2004
DOI: 10.1039/b411021h
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Synthesis of anti-tumour phosphatidylinositol analogues from glucose by the use of ring-closing olefin metathesis

Abstract: A divergent strategy is described for synthesis of the novel phosphatidylinositols 1-3. The synthetic approach commences from benzyl-protected methyl 6-iodo-6-deoxy-alpha-D-glucopyranoside, which undergoes zinc-mediated reductive fragmentation followed by vinyl Grignard addition and ring-closing metathesis to afford the key conduritol B intermediate 7. This can trifurcate to form three different benzyl-protected myo-inositol headgroups 4-6, which after phosphorylation and attachment of the glycerolipid part gi… Show more

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Cited by 30 publications
(21 citation statements)
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“…Both phospholipase C and PI3K exhibit this enhanced activity with interfacial substrates / inhibitors. 35,36 Since the 3-deoxy-diC 8 PI molecules, unlike the longer acyl chain synthetic 3-deoxy-PI molecules examined previously, 7,14 can exist as both monomers and micelles in solution, we require information on the physical state of the short chain PI analogues, notably their CMC as well as roughly what size micelles they form. This is also critical information for determining the distribution of the 3-deoxy-diC 8 PI species in cells at concentrations where they may cause cell death.…”
Section: Characterization Of Dic 8 Pi Compoundsmentioning
confidence: 99%
“…Both phospholipase C and PI3K exhibit this enhanced activity with interfacial substrates / inhibitors. 35,36 Since the 3-deoxy-diC 8 PI molecules, unlike the longer acyl chain synthetic 3-deoxy-PI molecules examined previously, 7,14 can exist as both monomers and micelles in solution, we require information on the physical state of the short chain PI analogues, notably their CMC as well as roughly what size micelles they form. This is also critical information for determining the distribution of the 3-deoxy-diC 8 PI species in cells at concentrations where they may cause cell death.…”
Section: Characterization Of Dic 8 Pi Compoundsmentioning
confidence: 99%
“…The PTEN active site is rich in charged residues that could interact differently with modified inositol compounds. Limited modeling suggests how PI(1,3,4,5)P 3 might bind in the PTEN active site, but there is no structure to confirm this arrangement, or to suggest where any hydrophobic segments, which are present in all the optimized 3-deoxy-PI inhibitors [2224], might bind. Given its extreme functional importance, understanding how different substrate-like molecules bind to PTEN is critical.…”
Section: Introductionmentioning
confidence: 99%
“…The reason why the chloride reagent gives better selectivity than the bromide reagent is unclear, but similar behaviour has been observed before in related systems. 40 Triol 3a was treated with 2,2-dimethoxypropane and catalytic camphorsulfonic acid, giving the five-membered ring acetonide 4 in a poor 33% yield along with two more products, which were identified as the six-membered (5) and seven-membered (6) ring isomers, respectively (4:5:6; 10:2:5). The regiochemical assignment of 4-6 was made based on 13 C NMR chemical shifts of the acetonide methyl groups and quaternary carbons.…”
Section: Resultsmentioning
confidence: 99%