4.7 Article

An Experimental Framework for Developing Point-of-Need Biosensors: Connecting Bio-Layer Interferometry and Electrochemical Impedance Spectroscopy

期刊

BIOSENSORS-BASEL
卷 12, 期 11, 页码 -

出版社

MDPI
DOI: 10.3390/bios12110938

关键词

biosensor design; protein-protein interaction; molecular affinity; binding kinetics; analytical sensing; SARS-CoV-2

资金

  1. National Institute on Alcohol Abuse and Alcoholism of the National Institutes of Health [U01AA029328]
  2. COVID Research Seed Grant Program, Clemson University [2021001151]
  3. Department of Environmental Engineering and Earth Sciences of Clemson University

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BLI is a crucial laboratory technique used in studying biomolecular interactions and this paper introduces a framework connecting BLI research outputs with key performance indicators in biosensor design, serving as guidance for the development of point-of-need biosensors.
Biolayer interferometry (BLI) is a well-established laboratory technique for studying biomolecular interactions important for applications such as drug development. Currently, there are interesting opportunities for expanding the use of BLI in other fields, including the development of rapid diagnostic tools. To date, there are no detailed frameworks for implementing BLI in target-recognition studies that are pivotal for developing point-of-need biosensors. Here, we attempt to bridge these domains by providing a framework that connects output(s) of molecular interaction studies with key performance indicators used in the development of point-of-need biosensors. First, we briefly review the governing theory for protein-ligand interactions, and we then summarize the approach for real-time kinetic quantification using various techniques. The 2020 PRISMA guideline was used for all governing theory reviews and meta-analyses. Using the information from the meta-analysis, we introduce an experimental framework for connecting outcomes from BLI experiments (K-D, k(on), k(off)) with electrochemical (capacitive) biosensor design. As a first step in the development of a larger framework, we specifically focus on mapping BLI outcomes to five biosensor key performance indicators (sensitivity, selectivity, response time, hysteresis, operating range). The applicability of our framework was demonstrated in a study of case based on published literature related to SARS-CoV-2 spike protein to show the development of a capacitive biosensor based on truncated angiotensin-converting enzyme 2 (ACE2) as the receptor. The case study focuses on non-specific binding and selectivity as research goals. The proposed framework proved to be an important first step toward modeling/simulation efforts that map molecular interactions to sensor design.

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