Single-molecule fingerprinting of protein-drug interaction using a funneled biological nanopore

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作者
Ki-Baek Jeong
Minju Ryu
Jin-Sik Kim
Minsoo Kim
Jejoong Yoo
Minji Chung
Sohee Oh
Gyunghee Jo
Seong-Gyu Lee
Ho Min Kim
Mi-Kyung Lee
Seung-Wook Chi
机构
[1] Division of Biomedical Research,Disease Target Structure Research Center
[2] Korea Research Institute of Bioscience and Biotechnology (KRIBB),Department of Proteome Structural Biology
[3] Critical Diseases Diagnostics Convergence Research Center,Department of Physics
[4] KRIBB,Center for Biomolecular and Cellular Structure
[5] KRIBB School of Bioscience,Graduate School of Medical Science and Engineering
[6] University of Science and Technology,School of Pharmacy
[7] Sungkyunkwan University,undefined
[8] Institute for Basic Science (IBS),undefined
[9] Korea Advanced Institute of Science and Technology (KAIST),undefined
[10] Sungkyunkwan University,undefined
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摘要
In drug discovery, efficient screening of protein-drug interactions (PDIs) is hampered by the limitations of current biophysical approaches. Here, we develop a biological nanopore sensor for single-molecule detection of proteins and PDIs using the pore-forming toxin YaxAB. Using this YaxAB nanopore, we demonstrate label-free, single-molecule detection of interactions between the anticancer Bcl-xL protein and small-molecule drugs as well as the Bak-BH3 peptide. The long funnel-shaped structure and nanofluidic characteristics of the YaxAB nanopore enable the electro-osmotic trapping of diverse folded proteins and high-resolution monitoring of PDIs. Distinctive nanopore event distributions observed in the two-dimensional (ΔI/Io-versus-IN) plot illustrate the ability of the YaxAB nanopore to discriminate individual small-molecule drugs bound to Bcl-xL from non-binders. Taken together, our results present the YaxAB nanopore as a robust platform for label-free, ultrasensitive, single-molecule detection of PDIs, opening up a possibility for low-cost, highly efficient drug discovery against diverse drug targets.
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