In vivo architectonic stability of fully de novo designed protein-only nanoparticles

Author

Céspedes, María Virtudes

Unzueta Elorza, Ugutz

Tatkiewicz, Witold

Sánchez Chardi, Alejandro

Conchillo-Solé, Oscar

Álamo, Patricia

Xu, Zhikun

Casanova Rigat, Isolda

Corchero Nieto, José Luis

Pesarrodona Roches, Mireia

Cedano Rodríguez, Juan Antonio

Daura i Ribera, Xavier

Ratera Bastardas, Imma

Veciana i Miró, Jaume

Ferrer-Miralles, Neus

Vázquez Gómez, Esther

Villaverde Corrales, Antonio

Mangues, Ramon

Publication date

2014

Abstract

The fully de novo design of protein building blocks for self-assembling as functional nanoparticles is a challenging task in emerging nanomedicines, which urgently demand novel, versatile, and biologically safe vehicles for imaging, drug delivery, and gene therapy. While the use of viruses and virus-like particles is limited by severe constraints, the generation of protein-only nanocarriers is progressively reachable by the engineering of protein-protein interactions, resulting in self-assembling functional building blocks. In particular, end-terminal cationic peptides drive the organization of structurally diverse protein species as regular nanosized oligomers, offering promise in the rational engineering of protein self-assembling. However, the in vivo stability of these constructs, being a critical issue for their medical applicability, needs to be assessed. We have explored here if the cross-molecular contacts between protein monomers, generated by end-terminal cationic peptides and oligohistidine tags, are stable enough for the resulting nanoparticles to overcome biological barriers in assembled form. The analyses of renal clearance and biodistribution of several tagged modular proteins reveal long-term architectonic stability, allowing systemic circulation and tissue targeting in form of nanoparticulate material. This observation fully supports the value of the engineered of protein building blocks addressed to the biofabrication of smart, robust, and multifunctional nanoparticles with medical applicability that mimic structure and functional capabilities of viral capsids.

Document Type

Article

Language

English

Subjects and keywords

Protein nanoparticles; Building blocks; Genetic engineering; Biodistribution; Targeting; Drug delivery; Nanoparticles; Self-assembling; Architectonic stability; Protein folding; Artificial viruses

Publisher

 

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ACS nano ; Vol. 8, Num. 5 (May 2014), p. 4166-4176

Rights

open access

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