International Journal of Molecular Sciences (Jan 2021)

Computational Evolution of Beta-2-Microglobulin Binding Peptides for Nanopatterned Surface Sensors

  • Abimbola Feyisara Adedeji Olulana,
  • Miguel A. Soler,
  • Martina Lotteri,
  • Hendrik Vondracek,
  • Loredana Casalis,
  • Daniela Marasco,
  • Matteo Castronovo,
  • Sara Fortuna

DOI
https://doi.org/10.3390/ijms22020812
Journal volume & issue
Vol. 22, no. 2
p. 812

Abstract

Read online

The bottom-up design of smart nanodevices largely depends on the accuracy by which each of the inherent nanometric components can be functionally designed with predictive methods. Here, we present a rationally designed, self-assembled nanochip capable of capturing a target protein by means of pre-selected binding sites. The sensing elements comprise computationally evolved peptides, designed to target an arbitrarily selected binding site on the surface of beta-2-Microglobulin (β2m), a globular protein that lacks well-defined pockets. The nanopatterned surface was generated by an atomic force microscopy (AFM)-based, tip force-driven nanolithography technique termed nanografting to construct laterally confined self-assembled nanopatches of single stranded (ss)DNA. These were subsequently associated with an ssDNA–peptide conjugate by means of DNA-directed immobilization, therefore allowing control of the peptide’s spatial orientation. We characterized the sensitivity of such peptide-containing systems against β2m in solution by means of AFM-based differential topographic imaging and surface plasmon resonance (SPR) spectroscopy. Our results show that the confined peptides are capable of specifically capturing β2m from the surface–liquid interface with micromolar affinity, hence providing a viable proof-of-concept for our approach to peptide design.

Keywords