Epitaxy: Programmable Atom Equivalents versus Atoms

Mary X. Wang, Soyoung E. Seo, Paul A. Gabrys, Dagny Fleischman, Byeongdu Lee, Youngeun Kim, Harry A. Atwater, Robert J. Macfarlane, Chad A. Mirkin

Research output: Chapter in Book/Report/Conference proceedingChapter

Abstract

1160The programmability of DNA makes it an attractive structuredirecting ligand for the assembly of nanoparticle (NP) superlattices in a manner that mimics many aspects of atomic crystallization. However, the synthesis of multilayer single crystals of defined size remains a challenge. Though previous studies considered lattice mismatch as the major limiting factor for multilayer assembly, thin-film growth depends on many interlinked variables. Here, a more comprehensive approach is taken to study fundamental elements, such as the growth temperature and the thermodynamics of interfacial energetics, to achieve epitaxial growth of NP thin films. Both surface morphology and internal thin-film structure are examined to provide an understanding of particle attachment and reorganization during growth. Under equilibrium conditions, single-crystalline, multilayer thin films can be synthesized over 500 × 500 µm areas on lithographically patterned templates, whereas deposition under kinetic conditions leads to the rapid growth of glassy films. Importantly, these superlattices follow the same patterns of crystal growth demonstrated in atomic thin-film deposition, allowing these processes to be understood in the context of well-studied atomic epitaxy and enabling a nanoscale model to study fundamental crystallization processes. Through understanding the role of epitaxy as a driving force for NP assembly, we are able to realize 3D architectures of arbitrary domain geometry and size.

Original languageEnglish (US)
Title of host publicationSpherical Nucleic Acids
Subtitle of host publicationVolume 3
PublisherJenny Stanford Publishing
Pages1159-1176
Number of pages18
Volume3
ISBN (Electronic)9781000092486
ISBN (Print)9789814877237
DOIs
StatePublished - Jan 1 2021
Externally publishedYes

ASJC Scopus subject areas

  • General Biochemistry, Genetics and Molecular Biology
  • General Engineering
  • General Chemistry

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