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Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection

[Image: see text] The anterior gradient homologue-2 (AGR2) protein is an attractive biomarker for various types of cancer. In pancreatic cancer, it is secreted to the pancreatic juice by premalignant lesions, which would be an ideal stage for diagnosis. Thus, designing assays for the sensitive detec...

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Autores principales: Arshavsky-Graham, Sofia, Ward, Simon J., Massad-Ivanir, Naama, Scheper, Thomas, Weiss, Sharon M., Segal, Ester
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2021
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8532149/
https://www.ncbi.nlm.nih.gov/pubmed/34693403
http://dx.doi.org/10.1021/acsmeasuresciau.1c00019
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author Arshavsky-Graham, Sofia
Ward, Simon J.
Massad-Ivanir, Naama
Scheper, Thomas
Weiss, Sharon M.
Segal, Ester
author_facet Arshavsky-Graham, Sofia
Ward, Simon J.
Massad-Ivanir, Naama
Scheper, Thomas
Weiss, Sharon M.
Segal, Ester
author_sort Arshavsky-Graham, Sofia
collection PubMed
description [Image: see text] The anterior gradient homologue-2 (AGR2) protein is an attractive biomarker for various types of cancer. In pancreatic cancer, it is secreted to the pancreatic juice by premalignant lesions, which would be an ideal stage for diagnosis. Thus, designing assays for the sensitive detection of AGR2 would be highly valuable for the potential early diagnosis of pancreatic and other types of cancer. Herein, we present a biosensor for label-free AGR2 detection and investigate approaches for enhancing the aptasensor sensitivity by accelerating the target mass transfer rate and reducing the system noise. The biosensor is based on a nanostructured porous silicon thin film that is decorated with anti-AGR2 aptamers, where real-time monitoring of the reflectance changes enables the detection and quantification of AGR2, as well as the study of the diffusion and target-aptamer binding kinetics. The aptasensor is highly selective for AGR2 and can detect the protein in simulated pancreatic juice, where its concentration is outnumbered by orders of magnitude by numerous proteins. The aptasensor’s analytical performance is characterized with a linear detection range of 0.05–2 mg mL(–1), an apparent dissociation constant of 21 ± 1 μM, and a limit of detection of 9.2 μg mL(–1) (0.2 μM), which is attributed to mass transfer limitations. To improve the latter, we applied different strategies to increase the diffusion flux to and within the nanostructure, such as the application of isotachophoresis for the preconcentration of AGR2 on the aptasensor, mixing, or integration with microchannels. By combining these approaches with a new signal processing technique that employs Morlet wavelet filtering and phase analysis, we achieve a limit of detection of 15 nM without compromising the biosensor’s selectivity and specificity.
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spelling pubmed-85321492021-10-22 Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection Arshavsky-Graham, Sofia Ward, Simon J. Massad-Ivanir, Naama Scheper, Thomas Weiss, Sharon M. Segal, Ester ACS Meas Sci Au [Image: see text] The anterior gradient homologue-2 (AGR2) protein is an attractive biomarker for various types of cancer. In pancreatic cancer, it is secreted to the pancreatic juice by premalignant lesions, which would be an ideal stage for diagnosis. Thus, designing assays for the sensitive detection of AGR2 would be highly valuable for the potential early diagnosis of pancreatic and other types of cancer. Herein, we present a biosensor for label-free AGR2 detection and investigate approaches for enhancing the aptasensor sensitivity by accelerating the target mass transfer rate and reducing the system noise. The biosensor is based on a nanostructured porous silicon thin film that is decorated with anti-AGR2 aptamers, where real-time monitoring of the reflectance changes enables the detection and quantification of AGR2, as well as the study of the diffusion and target-aptamer binding kinetics. The aptasensor is highly selective for AGR2 and can detect the protein in simulated pancreatic juice, where its concentration is outnumbered by orders of magnitude by numerous proteins. The aptasensor’s analytical performance is characterized with a linear detection range of 0.05–2 mg mL(–1), an apparent dissociation constant of 21 ± 1 μM, and a limit of detection of 9.2 μg mL(–1) (0.2 μM), which is attributed to mass transfer limitations. To improve the latter, we applied different strategies to increase the diffusion flux to and within the nanostructure, such as the application of isotachophoresis for the preconcentration of AGR2 on the aptasensor, mixing, or integration with microchannels. By combining these approaches with a new signal processing technique that employs Morlet wavelet filtering and phase analysis, we achieve a limit of detection of 15 nM without compromising the biosensor’s selectivity and specificity. American Chemical Society 2021-08-25 /pmc/articles/PMC8532149/ /pubmed/34693403 http://dx.doi.org/10.1021/acsmeasuresciau.1c00019 Text en © 2021 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by-nc-nd/4.0/Permits non-commercial access and re-use, provided that author attribution and integrity are maintained; but does not permit creation of adaptations or other derivative works (https://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Arshavsky-Graham, Sofia
Ward, Simon J.
Massad-Ivanir, Naama
Scheper, Thomas
Weiss, Sharon M.
Segal, Ester
Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection
title Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection
title_full Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection
title_fullStr Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection
title_full_unstemmed Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection
title_short Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection
title_sort porous silicon-based aptasensors: toward cancer protein biomarker detection
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8532149/
https://www.ncbi.nlm.nih.gov/pubmed/34693403
http://dx.doi.org/10.1021/acsmeasuresciau.1c00019
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