By Simonelli Valeria; Leuzzi Giuseppe; Basile Giorgia; D'Errico Mariarosaria; Fortini Paola; Franchitto Annapaola; Parlanti Eleonora;…
By Noguera Martin E; Vazquez Diego S; Herrera Maria Georgina; Roman Ernesto A; Aran Martin; Smal Clara; Alaimo Nadine; Gallo Mariana; Santos Javier
From Archives of biochemistry and biophysics (2017), 636123-137, Language: English, Database: MEDLINE
Human frataxin (FXN) is a highly conserved mitochondrial protein involved in iron homeostasis and activation of the iron-sulfur cluster assembly. FXN deficiency causes the neurodegenerative disease Friedreich’s Ataxia. Here, we investigated the effect of alterations in loop-1, a stretch presumably essential for FXN function, on the conformational stability and dynamics of the native state. We generated four loop-1 variants, carrying substitutions, insertions and deletions. All of them were stable and well-folded proteins. Fast local motions (ps-ns) and slower long-range conformational dynamics (μs-ms) were altered in some mutants as judged by NMR. Particularly, loop-1 modifications impact on the dynamics of a distant region that includes residues from the β-sheet, helix α1 and the C-terminal. Remarkably, all the mutants retain the ability to activate cysteine desulfurase, even when two of them exhibit a strong decrease in iron binding, revealing a differential sensitivity of these functional features to loop-1 perturbation. Consequently, we found that even for a small and relatively rigid protein, engineering a loop segment enables to alter conformational dynamics through a long-range effect, preserving the native-state structure and important aspects of function.