Valproic acid induces apoptosis dependent of Yca1p at concentrations that mildly affect the proliferation of yeast

Mitsui, Kazuhiro; Nakagawa, Daichi; Nakamura, Masahiro; Okamoto, Taro; Tsurugi, Kunio

doi:10.1016/j.febslet.2004.12.051

Cited by 49 publications

(43 citation statements)

References 18 publications

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“…However, apoptotic death induced by VPA in S. pombe and S. cerevisiae showed several differences. In S. cerevisiae, apoptotic death induced by VPA is dependent on metacaspase 22) and the Sir2 mutation makes cells resistant to VPA, 30) but as shown in Fig. 6, a pca1 mutant and a sir2 mutant of S. pombe showed sensitivity similar to VPA as the wild type.…”

Section: Discussionmentioning

confidence: 99%

“…pombe treated with VPA died with apoptotic markers Since S. cerevisiae died apoptotically when treated with VPA, 22) it was inferred that S. pombe also died apoptotically with VPA. We tested several apoptotic markers in S. pombe cells treated with VPA.…”

Section: Resultsmentioning

confidence: 99%

“…Fungi have a homologous enzyme, metacaspase. Disruption of the metacaspase gene of S. cerevisiae abrogated the apoptotic death caused by VPA 22) and H 2 O 2 . 29) We tested the effects of disruption of the metacaspase gene on VPA-induced cell death in S. pombe.…”

Section: Defects In Metacaspase and Sir2 Did Not Affect Sensitivity Tmentioning

confidence: 99%

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Apoptotic Cell Death in the Fission YeastSchizosaccharomyces pombeInduced by Valproic Acid and Its Extreme Susceptibility to pH Change

Mutoh

Kitajima

Ichihara

2011

Bioscience, Biotechnology, and Biochemistry

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Schizosaccharomyces pombe treated with valproic acid died with apoptotic markers such as DNA fragmentation, loss of a mitochondrial electrochemial gradient and chromatin condensation, independently of metacaspase, a yeast homolog of metazoan caspase. Sensitivity to valproic acid was strongly dependent on growth phase. Cells in a later growth phase were much more sensitive to valproic acid than those in an earlier one. Altering the pH of the medium with HCl and with NaOH also caused remarkable changes in sensitivity. Cells in an acidic medium were more sensitive to valproic acid. This pH-dependent change in sensitivity did not require de novo protein synthesis, and a change in pH 60 min after the administration of valproic acid affected sensitivity. These results suggest that the intracellular cell death process was susceptible to extracellular pH. Although a sir2 mutant of Saccharomyces cerevisiae has been reported to be resistant to valproic acid, mutations in sir2 did not affect the sensitivity to valproic acid of S. pombe.

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Section: Discussionmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Apoptotic Cell Death in the Fission YeastSchizosaccharomyces pombeInduced by Valproic Acid and Its Extreme Susceptibility to pH Change

Mutoh

Kitajima

Ichihara

2011

Bioscience, Biotechnology, and Biochemistry

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“…Furthermore, we found [9] that a mutation in the ARL1 encoding ADP-ribosylation factorlike protein 1, which functions in vesicular transport in both exocytic and endocytic pathways, caused a defect in central vacuole formation and delayed the progress of autophagic death in cdc28 and also that Bax-induced cell death. We reported recently [10] that valproic acid (VPA, 2-propylpentanoic acid) induced apoptosis in an YCA1-dependent manner when the cell's proliferative activity is mildly impaired by low concentration of VPA, whereas they die via autophagic death when it is impaired severely or completely. The mechanism of apoptosis induced by low concentration of VPA in yeast has not been clarified so far.…”

Section: Introductionmentioning

confidence: 99%

Valproate induces apoptosis by inducing accumulation of neutral lipids which was prevented by disruption of the SIR2 gene in Saccharomyces cerevisiae

Sun

et al. 2007

FEBS Letters

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We investigated the participation of HDACs in VPA induced apoptosis in Saccharomyces cerevisiae. VPA (20 mM) induced apoptosis in several HDAC mutants, including PRD3 and HDA1-disrupted cells and SIR2 over expressing cells, as well as in wild-type cells but not SIR2-disrupted cells. Intracellular reactive oxygen species and neutral lipid content increased markedly in all kinds of HDAC mutant cells tested except for SIR2-disrupted cells. Thus, these results suggest that 20 mM VPA induces neutral lipid accumulation and apoptosis-like features in S. cerevisiae, and that VPA-induced apoptosis was evaded by deletion of SIR2.

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“…Additionally, yeasts possess several orthologs of mammalian celldeath mediators . Metacaspase Yca1 in S. cerevisiae was shown to undergo caspase-like proteolytic processing and mediate apoptosis under a wide range of stimuli, including in conditions involving hydrogen peroxide, acetic acid, chronological aging, hyper-osmotic shock, viral killer toxins, valproic acid, deleterious mutations in mRNA decapping, DNA replication and protein deubiquitylation, and heterologous expression of α-synuclein (Bettiga et al, 2004;Flower et al, 2005;Madeo et al, 2002;Mazzoni et al, 2005;Mitsui et al, 2005;Reiter et al, 2005;Silva et al, 2005;Weinberger et al, 2005). Overexpression of Trypanosoma brucei metacaspase promotes mitochondrion-associated cell death in S. cerevisiae, and Leishmania major metacaspase can functionally replace S. cerevisiae Yca1, alluding to the functional conservation of metacaspases in lower eukaryotes (Gonzalez et al, 2007;Szallies et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

Caspase-dependent and -independent lipotoxic cell-death pathways in fission yeast

Low

Shui

Liew

et al. 2008

Journal of Cell Science

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Understanding the mechanisms underlying lipid-induced cell death has significant implications in both cell biology and human diseases. Previously, we showed that fission-yeast Schizosaccharomyces pombe cells deficient in triacylglycerol synthesis display apoptotic markers upon entry into stationary phase. Here, we characterize the sequential molecular events that take place at the onset of cell death in S. pombe, including a surge of diacylglycerol, post-mitotic arrest, alterations in mitochondrial activities and in intracellular redox balance, chromatin condensation, nuclear-envelope fragmentation, and eventually plasma-membrane permeabilization. Our results demonstrated active roles of mitochondria and reactive oxygen species in cell death, and identified novel cell-death regulators – including metacaspase Pca1, BH3-domain protein Rad9, and diacylglycerol-binding proteins Pck1 and Bzz1. Most importantly, we show that, under different conditions and stimuli, failure to maintain intracellular-lipid homeostasis can lead to cell death with different phenotypic manifestations, genetic criteria and cellular mechanisms, pointing to the existence of multiple lipotoxic pathways in this organism. Our study represents the first in-depth analysis of cell-death pathways in S. pombe.

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Valproic acid induces apoptosis dependent of Yca1p at concentrations that mildly affect the proliferation of yeast

Cited by 49 publications

References 18 publications

Apoptotic Cell Death in the Fission YeastSchizosaccharomyces pombeInduced by Valproic Acid and Its Extreme Susceptibility to pH Change

Apoptotic Cell Death in the Fission YeastSchizosaccharomyces pombeInduced by Valproic Acid and Its Extreme Susceptibility to pH Change

Valproate induces apoptosis by inducing accumulation of neutral lipids which was prevented by disruption of the SIR2 gene in Saccharomyces cerevisiae

Caspase-dependent and -independent lipotoxic cell-death pathways in fission yeast

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