Mechanism of Thiazolidinedione-Dependent Cell Death in Jurkat T Cells

Soller, Mathias; Dröse, Stefan; Brandt, Ulrich; Brüne, Bernhard; Knethen, Andreas von

doi:10.1124/mol.107.034371

Cited by 31 publications

(11 citation statements)

References 40 publications

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“…That CII is of importance in ROS formation is further evidenced by a recent report showing that non-steroid anti-inflammatory drugs caused ROS generation in cells, of which the majority was derived from CII (Soller et al, 2007). Moreover, ferulenol, a coumarine derivative, has been reported to affect the succinate UbQ reductase by interfering with the UbQ cycle (Lahouel et al, 2007).…”

Section: Complex II As An Anti-cancer Drug Target L-f Dong Et Almentioning

confidence: 90%

α-Tocopheryl succinate induces apoptosis by targeting ubiquinone-binding sites in mitochondrial respiratory complex II

et al. 2008

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a-Tocopheryl succinate (a-TOS) is a selective inducer of apoptosis in cancer cells, which involves the accumulation of reactive oxygen species (ROS). The molecular target of a-TOS has not been identified. Here, we show that a-TOS inhibits succinate dehydrogenase (SDH) activity of complex II (CII) by interacting with the proximal and distal ubiquinone (UbQ)-binding site (Q P and Q D , respectively). This is based on biochemical analyses and molecular modelling, revealing similar or stronger interaction energy of a-TOS compared to that of UbQ for the Q P and Q D sites, respectively. CybL-mutant cells with dysfunctional CII failed to accumulate ROS and underwent apoptosis in the presence of a-TOS. Similar resistance was observed when CybL was knocked down with siRNA. Reconstitution of functional CII rendered CybL-mutant cells susceptible to a-TOS. We propose that a-TOS displaces UbQ in CII causing electrons generated by SDH to recombine with molecular oxygen to yield ROS. Our data highlight CII, a known tumour suppressor, as a novel target for cancer therapy.

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Section: Complex II As An Anti-cancer Drug Target L-f Dong Et Almentioning

confidence: 90%

α-Tocopheryl succinate induces apoptosis by targeting ubiquinone-binding sites in mitochondrial respiratory complex II

et al. 2008

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“…However, in contrast to a-TOS, its practical application as an anticancer agent is restricted, as it is also very toxic to noncancerous cells, such as hepatocytes (226). Interestingly, the anti-diabetic and antiinflammatory drug, troglitazone, which contains the atocopheryl moiety similar to a-TOS, also interferes with CII activity (186). The drug was registered, but was subsequently withdrawn from the clinic due to liver toxicity (85).…”

Section: Complex IImentioning

confidence: 98%

Anticancer Drugs Targeting the Mitochondrial Electron Transport Chain

Rohlena

Dong

Ralph

et al. 2011

Antioxidants & Redox Signaling

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“…Different studies demonstrated that inhibition of complex II governs a direct apoptotic process in neurons through cell-specific pathways. It was recently shown that neurons, which require high levels of energy, are sensitive to complex II-induced OxPhos impairment and this results in a rapid ATP decrease (Mandavilli et al, 2005;Liot et al, 2009;Mbaya et al, 2010), contrary to other cell types, which did not show such a rapid ATP drop in response to complex II inhibition by a SDHC mutant or by the inhibitor thenoyltrifluoroacetate (Senoo-Matsuda et al, 2001;Ishii et al, 2007;Soller et al, 2007;Byun et al, 2008). In neurons, this ATP decrease induced by either 3-nitropropionate, aptenin or a SDHA mutant causes a profound alteration of the intracellular and mitochondrial calcium homeostasis, which then leads to an amplification of mitochondrial ROS formation by complex II and probably by other sources, DC M loss and finally neuronal apoptotic cell death (Liot et al, 2009;Mbaya et al, 2010).…”

Section: Respiratory Chain Complexes and Apoptosis A Lemarie And S Grimmmentioning

confidence: 99%

Mitochondrial respiratory chain complexes: apoptosis sensors mutated in cancer?

2011

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Mutations in cancer cells affecting subunits of the respiratory chain (RC) indicate a central role of oxidative phosphorylation for tumourigenesis. Recent studies have suggested that such mutations of RC complexes impact apoptosis induction. We review here the evidence for this hypothesis, which in particular emerged from work on how complex I and II mediate signals for apoptosis. Both protein aggregates are specifically inhibited for apoptosis induction through different means by exploiting with protease activation and pH change, two widespread but independent features of dying cells. Nevertheless, both converge on forming reactive oxygen species for the demise of the cell. Investigations into these mitochondrial processes will remain a rewarding area for unravelling the causes of tumourigenesis and for discovering interference options.

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Mechanism of Thiazolidinedione-Dependent Cell Death in Jurkat T Cells

Cited by 31 publications

References 40 publications

α-Tocopheryl succinate induces apoptosis by targeting ubiquinone-binding sites in mitochondrial respiratory complex II

α-Tocopheryl succinate induces apoptosis by targeting ubiquinone-binding sites in mitochondrial respiratory complex II

Anticancer Drugs Targeting the Mitochondrial Electron Transport Chain

Mitochondrial respiratory chain complexes: apoptosis sensors mutated in cancer?

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