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Literature DB >> 18225861

synthesis and biological evaluation of fully functionalized seco-pancratistatin analogues.

James McNulty¹, Jerald J Nair, Carly Griffin, Siyaram Pandey.

Abstract

The total synthesis of fully functionalized polyhydroxyamide B,C- seco-analogues of the anticancer compound pancratistatin (PST) ( 1) is reported. Key steps include an Evans' MgCl 2-promoted anti-aldol reaction between a functionalized l-threose derivative and ( R)-(+)-oxazolidinone to stereoselectively form the C-1/C-10b bond and a regiospecific radical-mediated oxidative fragmentation of a 1,3-benzylidene. The B,C- seco compounds 25 and 26 exhibited low activity (ED 50 > 30 microg/mL) for inducing apoptosis in human cancer cells.

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Year: 2008 PMID： 18225861 DOI： 10.1021/np0705460

Source DB: PubMed Journal: J Nat Prod ISSN： 0163-3864 Impact factor: 4.050

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Cited

10 in total

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2. A novel synthetic C-1 analogue of 7-deoxypancratistatin induces apoptosis in p53 positive and negative human colorectal cancer cells by targeting the mitochondria: enhancement of activity by tamoxifen.

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6. Synthesis of structurally simplified analogues of pancratistatin: truncation of the cyclitol ring.

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9. Potential anti-proliferative effects of chemical constituents and hemisynthetic derivatives from Scadoxus pseudocaulus (Amarillydaceae).

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10. Structure-activity studies on the lycorine pharmacophore: A potent inducer of apoptosis in human leukemia cells.

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