| Literature DB >> 30366134 |
Hèctor López-Laguna1, Ugutz Unzueta2, Oscar Conchillo-Solé3, Alejandro Sánchez-Chardi4, Mireia Pesarrodona5, Olivia Cano-Garrido1, Eric Voltà1, Laura Sánchez-García5, Naroa Serna5, Paolo Saccardo6, Ramón Mangues7, Antonio Villaverde8, Esther Vázquez9.
Abstract
Nanostructured protein materials show exciting biomedical applications, since both structure and function can be genetically programmed. In particular, self-assembling histidine-rich proteins benefit from functional plasticity that allows the generation of protein-only nanoparticles for cell targeted drug delivery. However, the rational development of constructs with improved functions is limited by a poor control of the oligomerization process. By exploring cross-interactions between histidine-tagged building blocks, we have identified a critical architectonic role of divalent cations. The obtained data instruct about how histidine-rich protein materials can be assembled, disassembled and reassembled within the nanoscale through the stoichiometric manipulation of divalent ions, in a biochemical approach to biomaterials design. STATEMENT OF SIGNIFICANCE: Divalent metal and non-metal cations such as Ni2+, Cu2+ Ca2+ and Zn2+ have been identified as unexpected molecular tools to control the assembling, disassembling and reassembling of histidine-rich protein materials at the nanoscale. Their stoichiometric manipulation allows generating defined protein-protein cross-molecular contacts between building blocks, for a powerful nano-biochemical manipulation of the material's architecture.Entities:
Keywords: Controlled oligomerization; Functional materials; Genetic design; Nanoparticles; Protein materials
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Year: 2018 PMID: 30366134 DOI: 10.1016/j.actbio.2018.10.030
Source DB: PubMed Journal: Acta Biomater ISSN: 1742-7061 Impact factor: 8.947