NMR investigation of ion-pair modulation of protein structure and dynamics and its relation to protein misfolding diseases

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Fast NMR method to probe solvent accessibility and disordered regions in proteins

Publication . Faustino, André F.; Barbosa, Glauce M.; Silva, Micael; Castanho, Miguel; Da Poian, Andrea T .; Cabrita, Eurico J.; Santos, Nuno C.; Almeida, Fabio C. L.; Martins, Ivo C.

Understanding protein structure and dynamics, which govern key cellular processes, is crucial for basic and applied research. Intrinsically disordered protein (IDP) regions display multifunctionality via alternative transient conformations, being key players in disease mechanisms. IDP regions are abundant, namely in small viruses, allowing a large number of functions out of a small proteome. The relation between protein function and structure is thus now seen from a different perspective: as IDP regions enable transient structural arrangements, each conformer can play different roles within the cell. However, as IDP regions are hard and time-consuming to study via classical techniques (optimized for globular proteins with unique conformations), new methods are required. Here, employing the dengue virus (DENV) capsid (C) protein and the immunoglobulin-binding domain of streptococcal protein G, we describe a straightforward NMR method to differentiate the solvent accessibility of single amino acid N-H groups in structured and IDP regions. We also gain insights into DENV C flexible fold region biological activity. The method, based on minimal pH changes, uses the well-established 1H-15N HSQC pulse sequence and is easily implementable in current protein NMR routines. The data generated are simple to interpret, with this rapid approach being an useful first-choice IDPs characterization method.

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Fundação para a Ciência e a Tecnologia

Número da atribuição

PD/BD/128202/2016