Crystal Structure of Mitochondrial Respiratory Membrane Protein Complex II

Sun, Fei; Huang, Xia; Zhai, Yujia; Wang, Aojin; Xu, Jie; Su, Dan; Bartlam, Mark; Rao, Zihe

doi:10.1016/j.cell.2005.05.025

Cited by 701 publications

(703 citation statements)

References 57 publications

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“…UbQ5 was chosen as it is of similar size to a-TOS ( Figure 5e) and contains a similar number of rotatable bonds (16 and 17, respectively). Figure 5a indicates that UbQ5 docked in Q P to a deeper position than that observed for the portion of UbQ resolved in the published crystal structure (Sun et al, 2005). UbQ5 was also found to dock into the proposed Q D site, with the UbQ ring positioned in front of the binding site and the hydrophobic tail located inside the site (Figure 5c).…”

Section: Molecular Modelling Reveals Strong Binding Of A-tosmentioning

confidence: 80%

“…To establish the relationship between inhibition of SDH and 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) reduction, initial experiments with 3BP and 3NPA were performed in the absence of succinate that might otherwise compete for binding to the enzyme, and the results confirmed that 3BP and 3NPA inhibited CII-mediated MTT reduction and that SDH activity and MTT reduction were closely related ( Figure 2a). Thenoyltrifluoroacetone (TTFA) is an inhibitor of CII that blocks the succinate-dependent MTT reduction by targeting the UbQ-binding sites rather than the SDH enzyme catalytic site (Sun et al, 2005). The CII UbQ sites are situated beneath the active site of SDH, in the transmembrane region of the CII.…”

Section: Resultsmentioning

confidence: 99%

“…Also, data analysis from the published crystal structure only shows electron density for the very start of the isoprenoid chain suggesting that the rest of the tail is not particularly tightly bound at this site (Sun et al, 2005). Therefore, the expected interaction energies of UbQ10 for the two sites will be similar to those calculated for UbQ5.…”

Section: Molecular Modelling Reveals Strong Binding Of A-tosmentioning

confidence: 87%

“…MitoQ overcame both the TTFAand a-TOS-mediated inhibition of SDH activity. While TTFA binds to both Q P and Q D sites in CII (Sun et al, 2005) like a-TOS, it displays less selective toxicity ) than the VE analogue for killing cancer cells (Neuzil et al, 2001b). Further studies are required to understand this differential specificity.…”

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

confidence: 99%

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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: Molecular Modelling Reveals Strong Binding Of A-tosmentioning

confidence: 80%

Section: Resultsmentioning

confidence: 99%

Section: Molecular Modelling Reveals Strong Binding Of A-tosmentioning

confidence: 87%

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

confidence: 99%

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

et al. 2008

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“…More recently, investigators have begun to identify some of the molecules required for mitophagy. (Sun et al, 2005). bc 1 , cytochrome c reductase; CcO, cytochrome c oxidase; Cyc, cytochrome c; Fe/S, iron/sulphur; SDH, succinate dehydrogenase.…”

Section: Molecular Events During Mitophagymentioning

confidence: 99%

Shaping the mitochondrion: mitochondrial biogenesis, dynamics and dysfunction

Shaw

Winge

2009

EMBO Reports

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Mitochondrial Respiratory C omplex II

Bartlam

Sun

Rao

2004

Handbook of Metalloproteins

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The mitochondrial respiratory Complex II, or succinate : ubiquinone oxidoreductase (SQR), is an integral membrane protein complex in both the tricarboxylic acid cycle (Krebs cycle) and aerobic respiration. To date, X‐ray crystal structures of mitochondrial respiratory Complex II have been reported from porcine heart and from chicken, as well as the structures of a number of related bacterial SQR or quinol : fumarate oxidoreductase (QFR) structures. Complex II comprises of two hydrophilic proteins (flavoprotein (Fp) and iron–sulfur protein (Ip)) and two transmembrane proteins (CybL and CybS), as well as prosthetic groups required for electron transfer from succinate to ubiquinone. A proximal ubiquinone site (Qp) is located on the matrix side of the protein complex. Inhibitor‐bound structures using 3‐nitropropionate (NPA), 2‐thenoyltrifluoroacetone (TTFA), and carboxin provide further functional details for Complex II. NPA, a succinate analog, confirms the location of the succinate binding site. TTFA, a classical inhibitor for the ubiquinone reduction of Complex II that works by occupying its ubiquinone binding sites, confirms the location of the Qp site in both porcine heart and chicken structures. The available Complex II structures provide models for studying the mitochondrial respiratory system and human mitochondrial diseases related to mutations in this complex.

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Crystal Structure of Mitochondrial Respiratory Membrane Protein Complex II

Cited by 701 publications

References 57 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

Shaping the mitochondrion: mitochondrial biogenesis, dynamics and dysfunction

Mitochondrial Respiratory C omplex II

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