A self-assembly pathway to aligned monodomain gels

Aggregates of charged amphiphilic molecules have been found to access a structure at elevated temperature that templates alignment of supramolecular fibrils over macroscopic scales. The thermal pathway leads to a lamellar plaque structure with fibrous texture that breaks on cooling into large arrays...

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Veröffentlicht in:Nat. Mater 2010-07, Vol.9 (7), p.594-601
Hauptverfasser: Zhang, Shuming, Greenfield, Megan A., Mata, Alvaro, Palmer, Liam C., Bitton, Ronit, Mantei, Jason R., Aparicio, Conrado, de la Cruz, Monica Olvera, Stupp, Samuel I.
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Sprache:eng
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Zusammenfassung:Aggregates of charged amphiphilic molecules have been found to access a structure at elevated temperature that templates alignment of supramolecular fibrils over macroscopic scales. The thermal pathway leads to a lamellar plaque structure with fibrous texture that breaks on cooling into large arrays of aligned nanoscale fibres and forms a strongly birefringent liquid. By manually dragging this liquid crystal from a pipette onto salty media, it is possible to extend this alignment over centimetres in noodle-shaped viscoelastic strings. Using this approach, the solution of supramolecular filaments can be mixed with cells at physiological temperatures to form monodomain gels of aligned cells and filaments. The nature of the self-assembly process and its biocompatibility would allow formation of cellular wires in situ that have any length and customized peptide compositions for use in biological applications. Peptide-based molecules that self-assemble into lamellar plaques with fibrous texture on heating, subsequently break on cooling to form long-range aligned bundles of nanofibres. This thermal route to monodomain gels is compatible for living cells and allows the formation of noodle-like viscoelastic strings of any length.
ISSN:1476-1122
1476-4660
DOI:10.1038/nmat2778