Articolo in rivista, 2017, ENG, 10.1002/2211-5463.12259

Structural flexibility of human alpha-dystroglycan

Covaceuszach, Sonia (1); Bozzi, Manuela (2,3); Bigotti, Maria Giulia (4); Sciandra, Francesca (3); Konarev, Petr Valeryevich (5, 6); Brancaccio, Andrea (3); Cassetta, Alberto (1)

(1) CNR - Istituto di Cristallografia, Trieste (2) Istituto di Biochimica e Biochimica Clinica- Università Cattolica del Sacro Cuore, Roma (3) CNR - Istituto di Chimica del Riconoscimento Molecolare, Roma (4) School of Biochemistry, University of Bristol, UK (5) Shubnikov Institute of Crystallography of Federal Scientific Research Centre,"Crystallography and Photonics" of Russian Academy of Sciences, Moscow, Russia (6) National Research Centre "Kurchatov Institute", Moscow, Russia

Dystroglycan (DG), composed of and subunits, belongs to the dystrophin-associated glycoprotein complex. alpha-DG is an extracellular matrix protein that undergoes a complex post-translational glycosylation process. The bifunctional glycosyltransferase like-acetylglucosaminyltransferase (LARGE) plays a crucial role in the maturation of alpha-DG, enabling its binding to laminin. We have already structurally analyzed the N-terminal region of murine alpha-DG (alpha-DG-Nt) and of a pathological single point mutant that may affect recognition of LARGE, although the structural features of the potential interaction between LARGE and DG remain elusive. We now report on the crystal structure of the wild-type human alpha-DG-Nt that has allowed us to assess the reliability of our murine crystallographic structure as alpha-DG-Nt general model. Moreover, we address for the first time both structures in solution. Interestingly, small-angle X-ray scattering (SAXS) reveals the existence of two main protein conformations ensembles. The predominant species is reminiscent of the crystal structure, while the less populated one assumes a more extended fold. A comparative analysis of the human and murine alpha-DG-Nt solution structures reveals that the two proteins share a common interdomain flexibility and population distribution of the two conformers. This is confirmed by the very similar stability displayed by the two orthologs as assessed by biochemical and biophysical experiments. These results highlight the need to take into account the molecular plasticity of alpha-DG-Nt in solution, as it can play an important role in the functional interactions with other binding partners.

FEBS openbio 7 (8), pp. 1064–1077

Keywords

conformational stability, muscular dystrophy, small-angle X-ray scattering, structural flexibility, X-ray crystal structure, alpha-Dystroglycan

CNR authors

Sciandra Francesca, Bozzi Manuela, Cassetta Alberto, Brancaccio Andrea, Covaceuszach Sonia

CNR institutes

ICRM – Istituto di chimica del riconoscimento molecolare, IC – Istituto di cristallografia