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An Ultrasensitive miRNA-Based Genosensor for Detection of MicroRNA 21 in Gastric Cancer Cells Based on Functional Signal Amplifier and Synthesized Perovskite-Graphene Oxide and AuNPs

In the present research work, the state-of-art label-free electrochemical genosensing platform was developed based on the hybridization process in the presence of [Fe(CN)(6)](3−/4−) as an efficient redox probe for sensitive recognition of the miRNA-21 in human gastric cell lines samples. To attain t...

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Autores principales: Shahbazi-Derakhshi, Payam, Mahmoudi, Elham, Majidi, Mir Mostafa, Sohrabi, Hessamaddin, Amini, Mohammad, Majidi, Mir Reza, Niaei, Aligholi, Shaykh-Baygloo, Nima, Mokhtarzadeh, Ahad
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9953341/
https://www.ncbi.nlm.nih.gov/pubmed/36831939
http://dx.doi.org/10.3390/bios13020172
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author Shahbazi-Derakhshi, Payam
Mahmoudi, Elham
Majidi, Mir Mostafa
Sohrabi, Hessamaddin
Amini, Mohammad
Majidi, Mir Reza
Niaei, Aligholi
Shaykh-Baygloo, Nima
Mokhtarzadeh, Ahad
author_facet Shahbazi-Derakhshi, Payam
Mahmoudi, Elham
Majidi, Mir Mostafa
Sohrabi, Hessamaddin
Amini, Mohammad
Majidi, Mir Reza
Niaei, Aligholi
Shaykh-Baygloo, Nima
Mokhtarzadeh, Ahad
author_sort Shahbazi-Derakhshi, Payam
collection PubMed
description In the present research work, the state-of-art label-free electrochemical genosensing platform was developed based on the hybridization process in the presence of [Fe(CN)(6)](3−/4−) as an efficient redox probe for sensitive recognition of the miRNA-21 in human gastric cell lines samples. To attain this aim, perovskite nanosheets were initially synthesized. Afterward, the obtained compound was combined with the graphene oxide resulting in an effective electrochemical modifier, which was dropped on the surface of the Au electrode. Then, AuNPs (Gold Nano Particles) have been electrochemically-immobilized on perovskite-graphene oxide/Au-modified electrode surface through the chronoamperometry (CA) technique. Finally, a self-assembling monolayer reaction of ss-capture RNA ensued by the thiol group at the end of the probe with AuNPs on the modified electrode surface. miRNA-21 has been cast on the Au electrode surface to apply the hybridization process. To find out the effectiveness of the synthesized modifier agent, the electrochemical behavior of the modified electrode has been analyzed through DPV (differential pulse voltammetry) and CV (cyclic voltammetry) techniques. The prepared biomarker-detection bioassay offers high sensitivity and specificity, good performance, and appropriate precision and accuracy for the highly-sensitive determination of miRNA-21. Different characterization methods have been used, such as XRD, Raman, EDS, and FE-SEM, for morphological characterization and investigation of particle size. Based on optimal conditions, the limit of detection and quantification have been acquired at 2.94 fM and 8.75 fM, respectively. Furthermore, it was possible to achieve a wide linear range which is between 10(−14) and 10(−7) for miRNA-21. Moreover, the selectivity of the proposed biosensing assay was investigated through its potential in the detection of one, two, and three-base mismatched sequences. Moreover, it was possible to investigate the repeatability and reproducibility of the related bio-assay. To evaluate the hybridization process, it is important that the planned biomarker detection bio-assay could be directly re-used and re-generated.
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spelling pubmed-99533412023-02-25 An Ultrasensitive miRNA-Based Genosensor for Detection of MicroRNA 21 in Gastric Cancer Cells Based on Functional Signal Amplifier and Synthesized Perovskite-Graphene Oxide and AuNPs Shahbazi-Derakhshi, Payam Mahmoudi, Elham Majidi, Mir Mostafa Sohrabi, Hessamaddin Amini, Mohammad Majidi, Mir Reza Niaei, Aligholi Shaykh-Baygloo, Nima Mokhtarzadeh, Ahad Biosensors (Basel) Article In the present research work, the state-of-art label-free electrochemical genosensing platform was developed based on the hybridization process in the presence of [Fe(CN)(6)](3−/4−) as an efficient redox probe for sensitive recognition of the miRNA-21 in human gastric cell lines samples. To attain this aim, perovskite nanosheets were initially synthesized. Afterward, the obtained compound was combined with the graphene oxide resulting in an effective electrochemical modifier, which was dropped on the surface of the Au electrode. Then, AuNPs (Gold Nano Particles) have been electrochemically-immobilized on perovskite-graphene oxide/Au-modified electrode surface through the chronoamperometry (CA) technique. Finally, a self-assembling monolayer reaction of ss-capture RNA ensued by the thiol group at the end of the probe with AuNPs on the modified electrode surface. miRNA-21 has been cast on the Au electrode surface to apply the hybridization process. To find out the effectiveness of the synthesized modifier agent, the electrochemical behavior of the modified electrode has been analyzed through DPV (differential pulse voltammetry) and CV (cyclic voltammetry) techniques. The prepared biomarker-detection bioassay offers high sensitivity and specificity, good performance, and appropriate precision and accuracy for the highly-sensitive determination of miRNA-21. Different characterization methods have been used, such as XRD, Raman, EDS, and FE-SEM, for morphological characterization and investigation of particle size. Based on optimal conditions, the limit of detection and quantification have been acquired at 2.94 fM and 8.75 fM, respectively. Furthermore, it was possible to achieve a wide linear range which is between 10(−14) and 10(−7) for miRNA-21. Moreover, the selectivity of the proposed biosensing assay was investigated through its potential in the detection of one, two, and three-base mismatched sequences. Moreover, it was possible to investigate the repeatability and reproducibility of the related bio-assay. To evaluate the hybridization process, it is important that the planned biomarker detection bio-assay could be directly re-used and re-generated. MDPI 2023-01-22 /pmc/articles/PMC9953341/ /pubmed/36831939 http://dx.doi.org/10.3390/bios13020172 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Shahbazi-Derakhshi, Payam
Mahmoudi, Elham
Majidi, Mir Mostafa
Sohrabi, Hessamaddin
Amini, Mohammad
Majidi, Mir Reza
Niaei, Aligholi
Shaykh-Baygloo, Nima
Mokhtarzadeh, Ahad
An Ultrasensitive miRNA-Based Genosensor for Detection of MicroRNA 21 in Gastric Cancer Cells Based on Functional Signal Amplifier and Synthesized Perovskite-Graphene Oxide and AuNPs
title An Ultrasensitive miRNA-Based Genosensor for Detection of MicroRNA 21 in Gastric Cancer Cells Based on Functional Signal Amplifier and Synthesized Perovskite-Graphene Oxide and AuNPs
title_full An Ultrasensitive miRNA-Based Genosensor for Detection of MicroRNA 21 in Gastric Cancer Cells Based on Functional Signal Amplifier and Synthesized Perovskite-Graphene Oxide and AuNPs
title_fullStr An Ultrasensitive miRNA-Based Genosensor for Detection of MicroRNA 21 in Gastric Cancer Cells Based on Functional Signal Amplifier and Synthesized Perovskite-Graphene Oxide and AuNPs
title_full_unstemmed An Ultrasensitive miRNA-Based Genosensor for Detection of MicroRNA 21 in Gastric Cancer Cells Based on Functional Signal Amplifier and Synthesized Perovskite-Graphene Oxide and AuNPs
title_short An Ultrasensitive miRNA-Based Genosensor for Detection of MicroRNA 21 in Gastric Cancer Cells Based on Functional Signal Amplifier and Synthesized Perovskite-Graphene Oxide and AuNPs
title_sort ultrasensitive mirna-based genosensor for detection of microrna 21 in gastric cancer cells based on functional signal amplifier and synthesized perovskite-graphene oxide and aunps
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9953341/
https://www.ncbi.nlm.nih.gov/pubmed/36831939
http://dx.doi.org/10.3390/bios13020172
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