The Anticancer Natural Product Pironetin Selectively Targets Lys352 of α-Tubulin

Usui, Takeo; Watanabe, Hiroyuki; Nakayama, Hiroshi; Tada, Yukio; Kanoh, Naoki; Kondoh, Masuo; Asao, Tetsuji; Takio, Koji; Watanabe, Hidenobu; Nishikawa, Kiyohiro; Kitahara, Takeshi; Osada, Hiroyuki

doi:10.1016/j.chembiol.2004.03.028

Cited by 97 publications

(76 citation statements)

References 33 publications

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“…Because IEJLs possess a Michael addition-type reactive portion, the irreversibility of IEJLs might be owing to the covalent binding to target molecules like leptomycin B, pironetin, amphidinolide H, and so on. [22][23][24] However, since reducing reagent dithiothreitol, which inactivates the reactivity of most Michael addition-type inhibitors, did not interfere with V-ATPase inhibition by IEJLs (data not shown), covalent binding might not be necessary for V-ATPase inhibition as in the case of PP2A inhibitors fostriecin/ phoslactomycins. 25,26) Further investigation is required to clarify whether IEJLs covalently bind targets molecules.…”

Section: Discussionmentioning

confidence: 99%

Iejimalides Show Anti-Osteoclast ActivityviaV-ATPase Inhibition

Kazami

Muroi²,

Kawatani³

et al. 2006

Bioscience, Biotechnology, and Biochemistry

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Iejimalides (IEJLs), 24-membered macrolides, are potent antitumor compounds, but their molecular targets remain to be revealed. In the course of screening, we identified IEJLs as potent osteoclast inhibitors. Since it is known that osteoclasts are sensitive to vacuolar H þ -ATPase (V-ATPase) inhibitor, we investigated the effect of IEJLs on V-ATPases. IEJLs inhibited the V-ATPases of both mammalian and yeast cells in situ, and of yeast V-ATPases in vitro. A bafilomycin-resistant yeast mutant conferred IEJL resistance, suggesting that IEJLs bind a site similar to the bafilomycins/concanamycins-binding site. These results indicate that IEJLs are novel V-ATPase inhibitors, and that antitumor and antiosteporotic activities are exerted via V-ATPase inhibition.

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Section: Discussionmentioning

confidence: 99%

Iejimalides Show Anti-Osteoclast ActivityviaV-ATPase Inhibition

Kazami

Muroi²,

Kawatani³

et al. 2006

Bioscience, Biotechnology, and Biochemistry

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“…2). To date, some bioactive compounds containing a,b-unsaturated lactone have been reported to bind to proteins by Michael addition, a reaction that is likely to be non-specific to biological nucleophiles such as cysteine residues; however, it has been shown that the binding of some compounds such as leptomycin B [28], and pironetin [6] to targeted proteins proceeds in a site and/or protein-specific manner. As for PP2A inhibitors, although it is speculated that fostriecin covalently binds to PP2Ac through the unsatulated lactone, the direct evidence has not yet been reported.…”

Section: Discussionmentioning

confidence: 99%

“…To date, several bioactive chemicals and their target proteins have been reported. One such example would be pironetin, which binds to Lys-352 of a-tubulin, inhibits tubulin assembly, and arrests cell cycle progression in M phase [6]. Another example reported to date is amphidinolide H, which binds to Tyr-200 of actin subdomain 4 and stimulates the formation of small actin-patches, followed by F-actin rearrangement into aggregates via the retraction of actin fibers [7].…”

Section: Introductionmentioning

confidence: 99%

Phoslactomycin targets cysteine‐269 of the protein phosphatase 2A catalytic subunit in cells

et al. 2005

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According to the chemical genetic approach, small molecules that bind directly to proteins are used to analyze protein function, thereby enabling the elucidation of complex mechanisms in mammal cells. Thus, it is very important to identify the molecular targets of compounds that induce a unique phenotype in a target cell. Phoslactomycin A (PLMA) is known to be a potent inhibitor of protein Ser/Thr phosphatase 2A (PP2A); however, the inhibitory mechanism of PP2A by PLMA has not yet been elucidated. Here, we demonstrated that PLMA directly binds to the PP2A catalytic subunit (PP2Ac) in cells by using biotinylated PLMA, and the PLMA-binding site was identified as the Cys-269 residue of PP2Ac. Moreover, we revealed that the Cys-269 contributes to the potent inhibition of PP2Ac activity by PLMA. These results suggest that PLMA is a PP2A-selective inhibitor and is therefore expected to be useful for future investigation of PP2A function in cells.

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“…Pironetin covalently binds to Lys352 of a-tubulin and inhibits the interaction of tubulin heterodimers (Usui et al, 2004). A JNK inhibitor, SP600125, was purchased from Tocris Cookson Inc. (Ellisville, MO, USA).…”

Section: Methodsmentioning

confidence: 99%