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Artículo

Asymmetric bifunctional protein nanoparticles through redesign of self-assembly

Sosa, SantiagoIcon ; Rossi, Andrés HugoIcon ; Szalai, Alan MarceloIcon ; Klinke, SebastianIcon ; Rinaldi, Jimena JulietaIcon ; Farias, AnaIcon ; Berguer, Paula MercedesIcon ; Nadra, Alejandro DanielIcon ; Stefani, Fernando DanielIcon ; Goldbaum, Fernando AlbertoIcon ; Bonomi, Hernán RuyIcon
Fecha de publicación: 02/2019
Editorial: Royal Society of Chemistry
Revista: Nanoscale Advances
ISSN: 2516-0230
Idioma: Inglés
Tipo de recurso: Artículo publicado
Clasificación temática:
Nano-materiales

Resumen

Engineering oligomeric protein self-assembly is an attractive approach to fabricatenanostructures with well-defined geometries, stoichiometry and functions. The homodecamerBrucella Lumazine Synthase (BLS) is a highly stable and immunogenic protein nanoparticle (PNP).Here, we engineered the BLS protein scaffold to display two functions in spatially opposite regions ofits structure yielding a Janus-like nanoparticle. An in silico analysis of the BLS head-to-head dimer ofhomopentamers shows major inter-pentameric interactions located in the equatorial interface. Basedon this analysis, two BLS protomer variants were designed to interrupt pentamer self-dimerizationand promote heteropentameric dimers. This strategy enabled us to generate a decameric particle withtwo distinct sides formed by two independent pentamers. The versatility of this new self-assemblynanofabrication strategy is illustrated with two example applications. First, a bifunctional BLSbearing Alexa Fluor 488 fluorophores on one side and sialic acid binding domains on the other sidewas used for labelling murine and human cells and analyzed by flow cytometry and confocalmicroscopy. Second, multichromophoric FRET nanoparticles were fabricated and characterized at thesingle molecule level, showing discrete energy transfer events. The engineered BLS variantsconstitute a general platform for displaying two functions in a controlled manner within the same PNPwith potential applications in various areas such as biomedicine, biotechnology and nanotechnology.
Palabras clave: BRUCELLA LUMAZINE SYNTHASE , VACCINE PLATFORM , PROTEIN SCAFFOLD ENGINEERING , INTERFACE REDESIGN , SINGLE-MOLECULE FRET
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info:eu-repo/semantics/openAccess Excepto donde se diga explícitamente, este item se publica bajo la siguiente descripción: Creative Commons Attribution-NonCommercial 2.5 Unported (CC BY-NC 2.5)
Identificadores
URI: http://hdl.handle.net/11336/105020
URL: https://pubs.rsc.org/en/content/articlelanding/2019/NA/C8NA00375K
DOI: http://dx.doi.org/10.1039/C8NA00375K
Colecciones
Articulos(IIBBA)
Articulos de INST.DE INVEST.BIOQUIMICAS DE BS.AS(I)
Articulos(IQUIBICEN)
Articulos de INSTITUTO DE QUIMICA BIOLOGICA DE LA FACULTAD DE CS. EXACTAS Y NATURALES
Articulos(CIBION)
Articulos de CENTRO DE INVESTIGACIONES EN BIONANOCIENCIAS "ELIZABETH JARES ERIJMAN"
Citación
Sosa, Santiago; Rossi, Andrés Hugo; Szalai, Alan Marcelo; Klinke, Sebastian; Rinaldi, Jimena Julieta; et al.; Asymmetric bifunctional protein nanoparticles through redesign of self-assembly; Royal Society of Chemistry; Nanoscale Advances; 1; 5; 2-2019; 1833-1846
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