Identificador persistente para citar o vincular este elemento: http://hdl.handle.net/10553/75603
Título: Decoding Biomineralization: Interaction of a Mad10-Derived Peptide with Magnetite Thin Films
Autores/as: Pohl, Anna
Berger, Florian
Sullan, Ruby M. A.
Valverde Tercedor, María Del Carmen 
Freindl, Kinga
Spiridis, Nika
Lefevre, Christopher T.
Menguy, Nicolas
Klumpp, Stefan
Blank, Kerstin G.
Faivre, Damien
Clasificación UNESCO: 3208 Farmacodinámica
Palabras clave: Magnetite
Magnetotactic Bacteria
Magnetite-Binding Peptide
Single-Molecule Force Spectroscopy
Biomineralization, et al.
Fecha de publicación: 2019
Publicación seriada: Nano Letters 
Resumen: Protein-surface interactions play a pivotal role in processes as diverse as biomineralization, biofouling, and the cellular response to medical implants. In biomineralization processes, biomacromolecules control mineral deposition and architecture via complex and often unknown mechanisms. For studying these mechanisms, the formation of magnetite nanoparticles in magnetotactic bacteria has become an excellent model system. Most interestingly, nanoparticle morphologies have been discovered that defy crystallographic rules (e.g., in the species Desulfamplus magnetovallimortis strain BW-1). In certain conditions, this strain mineralizes bullet-shaped magnetite nanoparticles, which exhibit defined (111) crystal faces and are elongated along the [100] direction. We hypothesize that surface-specific protein interactions break the nanoparticle symmetry, inhibiting the growth of certain crystal faces and thereby favoring the growth of others. Screening the genome of BW-1, we identified Mad10 (Magnetosome-associated deep-branching) as a potential magnetite-binding protein. Using atomic force microscope (AFM)-based single-molecule force spectroscopy, we show that a Mad10-derived peptide, which represents the most conserved region of Mad10, binds strongly to (100)- and (111)-oriented single-crystalline magnetite thin films. The peptide-magnetite interaction is thus material- but not crystal-face-specific. It is characterized by broad rupture force distributions that do not depend on the retraction speed of the AFM cantilever. To account for these experimental findings, we introduce a three-state model that incorporates fast rebinding. The model suggests that the peptide-surface interaction is strong in the absence of load, which is a direct result of this fast rebinding process. Overall, our study sheds light on the kinetic nature of peptide-surface interactions and introduces a new magnetite-binding peptide with potential use as a functional coating for magnetite nanoparticles in biotechnological and biomedical applications.
URI: http://hdl.handle.net/10553/75603
ISSN: 1530-6984
DOI: 10.1021/acs.nanolett.9b03560
Fuente: Nano Letters [ISSN 1530-6984], v. 19 (11), p. 8207-8215
Colección:Artículos
miniatura
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