Maria Petrosino Alessandra Pasquo Leonore Novak Angelo Toto Stefano Gianni Elide Mantuano Liana Veneziano Velia Minicozzi Annalisa Pastore Rita Puglisi Emidio Capriotti Roberta Chiaraluce Valerio Consalvi; Hum Mutat. 2019 May 10. doi: 10.1002/humu.23789.
Defective function of frataxin may cause defects in mitochondria, leading to increased tumorigenesis. Tumour initiating cells show higher iron uptake, a decrease in iron storage and a reduced Fe‐S clusters synthesis and utilization. In this study we selected, from COSMIC database, the somatic human frataxin missense variants found in cancer tissues p.D104G, p.A107V, p.F109L, p.Y123S, p.S161I, p.W173C, p.S181F, and p.S202F to analyze the effect of the single amino acid substitutions on frataxin structure, function and stability. The spectral properties, the thermodynamic and the kinetic stability, as well as the molecular dynamics of the frataxin missense variants found in cancer tissues point to local changes confined to the environment of the mutated residues. The global fold of the variants is not altered by the amino acid substitutions, however some of the variants show a decreased stability and a decreased functional activity in comparison to that of the wild type protein.
Characterization of human frataxin missense variants in cancer tissues