Total Synthesis and Biological Evaluation of the Protein Phosphatase 2A Inhibitor Cytostatin and Analogues

Bialy, Laurent; Waldmann, Herbert

doi:10.1002/chem.200305543

Cited by 69 publications

(49 citation statements)

References 99 publications

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“…Screening of a BIOS-derived a,b-unsaturated d-lactone compound collection in two cell based screens yielded small molecule modulators of cell cycle progression and of viral entry via the secretory pathway (Leßmann et al, 2007). Extensive screening and synthesis efforts also resulted in highly selective phosphatase inhibitors with enhanced properties (Bialy and Waldmann, 2004;Umarye et al, 2007).…”

Section: Bios Libraries Yield Small Molecule Probes For Different Biomentioning

confidence: 99%

Principles, implementation, and application of biology-oriented synthesis (BIOS)

Wilk¹,

Zimmermann²,

Kaiser

et al. 2010

Biological Chemistry

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Biology-oriented synthesis (BIOS) represents an alternative approach for the generation of compound collections for biological applications. In BIOS, biologically relevant and prevalidated scaffold structures, such as core structures of natural products or known drugs, are employed as scaffolds for the generation of compound collections with focused diversity. In this review, we discuss the underlying concept of the BIOS approach, and its practical implementation in library design and synthesis. To highlight its relevance for chemical biology applications, we finally present examples in which compound collections generated under the BIOS principle have been used to elucidate biological questions.

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Section: Bios Libraries Yield Small Molecule Probes For Different Biomentioning

confidence: 99%

Principles, implementation, and application of biology-oriented synthesis (BIOS)

Wilk¹,

Zimmermann²,

Kaiser

et al. 2010

Biological Chemistry

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“…Subsequently, fostriecin (Walsh et al, 1997;Buck et al, 2003), cytostatin (Bialy and Waldmann, 2004;Lawhorn et al, 2006), and structurally related natural products [phospholine, leustroducsin, and phoslactomycins (Usui et al, 1999;Kawada et al, 2003); Fig. 1] have all been shown to inhibit a subset of PPP-family serine/threonine protein phosphatases.…”

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confidence: 99%

“…Fostriecin acts as a potent inhibitor of PP2A/PP4 (IC 50 0.2-4 nM) and a weak inhibitor of PP1 and PP5 (PP2A/PP4 versus PP1/PP5 selectivity Ͼ10 4 ) (Walsh et al, 1997;Buck et al, 2003). Cytostatin is also a potent and selective inhibitor of PP2A (PP2A IC 50 ϭ 20 -400 nM; PP2A versus PP1/PP5 Ͼ 10 3 ) (Bialy and Waldmann, 2004;Lawhorn et al, 2006). Phospholine, leustroducsin H, and phoslactomycins are weaker inhibitors of PP2A (Usui et al, 1999;Kawada et al, 2003) and have not been examined using other phosphatases.…”

mentioning

confidence: 99%

“…Following the first total synthesis of fostriecin (Boger et al, 2001), at least nine total or formal syntheses have been reported (Chavez and Jacobsen, 2001;Esumi et al, 2002;Reddy and Falck, 2002;Miyashita et al, 2003;Maki et al, 2005;Trost et al, 2005). The total synthesis of cytostatin (Bialy and Waldmann, 2004;Lawhorn et al, 2006;Jung et al, 2008) and cytostatin analogs (Lawhorn et al, 2006;Jung et al, 2008) have also been reported. These studies have sparked renewed interest in the potential for development of more stable derivatives that may have utility as novel antitumor drugs.…”

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confidence: 99%

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Structure-Activity Relationship Studies of Fostriecin, Cytostatin, and Key Analogs, with PP1, PP2A, PP5, and (β12–β13)-Chimeras (PP1/PP2A and PP5/PP2A), Provide Further Insight into the Inhibitory Actions of Fostriecin Family Inhibitors

Swingle¹,

Amable²,

Lawhorn³

et al. 2009

J Pharmacol Exp Ther

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Fostriecin and cytostatin are structurally related natural inhibitors of serine/threonine phosphatases, with promising antitumor activity. The total synthesis of these antitumor agents has enabled the production of structural analogs, which are useful to explore the biological significance of features contained in the parent compounds. Here, the inhibitory activity of fostriecin, cytostatin, and 10 key structural analogs were tested in sideby-side phosphatase assays to further characterize their inhibitory activity against PP1c (Ser/Thr protein phosphatase 1 catalytic subunit), PP2Ac (Ser/Thr protein phosphatase 2A catalytic subunit), PP5c (Ser/Thr protein phosphatase 5 catalytic subunit), and chimeras of PP1 (Ser/Thr protein phosphatase 1) and PP5 (Ser/Thr protein phosphatase 5), in which key residues predicted for inhibitor contact with PP2A (Ser/Thr protein phosphatase 2A) were introduced into PP1 and PP5 using sitedirected mutagenesis. The data confirm the importance of the C9-phosphate and C11-alcohol for general inhibition and further demonstrate the importance of a predicted C3 interaction with a unique cysteine (Cys 269 ) in the ␤12-␤13 loop of PP2A. The data also indicate that additional features beyond the unsaturated lactone contribute to inhibitory potency and selectivity. Notably, a derivative of fostriecin lacking the entire lactone subunit demonstrated marked potency and selectivity for PP2A, while having substantially reduced and similar activity against PP1 and PP1/PP2A-PP5/PP2A-chimeras that have greatly increased sensitivity to both fostriecin and cytostatin. This suggests that other features [e.g., the (Z,Z,E)-triene] also contribute to inhibitory selectivity. When considered together with previous data, these studies suggest that, despite the high structural conservation of the catalytic site in PP1, PP2A and PP5, the development of highly selective catalytic inhibitors should be feasible.Fostriecin and cytostatin are structurally related phosphate monoesters produced by Streptomyces pulveraceus and Streptomyces sp. MJ654-Nf4, respectively, that display cytotoxicity and antitumor activity (for review, see Lewy et al., 2002). Cytostatin has cytotoxic activity toward melanoma and leukemia cell lines and has been shown to inhibit lung tumor metastasis (Masuda et al., 1995;Kawada et al., 1999). The antitumor activity of fostriecin (also called CI-920, NSC 339638, or PD 110,161) has been evaluated extensively (for review, see de Jong et al., 1997;Lewy et al., 2002;Honkanen, 2005). It demonstrates marked cytotoxicity against many cancer cell lines and potent antitumor activity in animals (for

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“…Conversion to Fm-protected phosphate 8 was achieved by a onepot treatment with Fm-substituted diisopropylphosphoramidate followed by oxidation of the resulting trivalent phosphorus to pentavalent phosphorus. [16] The high stability of the Fm groups towards acidic hydrolysis allowed for concomitant cleavage of the TBDPS group and both N-Boc groups with a mixture of HF and HCl to give 3. The terminal amino group of 3 was expected to react regioselectively with the reactive groups of the selected affinity matrix, [9] that is, Affi-Gel 10 loaded with 15 mmol mL À1 of NHS esters linked to the gel beads by decapeptide spacers.…”

Section: Resultsmentioning

confidence: 99%

Synthesis and Immobilization of erythro‐C14‐ω‐Aminosphingosine‐1‐phosphate as a Potential Tool for Affinity Chromatography

et al. 2008

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A sphingosine-1-phosphate (S1P) analogue containing a terminal alkyl chain amino group is synthesized in a few steps via olefin cross-metathesis of an optically resolved intermediate and subsequent phosphorylation. Regioselective acylation of this intermediate at its N terminus in solution is demonstrated as a model reaction and provides a biologically active derivative. Finally, the omega-amino intermediate is immobilized on an affinity matrix. The choice of a UV-active phosphate protecting group allows for quantification of resin loading after cleavage which amounted to 66 %.

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Total Synthesis and Biological Evaluation of the Protein Phosphatase 2A Inhibitor Cytostatin and Analogues

Cited by 69 publications

References 99 publications

Principles, implementation, and application of biology-oriented synthesis (BIOS)

Principles, implementation, and application of biology-oriented synthesis (BIOS)

Structure-Activity Relationship Studies of Fostriecin, Cytostatin, and Key Analogs, with PP1, PP2A, PP5, and (β12–β13)-Chimeras (PP1/PP2A and PP5/PP2A), Provide Further Insight into the Inhibitory Actions of Fostriecin Family Inhibitors

Synthesis and Immobilization of erythro‐C14‐ω‐Aminosphingosine‐1‐phosphate as a Potential Tool for Affinity Chromatography

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