Literature DB >> 23909240

His86 from the N-terminus of frataxin coordinates iron and is required for Fe-S cluster synthesis.

Leslie E Gentry1, Matthew A Thacker, Reece Doughty, Russell Timkovich, Laura S Busenlehner.   

Abstract

Human frataxin has a vital role in the biosynthesis of iron-sulfur (Fe-S) clusters in mitochondria, and its deficiency causes the neurodegenerative disease Friedreich's ataxia. Proposed functions for frataxin in the Fe-S pathway include iron donation to the Fe-S cluster machinery and regulation of cysteine desulfurase activity to control the rate of Fe-S production, although further molecular detail is required to distinguish these two possibilities. It is well established that frataxin can coordinate iron using glutamate and aspartate side chains on the protein surface; however, in this work we identify a new iron coordinating residue in the N-terminus of human frataxin using complementary spectroscopic and structural approaches. Further, we demonstrate that His86 in this N-terminal region is required for high affinity iron coordination and iron assembly of Fe-S clusters by ISCU as part of the Fe-S cluster biosynthetic complex. If a binding site that includes His86 is important for Fe-S cluster synthesis as part of its chaperone function, this raises the possibility that either iron binding at the acidic surface of frataxin may be spurious or that it is required for protein-protein interactions with the Fe-S biosynthetic quaternary complex. Our data suggest that iron coordination to frataxin may be significant to the Fe-S cluster biosynthesis pathway in mitochondria.

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Year:  2013        PMID: 23909240      PMCID: PMC3871887          DOI: 10.1021/bi400443n

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


  39 in total

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2.  Yeast frataxin solution structure, iron binding, and ferrochelatase interaction.

Authors:  Yanan He; Steven L Alam; Simona V Proteasa; Yan Zhang; Emmanuel Lesuisse; Andrew Dancis; Timothy L Stemmler
Journal:  Biochemistry       Date:  2004-12-28       Impact factor: 3.162

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4.  Normal and Friedreich ataxia cells express different isoforms of frataxin with complementary roles in iron-sulfur cluster assembly.

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Review 7.  Human iron-sulfur cluster assembly, cellular iron homeostasis, and disease.

Authors:  Hong Ye; Tracey A Rouault
Journal:  Biochemistry       Date:  2010-06-22       Impact factor: 3.162

Review 8.  Iron-sulfur cluster biogenesis and human disease.

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9.  Mammalian frataxin controls sulfur production and iron entry during de novo Fe4S4 cluster assembly.

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10.  N-terminal iron-mediated self-cleavage of human frataxin: regulation of iron binding and complex formation with target proteins.

Authors:  Taejin Yoon; Eric Dizin; J A Cowan
Journal:  J Biol Inorg Chem       Date:  2007-02-07       Impact factor: 3.862

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Journal:  Science       Date:  2017-05-12       Impact factor: 47.728

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6.  SAXS and stability studies of iron-induced oligomers of bacterial frataxin CyaY.

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Review 7.  Iron in Friedreich Ataxia: A Central Role in the Pathophysiology or an Epiphenomenon?

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Review 9.  Ferroptosis in Friedreich's Ataxia: A Metal-Induced Neurodegenerative Disease.

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10.  A Combined Spectroscopic and In Silico Approach to Evaluate the Interaction of Human Frataxin with Mitochondrial Superoxide Dismutase.

Authors:  Davide Doni; Marta Meggiolaro; Javier Santos; Gérard Audran; Sylvain R A Marque; Paola Costantini; Marco Bortolus; Donatella Carbonera
Journal:  Biomedicines       Date:  2021-11-25
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