| Literature DB >> 32250516 |
Jian-An Huang1, Mansoureh Z Mousavi1, Giorgia Giovannini1,2, Yingqi Zhao1, Aliaksandr Hubarevich1, Miguel A Soler3, Walter Rocchia3, Denis Garoli1,4, Francesco De Angelis1.
Abstract
The SERS-based detection of protein sequences with single-residue sensitivity suffers from signal dominance of aromatic amino acid residues and backbones, impeding detection of non-aromatic amino acid residues. Herein, we trap a gold nanoparticle in a plasmonic nanohole to generate a single SERS hot spot for single-molecule detection of 2 similar polypeptides (vasopressin and oxytocin) and 10 distinct amino acids that constitute the 2 polypeptides. Significantly, both aromatic and non-aromatic amino acids are detected and discriminated at the single-molecule level either at individual amino acid molecules or within the polypeptide chains. Correlated with molecular dynamics simulations, our results suggest that the signal dominance due to large spatial occupancy of aromatic rings of the polypeptide sidechains on gold surfaces can be overcome by the high localization of the single hot spot. The superior spectral and spatial discriminative power of our approach can be applied to single-protein analysis, fingerprinting, and sequencing.Entities:
Keywords: Raman spectroscopy; amino acids; molecular dynamics; proteins; single-molecule sequencing
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Year: 2020 PMID: 32250516 DOI: 10.1002/anie.202000489
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336