Three Classes of Inhibitors Share a Common Binding Domain in Mitochondrial Complex I (NADH:Ubiquinone Oxidoreductase)

Okun, Jürgen G.; Lümmen, Peter; Brandt, Ulrich

doi:10.1074/jbc.274.5.2625

Cited by 306 publications

(282 citation statements)

References 56 publications

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“…The simplest explanation of these observations is that there is a particular state of complex I that leads to high superoxide production, and this state can be accessed either during reverse electron transport, or during forward electron transport when an inhibitor occupies the Q-binding site. The fact that different rates of superoxide production were obtained with the three different Q site inhibitors is consistent with the concept of two or three classes of complex I inhibitor with different degrees of overlap in a large Q-binding pocket (25,27). Occupation of one of these binding sites by an inhibitor would trigger superoxide production by promoting the reaction with oxygen of some reductant either within the Q site (such as a semiquinone) or elsewhere within complex I.…”

Section: Discussionsupporting

confidence: 77%

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Inhibitors of the Quinone-binding Site Allow Rapid Superoxide Production from Mitochondrial NADH:Ubiquinone Oxidoreductase (Complex I)

Lambert

Brand

2004

Journal of Biological Chemistry

436

353

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Neither the route of electron transport nor the sites or mechanism of superoxide production in mitochondrial complex I has been established. We examined the rates of superoxide generation (measured as hydrogen peroxide production) by rat skeletal muscle mitochondria under a variety of conditions. The rate of superoxide production by complex I during NADH-linked forward electron transport was less than 10% of that during succinate-linked reverse electron transport even when complex I was fully reduced by pyruvate plus malate in the presence of the complex III inhibitor, stigmatellin. This asymmetry was not explained by differences in protonmotive force or its components. However, when inhibitors of the quinone-binding site of complex I were added in the presence of ATP to generate a pH gradient, there was a rapid rate of superoxide production by forward electron transport that was as great as the rate seen with reverse electron transport at the same pH gradient. These observations suggest that quinone-binding site inhibitors can make complex I adopt the highly radical-producing state that occurs during reverse electron transport. Despite complete inhibition of NADH: ubiquinone oxidoreductase activity in each case, different classes of quinone-binding site inhibitor (rotenone, piericidin, and high concentrations of myxothiazol) gave different rates of superoxide production during forward electron transport (the rate with myxothiazol was twice that with rotenone) suggesting that the site of rapid superoxide generation by complex I is in the region of the ubisemiquinone-binding sites and not upstream at the flavin or low potential FeS centers.

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Section: Discussionsupporting

confidence: 77%

“…Recent models of complex I propose three different semiquinone sites: two quinone reduction sites and one quinol oxidation site (6,30). Three classes of inhibitor have been described, possibly corresponding to three semiquinone species in a large Q-binding pocket (25,27). Of these species, only SQ Nf exhibits sensitivity to ⌬p.…”

Section: Figmentioning

confidence: 99%

Inhibitors of the Quinone-binding Site Allow Rapid Superoxide Production from Mitochondrial NADH:Ubiquinone Oxidoreductase (Complex I)

Lambert

Brand

2004

Journal of Biological Chemistry

436

353

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“…In particular, the inhibitory potency of compound 7 possessing two n-butyl groups was equivalent to that of bullatacin, one of the most potent inhibitors of bovine complex I (4,6,9). Replacement of the n-butyl group of compound 7 with a bulky tert-butyl group little affected the activity (compound 7 vs 8).…”

Section: Crucial Structural Factors In the Thf Ring Moietymentioning

confidence: 97%

Synthesis and Inhibition Mechanism of Δlac-Acetogenins, a Novel Type of Inhibitor of Bovine Heart Mitochondrial Complex I

et al. 2004

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We have synthesized ∆lac-acetogenins that are new acetogenin mimics possessing two n-alkyl tails without an R, -unsaturated γ-lactone ring and suggested that their inhibition mechanism may be different from that of common acetogenins [Hamada et al. (2004) Biochemistry 43, 3651-3658]. To elucidate the inhibition mechanism of ∆lac-acetogenins in more detail, we carried out wide structural modifications of original ∆lac-acetogenins and characterized the inhibitory action with bovine heart mitochondrial complex I. In contrast to common acetogenins, both the presence of adjacent bis-THF rings and the stereochemistry around the hydroxylated bis-THF rings are important structural factors required for potent inhibition. The inhibitory potency of a derivative possessing an n-butylphenyl ether structure (compound 7) appeared to be superior to that of the original ∆lac-acetogenins and equivalent to that of bullatacin, one of the most potent natural acetogenins. Double-inhibitor titration of steady-state complex I activity showed that the extent of inhibition of compound 7 and bullatacin is not additive, suggesting that the binding sites of the two inhibitors are not identical. Competition tests using a fluorescent ligand indicated that the binding site of compound 7 does not overlap with that of other complex I inhibitors. The effects of compound 7 on superoxide production from complex I are also different from those of other complex I inhibitors. Our results clearly demonstrate that ∆lac-acetogenins are a novel type of inhibitor acting at the terminal electron-transfer step of bovine complex I.

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“…Structure elucidation was performed using mass spectrometry and NMR methods, and data were compared to that of iromycin A. The non-natural derivatives iromycin AH (13), AM (14), BM (15), AA (16), and BA (17) were prepared from the microbial metabolites iromycin A (7) and B (8) which can be isolated from Streptomyces sp. Dra 17 in reasonable amounts.…”

Section: Organic and Biomolecular Chemistrymentioning

confidence: 99%

“…Yet, the understanding of the competitive behaviour of established complex I inhibitors is hampered by the possibility, that the chemical diverse molecules might either compete for identical binding sites or induce structural dynamic changes in the enzyme which then influence the binding of a second inhibitor. 15,16 Recently, we reported about the isolation and total synthesis of iromycins A-D, a unique family of α-pyridone metabolites from Streptomyces sp. 17,18 The striking structural similarities and clear differences with inhibitors 5 and 6 gave rise to evaluate their inhibitory potential and the site of action within the mitochondrial electron transport chain.…”

Section: Introductionmentioning

confidence: 99%

Iromycins from Streptomyces sp. and from synthesis: New inhibitors of the mitochondrial electron transport chain

Surup

Shojaei

Zezschwitz

et al. 2008

Bioorganic & Medicinal Chemistry

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CitationIromycins Abstract:Two new α-pyridone metabolites, iromycin E and F, were isolated from cultures of strain Streptomyces sp. Dra 17, thus expanding the recently discovered iromycin family. Their inhibitory potential on the mitochondrial respiratory chain was examined and revealed that iromycin metabolites block NADH oxidation in beef heart submitochondrial particles with different efficacy, yet remarkably show only very low cytotoxicity. Difference spectroscopic studies indicated that iromycins inhibited the electron transport at the site of complex I (NADH-ubiquinone oxidoreductase). Derivatives of the natural products were semisynthetically prepared and provided detailed insights into structure activity relationships.Drawn from these results, there are strong similarities with the piercidins, which are among the most potent complex I inhibitors of the mitochondrial electron transport chain.Furthermore, total synthesis afforded new analogues, and the non-natural iromycin S (IC 50 = 58 ng/mL) emerged as the most active compound, thus opening avenues of future studies with the iromycins as new valuable biochemical tools.2

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Three Classes of Inhibitors Share a Common Binding Domain in Mitochondrial Complex I (NADH:Ubiquinone Oxidoreductase)

Cited by 306 publications

References 56 publications

Inhibitors of the Quinone-binding Site Allow Rapid Superoxide Production from Mitochondrial NADH:Ubiquinone Oxidoreductase (Complex I)

Inhibitors of the Quinone-binding Site Allow Rapid Superoxide Production from Mitochondrial NADH:Ubiquinone Oxidoreductase (Complex I)

Synthesis and Inhibition Mechanism of Δlac-Acetogenins, a Novel Type of Inhibitor of Bovine Heart Mitochondrial Complex I

Iromycins from Streptomyces sp. and from synthesis: New inhibitors of the mitochondrial electron transport chain

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