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      Porous Silicon-Based Aptasensors: Toward Cancer Protein Biomarker Detection

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          Abstract

          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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          Silicon quantum wire array fabrication by electrochemical and chemical dissolution of wafers

          L. Canham (1990)
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            A standardised static in vitro digestion method suitable for food - an international consensus.

            Simulated gastro-intestinal digestion is widely employed in many fields of food and nutritional sciences, as conducting human trials are often costly, resource intensive, and ethically disputable. As a consequence, in vitro alternatives that determine endpoints such as the bioaccessibility of nutrients and non-nutrients or the digestibility of macronutrients (e.g. lipids, proteins and carbohydrates) are used for screening and building new hypotheses. Various digestion models have been proposed, often impeding the possibility to compare results across research teams. For example, a large variety of enzymes from different sources such as of porcine, rabbit or human origin have been used, differing in their activity and characterization. Differences in pH, mineral type, ionic strength and digestion time, which alter enzyme activity and other phenomena, may also considerably alter results. Other parameters such as the presence of phospholipids, individual enzymes such as gastric lipase and digestive emulsifiers vs. their mixtures (e.g. pancreatin and bile salts), and the ratio of food bolus to digestive fluids, have also been discussed at length. In the present consensus paper, within the COST Infogest network, we propose a general standardised and practical static digestion method based on physiologically relevant conditions that can be applied for various endpoints, which may be amended to accommodate further specific requirements. A frameset of parameters including the oral, gastric and small intestinal digestion are outlined and their relevance discussed in relation to available in vivo data and enzymes. This consensus paper will give a detailed protocol and a line-by-line, guidance, recommendations and justifications but also limitation of the proposed model. This harmonised static, in vitro digestion method for food should aid the production of more comparable data in the future.
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              Visible light emission due to quantum size effects in highly porous crystalline silicon

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                Author and article information

                Journal
                ACS Meas Sci Au
                ACS Meas Sci Au
                tg
                amachv
                ACS Measurement Science Au
                American Chemical Society
                2694-250X
                25 August 2021
                20 October 2021
                : 1
                : 2
                : 82-94
                Affiliations
                []Department of Biotechnology and Food Engineering, Technion—Israel Institute of Technology , Haifa 3200003, Israel
                []Institute of Technical Chemistry, Leibniz Universität Hannover , Callinstraße 5, 30167 Hanover, Germany
                [§ ]Department of Electrical Engineering and Computer Science, Vanderbilt University , Nashville, Tennessee 37235, United States
                []The Russell Berrie Nanotechnology Institute, Technion—Israel Institute of Technology , Haifa 3200003, Israel
                Author notes
                Author information
                https://orcid.org/0000-0003-0915-7584
                https://orcid.org/0000-0003-2252-3104
                https://orcid.org/0000-0001-9472-754X
                Article
                10.1021/acsmeasuresciau.1c00019
                8532149
                34693403
                ffd89cbd-e9c3-4c25-94e1-635675dd31a8
                © 2021 The Authors. Published by American Chemical Society

                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/).

                History
                : 30 June 2021
                Funding
                Funded by: National Institutes of Health, doi 10.13039/100000002;
                Award ID: R21AI156693
                Funded by: Israel Science Foundation, doi 10.13039/501100003977;
                Award ID: 704/17
                Funded by: Deutsche Forschungsgemeinschaft, doi 10.13039/501100001659;
                Award ID: SCHE 279/32-1
                Categories
                Article
                Custom metadata
                tg1c00019
                tg1c00019

                optical biosensor,porous silicon,aptamer,anterior gradient homologue-2,cancer biomarker,label-free,microfluidics,isotachophoresis

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