Literature DB >> 24914854

Structural insights into the coenzyme mediated monomer-dimer transition of the pro-apoptotic apoptosis inducing factor.

Patricia Ferreira1, Raquel Villanueva, Marta Martínez-Júlvez, Beatriz Herguedas, Carlos Marcuello, Patricio Fernandez-Silva, Lauriane Cabon, Juan A Hermoso, Anabel Lostao, Santos A Susin, Milagros Medina.   

Abstract

The apoptosis-inducing factor (AIF) is a mitochondrial-flavoprotein that, after cell death induction, is distributed to the nucleus to mediate chromatinolysis. In mitochondria, AIF is present in a monomer-dimer equilibrium that after reduction by NADH gets displaced toward the dimer. The crystal structure of the human AIF (hAIF):NAD(H)-bound dimer revealed one FAD and, unexpectedly, two NAD(H) molecules per protomer. A 1:2 hAIF:NAD(H) binding stoichiometry was additionally confirmed in solution by using surface plasmon resonance. The here newly discovered NAD(H)-binding site includes residues mutated in human disorders, and accommodation of the coenzyme in it requires restructuring of a hAIF portion within the 509-560 apoptogenic segment. Disruption of interactions at the dimerization surface by production of the hAIF E413A/R422A/R430A mutant resulted in a nondimerizable variant considerably less efficiently stabilizing charge-transfer complexes upon coenzyme reduction than WT hAIF. These data reveal that the coenzyme-mediated monomer-dimer transition of hAIF modulates the conformation of its C-terminal proapoptotic domain, as well as its mechanism as reductase. These observations suggest that both the mitochondrial and apoptotic functions of hAIF are interconnected and coenzyme controlled: a key information in the understanding of the physiological role of AIF in the cellular life and death cycle.

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Year:  2014        PMID: 24914854     DOI: 10.1021/bi500343r

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  14 in total

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3.  Autophagy and Apoptosis Specific Knowledgebases-guided Systems Pharmacology Drug Research.

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4.  Oxidative Stress Impairs Cell Death by Repressing the Nuclease Activity of Mitochondrial Endonuclease G.

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5.  Basal metabolic state governs AIF-dependent growth support in pancreatic cancer cells.

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9.  FAD/NADH Dependent Oxidoreductases: From Different Amino Acid Sequences to Similar Protein Shapes for Playing an Ancient Function.

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10.  Cerebellar ataxia, neuropathy, hearing loss, and intellectual disability due to AIFM1 mutation.

Authors:  Massimo Pandolfo; Myriam Rai; Gauthier Remiche; Laurence Desmyter; Isabelle Vandernoot
Journal:  Neurol Genet       Date:  2020-04-09
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