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Cited 2 time in webofscience Cited 3 time in scopus
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Tuning Surface Plasmon Resonance Responses through Size and Crosslinking Control of Multivalent Protein Binding-Capable Nanoscale Hydrogels

Authors
Teoh, Jie YingJeon, SuhwanYim, BoraYang, Hae MinHwang, YunseoKim, JuhuiLee, Su-KyoungPark, EunyoungKong, Tae YeonKim, So YounPark, YongdooKim, Young GyuKim, JongseongYoo, Dongwon
Issue Date
Jul-2022
Publisher
American Chemical Society
Keywords
biomolecules; surface plasmon resonance; monoclonal antibodies; nanoscale hydrogels; multivalent protein binding
Citation
ACS Biomaterial Science and Engineering, v.8, no.7, pp 2878 - 2889
Pages
12
Indexed
SCIE
SCOPUS
Journal Title
ACS Biomaterial Science and Engineering
Volume
8
Number
7
Start Page
2878
End Page
2889
URI
https://scholarworks.korea.ac.kr/kumedicine/handle/2021.sw.kumedicine/61185
DOI
10.1021/acsbiomaterials.2c00250
ISSN
2373-9878
2373-9878
Abstract
Surface plasmon resonance (SPR) phenomena have been widely studied to detect biomolecules because of their high sensitivity and ability to determine biomolecular interactions with kinetic information. However, highly selective detection in specific concentration ranges relevant to target biomolecules is still a challenging task. Recently, we developed bioresponsive nanoscale hydrogels to selectively intensify SPR signals through multivalent protein binding (MPB) events with target biomolecules, including IL-2, where we were able to demonstrate exceptional selectivity for target biomolecules with minimal responses to nonspecific and monovalent binding events. In this work, we systematically explored the relationship between the physical properties of MPB-capable nanoscale hydrogels and their SPR response induced in the presence of the programmed cell death protein 1 antibody (PD-1Ab) as a model target biomolecule. First, we developed a synthetic protocol by controlling various reaction parameters to construct a library of nanoscale poly(N-isopropylacrylamide-co-acrylic acid) hydrogels (NHs) with different sizes (from 400 nm to 1 mu m) and degrees of crosslinking (from 2 to 8%). Then, by incorporating MPB-capable PD-1 receptors onto the surface of NHs to form PD-1-responsive nanoscale hydrogels (PNHs), the hydrogel size and crosslinking dependency of their SPR responses were investigated. Our results reveal the appropriate hydrogel size regime and degree of crosslinking for effective PD-1Ab detection at specific concentrations range between a few nM and 1 mu M. Overall, our study demonstrates that by tuning the physical properties of the nanoscale hydrogel matrix, the sensitivity and detection range of MPB-based SPR sensors can be modulated to potentially benefit clinical applications such as monitoring diverse therapeutic biomolecules.
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