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Multiple rereads of single proteins at single–amino acid resolution using nanopores
Author(s) -
Henry Brinkerhoff,
Albert S. W. Kang,
Jingqian Liu,
Aleksei Aksimentiev,
Cees Dekker
Publication year - 2021
Publication title -
science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 12.556
H-Index - 1186
eISSN - 1095-9203
pISSN - 0036-8075
DOI - 10.1126/science.abl4381
Subject(s) - nanopore , nanopore sequencing , amino acid , peptide , dna , chemistry , peptide sequence , computational biology , resolution (logic) , biophysics , nanotechnology , biology , dna sequencing , biochemistry , computer science , materials science , gene , artificial intelligence
Reading amino acids by nanopore Nanopore technology enables sensing of minute chemical changes at the single-molecule level by detecting differences in an ion current as molecules are drawn through a membrane-embedded pore. The sensitivity is sufficient to discriminate between nucleotide bases in nanopore sequencing, and other applications of this technology are promising. Brinkerhoffet al . developed a nanopore-based, single-molecule approach in which a protein was sequentially scanned in single-amino-acid steps through the narrow construction of a nanopore, and ion currents were monitored to resolve differences in the amino acid sequence along the peptide backbone (see the Perspective by Bošković and Keyser). The peptide reader was capable of reliably detecting single-amino-acid substitutions within individual peptides. An individual protein could be re-read many times, yielding very high read accuracy in variant identification. These proof-of-concept nanopore experiments constitute a promising basis for the development of a single-molecule protein sequencer. —DJ

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