2016
DOI: 10.1021/jacs.6b02075
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Synthesis and Biological Investigation of Δ12-Prostaglandin J312-PGJ3) Analogues and Related Compounds

Abstract: A series of Δ(12)-prostaglandin J3 (Δ(12)-PGJ3) analogues and derivatives were synthesized employing an array of synthetic strategies developed specifically to render them readily available for biological investigations. The synthesized compounds were evaluated for their cytotoxicity against a number of cancer cell lines, revealing nanomolar potencies for a number of them against certain cancer cell lines. Four analogues (2, 11, 21, and 27) demonstrated inhibition of nuclear export through a covalent addition … Show more

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Cited by 38 publications
(18 citation statements)
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“…63 – 65 ). Compound 63 was also tested in a mouse model at the NCI for its toxicity and was found to be tolerated up to 200 mg/kg per dose (athymic nude mice; intraperitoneally administered) . These results bode well for further optimization to potential preclinical candidates for in vivo efficacy studies and eventually perhaps clinical trials.…”
Section: Applications Of Total Synthesis To Potential Cancer Therapiesmentioning
confidence: 93%
“…63 – 65 ). Compound 63 was also tested in a mouse model at the NCI for its toxicity and was found to be tolerated up to 200 mg/kg per dose (athymic nude mice; intraperitoneally administered) . These results bode well for further optimization to potential preclinical candidates for in vivo efficacy studies and eventually perhaps clinical trials.…”
Section: Applications Of Total Synthesis To Potential Cancer Therapiesmentioning
confidence: 93%
“…Nicolaou and co‐workers recently reported several strategies for the total syntheses of Δ 12 ‐PGJ 3 . These strategies were subsequently applied to the development of a series of even more potent analogues as potential clinical candidates for stem cell cancer treatment, making this an even more sought‐after target . We have previously used 1 to form the C12−C13 bond (prostaglandin numbering) in the syntheses of a variety of prostanoids through conjugate addition of a nucleophile to the electrophilic enal moiety (Scheme A).…”
Section: Methodsmentioning
confidence: 99%
“…In order to construct Δ 12 ‐PGJ 3, disconnection of the C12−C13 bond through an aldol/dehydration reaction sequence would require β‐boryl aldehyde 8 and enone 9 (Scheme B). This type of aldol/dehydration strategy was originally reported by Kobayashi and has subsequently been applied to the syntheses of Δ 12 ‐PGJ 3 3 , and other closely related prostaglandins . Boryl aldehyde 8 was selected as a masked hydroxy aldehyde equivalent because it can be easily prepared by catalytic enantioselective conjugate borylation, and subsequently unmasked later in the synthesis by stereospecific oxidation of the boronic ester.…”
Section: Methodsmentioning
confidence: 99%
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“…Macrocyclization of therapeutically interesting compounds has proven to beneficially effect the selectivity and activity, especially when applied to peptides and carbohydrates . However, there are also excellent cases of macrocyclizations of non‐peptide natural products, for example the microtubule‐stabilizing diterpenoid docetaxel and the antileukemic agent Δ 12 ‐prostaglandin J 3 . Additionally, completely artificial macrocycles based on acyclic lead structures have been reported abundantly …”
Section: Introductionmentioning
confidence: 99%