typically 40% to 100%) but poor conversion to parent amidine, resulting in overall oral availability of Ͻ1% to 2% for the amidine drug. The authors noted that previous successes with amidine prodrugs were obtained with mono aryl structures (eg, benzamidine) or alkyl-amidines and hypothesized that the biaryl-amidine prodrugs were not recognized by the enzymatic machinery required for prodrug conversion.…”
Section: Shirk and Vlasukmentioning
confidence: 99%
“…Researchers at Celera Genomics attempted to improve oral bioavailability of compounds containing a biaryl P1 moiety, 5-amidinoindole. 37 A series of hydroxyl-, alkoxy-, and carbamate-amidine prodrugs were synthesized that showed moderate to good oral absorption of the prodrug in rat (typically 40% to 100%) but poor conversion to parent amidine, resulting in overall oral availability of Ͻ1% to 2% for the amidine drug. The authors noted that previous successes with amidine prodrugs were obtained with mono aryl structures (eg, benzamidine) or alkyl-amidines and hypothesized that the biaryl-amidine prodrugs were not recognized by the enzymatic machinery required for prodrug conversion.…”
Section: Shirk and Vlasukmentioning
confidence: 99%
“…Studies evaluating bleeding tendency [120] and surgical blood loss [121] have shown that inhibition earlier in the coagulation cascade, e.g., factor VIIa, may provide an increased These possible safety advantages lead Riggs et al [124] to focus on the development of an oral and selective factor VIIa inhibitor using a orodrug strategy.…”
Section: Iv12 Aromatic Amidoximes Prodrugs Of Amidines As Factor Vmentioning
confidence: 99%
“…1) display a wide range of pharmacological activities and therefore have been explored as a number of potential therapeutic agents [1] e.g. inhibitors of proteases involved in coagulation [23], antagonists of G-protein-coupled receptors [45], anti-angiogenic compounds [6] and inhibitors of endothelinconverting-enzyme [7]. 5-Alkyl substituted indoles e.g.…”
Section: Introductionmentioning
confidence: 99%