1996
DOI: 10.1021/jm960251b
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Synthesis, Biological Activity, and SARs of Pyrrolobenzoxazepine Derivatives, a New Class of Specific “Peripheral-Type” Benzodiazepine Receptor Ligands

Abstract: The "peripheral-type" benzodiazepine receptor (PBR) has been reported to play a role in many biological processes. We have synthesized and tested a novel series of PBR ligands based on a pyrrolobenzoxazepine skeleton, in order to provide new receptor ligands. Several of these new compounds proved to be high affinity and selective ligands for PBR, and benzoxazepines 17f and 17j were found to be the most potent ligands for this receptor to have been identified to date. The SAR and the molecular modeling studies … Show more

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Cited by 90 publications
(70 citation statements)
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“…OXA-17f and OXA-17j (Fig. 6, Table 3) were reported as the most potent PBR ligands from this series with K i values of 0.26 and 0.36 nM respectively compared to K i value of 0.78 nM for PK 11195 in the same assay [39]. These benzoxazepines were shown to be inactive on GABA A and CBRs and were thus found to be highly selective for the PBR.…”
Section: Benzoxazepinesmentioning
confidence: 76%
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“…OXA-17f and OXA-17j (Fig. 6, Table 3) were reported as the most potent PBR ligands from this series with K i values of 0.26 and 0.36 nM respectively compared to K i value of 0.78 nM for PK 11195 in the same assay [39]. These benzoxazepines were shown to be inactive on GABA A and CBRs and were thus found to be highly selective for the PBR.…”
Section: Benzoxazepinesmentioning
confidence: 76%
“…Over the last few decades various PBR pharmacophores have been postulated by different groups [39][40][41] alongside extensive structure activity relationship (SAR) studies. A hydrogenbond donor group (δ1: usually a carbonyl oxygen), two lipophilic regions (PAR and FRA) and another lipophilic region involved in modulating receptor binding (LA) are the general features of the most recently proposed PBR pharmacophore and are said to be necessary for a ligand to interact with the PBR.…”
Section: Synthetic Ligandsmentioning
confidence: 99%
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“…The 4-acetoxy-5-(1-(naphthyl))naphtho [2,3- ,4] oxazepine (PBOX-15) was synthesized as previously described 16 and dissolved in dimethylsulfoxide (DMSO). The chemotherapeutic agents used were oxaliplatin, kindly provided by Sanofi-Aventis Research, and 5-Fluorouracil (Sigma Aldrich).…”
Section: Chemicalsmentioning
confidence: 99%
“…16 In particular, PBOX-15 is a tubulin depolymerizing agent displaying a proapoptotic activity in a variety of human solid and hematological malignancies, [16][17][18][19][20][21] with minimal toxicity toward normal blood and bone marrow cells. 17 In the present study we identified PBOX-15 as a submicromolar selective inhibitor of FAAH enzyme (IC50= 0.843 mM) and we investigated the anti-tumor efficacy and mode of action of this compound on CRC cell lines.…”
Section: Introductionmentioning
confidence: 99%