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Exploring the folding landscape of leptin: Insights into threading pathways

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Autor(es):
da Silva, Fernando Bruno ; Simien, Jennifer M. ; Viegas, Rafael G. ; Haglund, Ellinor ; Leite, Vitor Barbanti Pereira
Número total de Autores: 5
Tipo de documento: Artigo Científico
Fonte: Journal of Structural Biology; v. 216, n. 1, p. 7-pg., 2023-12-14.
Resumo

The discovery of new protein topologies with entanglements and loop-crossings have shown the impact of local amino acid arrangement and global three-dimensional structures. This phenomenon plays a crucial role in understanding how protein structure relates to folding and function, affecting the global stability, and biological activity. Protein entanglements encompassing knots and non -trivial topologies add complexity to their folding free energy landscapes. However, the initial native contacts driving the threading event for entangled proteins remains elusive. The Pierced Lasso Topology (PLT) represents an entangled topology where a covalent linker creates a loop in which the polypeptide backbone is threaded through. Compared to true knotted topologies, PLTs are simpler topologies where the covalent-loop persists in all conformations. In this work, the PLT protein leptin, is used to visualize and differentiate the preference for slipknotting over plugging transition pathways along the folding route. We utilize the Energy Landscape Visualization Method (ELViM), a multidimensional projection technique, to visualize and distinguish early threaded conformations that cannot be observed in an in vitro experiment. Critical contacts for the leptin threading mechanisms were identified where the competing pathways are determined by the formation of a hairpin loop in the unfolded basin. Thus, prohibiting the dominant slipknotting pathway. Furthermore, ELViM offers insights into distinct folding pathways associated with slipknotting and plugging providing a novel tool for de novo design and in vitro experiments with residue specific information of threading events in silico. (AU)

Processo FAPESP: 23/02219-1 - Entendendo mecanismos funcionais de proteínas e RNAs por meio de relevos de superfícies de energia
Beneficiário:Vitor Barbanti Pereira Leite
Modalidade de apoio: Auxílio à Pesquisa - Regular