| Literature DB >> 31939159 |
Ignacio Hugo Castro1,2, María Florencia Pignataro1,2, Karl Ellioth Sewell1,2, Lucía Daniela Espeche3, María Georgina Herrera1, Martín Ezequiel Noguera1,2,4, Liliana Dain1,3, Alejandro Daniel Nadra1,5, Martín Aran6, Clara Smal6, Mariana Gallo7, Javier Santos8,9.
Abstract
Mammalian frataxin is a small mitochondrial protein involved in iron sulfur cluster assembly. Frataxin deficiency causes the neurodegenerative disease Friedreich's Ataxia. Valuable knowledge has been gained on the structural dynamics of frataxin, metal-ion-protein interactions, as well as on the effect of mutations on protein conformation, stability and internal motions. Additionally, laborious studies concerning the enzymatic reactions involved have allowed for understanding the capability of frataxin to modulate Fe-S cluster assembly function. Remarkably, frataxin biological function depends on its interaction with some proteins to form a supercomplex, among them NFS1 desulfurase and ISCU, the scaffolding protein. By combining multiple experimental tools including high resolution techniques like NMR and X-ray, but also SAXS, crosslinking and mass-spectrometry, it was possible to build a reliable model of the structure of the desulfurase supercomplex NFS1/ACP-ISD11/ISCU/frataxin. In this chapter, we explore these issues showing how the scientific view concerning frataxin structure-function relationships has evolved over the last years.Entities:
Keywords: Conformational stability; Frataxin; Iron binding; Iron–Sulfur cluster assembly; Structural dynamics; Structure-Function relationships
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Year: 2019 PMID: 31939159 DOI: 10.1007/978-3-030-28151-9_13
Source DB: PubMed Journal: Subcell Biochem ISSN: 0306-0225