AI Article Synopsis

  • Mesoporous thin films are used for applications requiring high surface area and effective mass and charge transport, typically made using a process involving organic and inorganic materials.
  • Traditional fabrication methods face challenges like anisotropic shrinkage during solvent evaporation and template removal, which can affect the final properties of the films.
  • The study proposes a two-step calcination process that enhances the structural integrity and porosity of these thin films, leading to better mass transport characteristics, as demonstrated through improved lysozyme adsorption.

Article Abstract

Mesoporous thin films are widely used for applications in need of high surface area and efficient mass and charge transport properties. A well-established fabrication process involves the supramolecular assembly of organic molecules (e.g., block copolymers and surfactants) with inorganic materials obtained by sol-gel chemistry. Typically, subsequent calcination in air removes the organic template and reveals the porous inorganic network. A significant challenge for such coatings is the anisotropic shrinkage due to the volume contraction related to solvent evaporation, inorganic condensation, and template removal, affecting the final porosity as well as pore shape, size, arrangement, and accessibility. Here, we show that a two-step calcination process, composed of high-temperature treatment in argon followed by air calcination, is an effective fabrication strategy to reduce film contraction and enhance structural control of mesoporous thin films. Crucially, the formation of a transient carbonaceous scaffold enables the inorganic matrix to fully condense before template removal. The resulting mesoporous films retain a higher porosity as well as bigger pores with extended porous order. Such films present favorable characteristics for mass transport of large molecules. This is demonstrated for lysozyme adsorption into the mesoporous thin films as an example of enzyme storage.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9782354PMC
http://dx.doi.org/10.1021/acsami.2c18090DOI Listing

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