Analysis of Clinical Samples of Pancreatic Cyst's Lesions with A Multi-Analyte Bioelectronic Simot Array Benchmarked Against Ultrasensitive Chemiluminescent Immunoassay

Cecilia Scandurra; Kim Björkström; Mariapia Caputo; Lucia Sarcina; Enrico Genco; Francesco Modena; Fabrizio Antonio Viola; Celestino Brunetti; Zsolt M. Kovács-Vajna; Cinzia Di Franco; Lena Haeberle; Piero Larizza; Maria Teresa Mancini; Ronald Österbacka; William Reeves; Gaetano Scamarcio; May Wheeler; Mario Caironi; Eugenio Cantatore; Fabrizio Torricelli; Irene Esposito; Eleonora Macchia; Luisa Torsi

doi:10.1002/advs.202308141

Analysis of Clinical Samples of Pancreatic Cyst's Lesions with A Multi-Analyte Bioelectronic Simot Array Benchmarked Against Ultrasensitive Chemiluminescent Immunoassay

Cecilia Scandurra, Kim Björkström, Mariapia Caputo, Lucia Sarcina, Enrico Genco, Francesco Modena, Fabrizio Antonio Viola, Celestino Brunetti, Zsolt M. Kovács-Vajna, Cinzia Di Franco, Lena Haeberle, Piero Larizza, Maria Teresa Mancini, Ronald Österbacka, William Reeves, Gaetano Scamarcio, May Wheeler, Mario Caironi, Eugenio Cantatore, Fabrizio TorricelliIrene Esposito, Eleonora Macchia (Corresponding author), Luisa Torsi (Corresponding author)

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Pancreatic cancer, ranking as the third factor in cancer-related deaths, necessitates enhanced diagnostic measures through early detection. In response, SiMoT-Single-molecule with a large Transistor multiplexing array, achieving a Technology Readiness Level of 5, is proposed for a timely identification of pancreatic cancer precursor cysts and is benchmarked against the commercially available chemiluminescent immunoassay SIMOA (Single molecule array) SP-X System. A cohort of 39 samples, comprising 33 cyst fluids and 6 blood plasma specimens, undergoes detailed examination with both technologies. The SiMoT array targets oncoproteins MUC1 and CD55, and oncogene KRAS, while the SIMOA SP-X planar technology exclusively focuses on MUC1 and CD55. Employing Principal Component Analysis (PCA) for multivariate data processing, the SiMoT array demonstrates effective discrimination of malignant/pre-invasive high-grade or potentially malignant low-grade pancreatic cysts from benign non-mucinous cysts. Conversely, PCA analysis applied to SIMOA assay reveals less effective differentiation ability among the three cyst classes. Notably, SiMoT unique capability of concurrently analyzing protein and genetic markers with the threshold of one single molecule in 0.1 mL positions it as a comprehensive and reliable diagnostic tool. The electronic response generated by the SiMoT array facilitates direct digital data communication, suggesting potential applications in the development of field-deployable liquid biopsy.

Originele taal-2	Engels
Artikelnummer	2308141
Pagina's (van-tot)	e2308141
Aantal pagina's	14
Tijdschrift	Advanced Science
Volume	11
Nummer van het tijdschrift	27
DOI's	https://doi.org/10.1002/advs.202308141
Status	Gepubliceerd - 17 jul. 2024

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Publisher Copyright:
© 2024 The Authors. Advanced Science published by Wiley-VCH GmbH.

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H2020 \u2013 Electronic Smart Systems \u2013 SiMBiT: Single\u2010molecule bio\u2010electronic smart system array for clinical testing (Grant agreement ID: 824946), NoOne\u2010A binary sensor with a single\u2010molecule digit to discriminate biofluids enclosing zero or at least one biomarker, ERC Stg2021, GA:101040383, Svenska Tekniska Vetenskapsakademien i Finland and CSGI are acknowledged for partial financial support. H2020 \u2013 Electronic Smart Systems \u2013 SiMBiT: Single-molecule bio-electronic smart system array for clinical testing (Grant agreement ID: 824946), NoOne-A binary sensor with a single-molecule digit to discriminate biofluids enclosing zero or at least one biomarker, ERC Stg2021, GA:101040383, Svenska Tekniska Vetenskapsakademien i Finland and CSGI are acknowledged for partial financial support.

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Scandurra, C., Björkström, K., Caputo, M., Sarcina, L., Genco, E., Modena, F., Viola, F. A., Brunetti, C., Kovács-Vajna, Z. M., Di Franco, C., Haeberle, L., Larizza, P., Mancini, M. T., Österbacka, R., Reeves, W., Scamarcio, G., Wheeler, M., Caironi, M., Cantatore, E., ... Torsi, L. (2024). Analysis of Clinical Samples of Pancreatic Cyst's Lesions with A Multi-Analyte Bioelectronic Simot Array Benchmarked Against Ultrasensitive Chemiluminescent Immunoassay. Advanced Science, 11(27), e2308141. Artikel 2308141. https://doi.org/10.1002/advs.202308141

@article{a53d25a61d114253b802dfd22a706919,

title = "Analysis of Clinical Samples of Pancreatic Cyst's Lesions with A Multi-Analyte Bioelectronic Simot Array Benchmarked Against Ultrasensitive Chemiluminescent Immunoassay",

abstract = "Pancreatic cancer, ranking as the third factor in cancer-related deaths, necessitates enhanced diagnostic measures through early detection. In response, SiMoT-Single-molecule with a large Transistor multiplexing array, achieving a Technology Readiness Level of 5, is proposed for a timely identification of pancreatic cancer precursor cysts and is benchmarked against the commercially available chemiluminescent immunoassay SIMOA (Single molecule array) SP-X System. A cohort of 39 samples, comprising 33 cyst fluids and 6 blood plasma specimens, undergoes detailed examination with both technologies. The SiMoT array targets oncoproteins MUC1 and CD55, and oncogene KRAS, while the SIMOA SP-X planar technology exclusively focuses on MUC1 and CD55. Employing Principal Component Analysis (PCA) for multivariate data processing, the SiMoT array demonstrates effective discrimination of malignant/pre-invasive high-grade or potentially malignant low-grade pancreatic cysts from benign non-mucinous cysts. Conversely, PCA analysis applied to SIMOA assay reveals less effective differentiation ability among the three cyst classes. Notably, SiMoT unique capability of concurrently analyzing protein and genetic markers with the threshold of one single molecule in 0.1 mL positions it as a comprehensive and reliable diagnostic tool. The electronic response generated by the SiMoT array facilitates direct digital data communication, suggesting potential applications in the development of field-deployable liquid biopsy.",

keywords = "bioelectronic transistors, liquid biopsy, multivariate data processing, SIMOA-single-molecule-array-, SiMoT-single-molecule-with-a-large-transistor, single-molecule biosensors, Immunoassay/methods, Pancreatic Cyst/diagnosis, Humans, Proto-Oncogene Proteins p21(ras)/genetics, Luminescent Measurements/methods, Biomarkers, Tumor/genetics, Pancreatic Neoplasms/diagnosis, Sensitivity and Specificity, Principal Component Analysis/methods",

author = "Cecilia Scandurra and Kim Bj{\"o}rkstr{\"o}m and Mariapia Caputo and Lucia Sarcina and Enrico Genco and Francesco Modena and Viola, {Fabrizio Antonio} and Celestino Brunetti and Kov{\'a}cs-Vajna, {Zsolt M.} and {Di Franco}, Cinzia and Lena Haeberle and Piero Larizza and Mancini, {Maria Teresa} and Ronald {\"O}sterbacka and William Reeves and Gaetano Scamarcio and May Wheeler and Mario Caironi and Eugenio Cantatore and Fabrizio Torricelli and Irene Esposito and Eleonora Macchia and Luisa Torsi",

note = "Publisher Copyright: {\textcopyright} 2024 The Authors. Advanced Science published by Wiley-VCH GmbH.",

year = "2024",

month = jul,

day = "17",

doi = "10.1002/advs.202308141",

language = "English",

volume = "11",

pages = "e2308141",

journal = "Advanced Science",

issn = "2198-3844",

publisher = "Wiley-VCH Verlag",

number = "27",

}

Scandurra, C, Björkström, K, Caputo, M, Sarcina, L, Genco, E, Modena, F, Viola, FA, Brunetti, C, Kovács-Vajna, ZM, Di Franco, C, Haeberle, L, Larizza, P, Mancini, MT, Österbacka, R, Reeves, W, Scamarcio, G, Wheeler, M, Caironi, M, Cantatore, E, Torricelli, F, Esposito, I, Macchia, E & Torsi, L 2024, 'Analysis of Clinical Samples of Pancreatic Cyst's Lesions with A Multi-Analyte Bioelectronic Simot Array Benchmarked Against Ultrasensitive Chemiluminescent Immunoassay', Advanced Science, vol. 11, nr. 27, 2308141, blz. e2308141. https://doi.org/10.1002/advs.202308141

Analysis of Clinical Samples of Pancreatic Cyst's Lesions with A Multi-Analyte Bioelectronic Simot Array Benchmarked Against Ultrasensitive Chemiluminescent Immunoassay. / Scandurra, Cecilia; Björkström, Kim; Caputo, Mariapia et al.
In: Advanced Science, Vol. 11, Nr. 27, 2308141, 17.07.2024, blz. e2308141.

Onderzoeksoutput: Bijdrage aan tijdschrift › Tijdschriftartikel › Academic › peer review

TY - JOUR

T1 - Analysis of Clinical Samples of Pancreatic Cyst's Lesions with A Multi-Analyte Bioelectronic Simot Array Benchmarked Against Ultrasensitive Chemiluminescent Immunoassay

AU - Scandurra, Cecilia

AU - Björkström, Kim

AU - Caputo, Mariapia

AU - Sarcina, Lucia

AU - Genco, Enrico

AU - Modena, Francesco

AU - Viola, Fabrizio Antonio

AU - Brunetti, Celestino

AU - Kovács-Vajna, Zsolt M.

AU - Di Franco, Cinzia

AU - Haeberle, Lena

AU - Larizza, Piero

AU - Mancini, Maria Teresa

AU - Österbacka, Ronald

AU - Reeves, William

AU - Scamarcio, Gaetano

AU - Wheeler, May

AU - Caironi, Mario

AU - Cantatore, Eugenio

AU - Torricelli, Fabrizio

AU - Esposito, Irene

AU - Macchia, Eleonora

AU - Torsi, Luisa

PY - 2024/7/17

Y1 - 2024/7/17

N2 - Pancreatic cancer, ranking as the third factor in cancer-related deaths, necessitates enhanced diagnostic measures through early detection. In response, SiMoT-Single-molecule with a large Transistor multiplexing array, achieving a Technology Readiness Level of 5, is proposed for a timely identification of pancreatic cancer precursor cysts and is benchmarked against the commercially available chemiluminescent immunoassay SIMOA (Single molecule array) SP-X System. A cohort of 39 samples, comprising 33 cyst fluids and 6 blood plasma specimens, undergoes detailed examination with both technologies. The SiMoT array targets oncoproteins MUC1 and CD55, and oncogene KRAS, while the SIMOA SP-X planar technology exclusively focuses on MUC1 and CD55. Employing Principal Component Analysis (PCA) for multivariate data processing, the SiMoT array demonstrates effective discrimination of malignant/pre-invasive high-grade or potentially malignant low-grade pancreatic cysts from benign non-mucinous cysts. Conversely, PCA analysis applied to SIMOA assay reveals less effective differentiation ability among the three cyst classes. Notably, SiMoT unique capability of concurrently analyzing protein and genetic markers with the threshold of one single molecule in 0.1 mL positions it as a comprehensive and reliable diagnostic tool. The electronic response generated by the SiMoT array facilitates direct digital data communication, suggesting potential applications in the development of field-deployable liquid biopsy.

AB - Pancreatic cancer, ranking as the third factor in cancer-related deaths, necessitates enhanced diagnostic measures through early detection. In response, SiMoT-Single-molecule with a large Transistor multiplexing array, achieving a Technology Readiness Level of 5, is proposed for a timely identification of pancreatic cancer precursor cysts and is benchmarked against the commercially available chemiluminescent immunoassay SIMOA (Single molecule array) SP-X System. A cohort of 39 samples, comprising 33 cyst fluids and 6 blood plasma specimens, undergoes detailed examination with both technologies. The SiMoT array targets oncoproteins MUC1 and CD55, and oncogene KRAS, while the SIMOA SP-X planar technology exclusively focuses on MUC1 and CD55. Employing Principal Component Analysis (PCA) for multivariate data processing, the SiMoT array demonstrates effective discrimination of malignant/pre-invasive high-grade or potentially malignant low-grade pancreatic cysts from benign non-mucinous cysts. Conversely, PCA analysis applied to SIMOA assay reveals less effective differentiation ability among the three cyst classes. Notably, SiMoT unique capability of concurrently analyzing protein and genetic markers with the threshold of one single molecule in 0.1 mL positions it as a comprehensive and reliable diagnostic tool. The electronic response generated by the SiMoT array facilitates direct digital data communication, suggesting potential applications in the development of field-deployable liquid biopsy.

KW - bioelectronic transistors

KW - liquid biopsy

KW - multivariate data processing

KW - SIMOA-single-molecule-array-

KW - SiMoT-single-molecule-with-a-large-transistor

KW - single-molecule biosensors

KW - Immunoassay/methods

KW - Pancreatic Cyst/diagnosis

KW - Humans

KW - Proto-Oncogene Proteins p21(ras)/genetics

KW - Luminescent Measurements/methods

KW - Biomarkers, Tumor/genetics

KW - Pancreatic Neoplasms/diagnosis

KW - Sensitivity and Specificity

KW - Principal Component Analysis/methods

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U2 - 10.1002/advs.202308141

DO - 10.1002/advs.202308141

M3 - Article

C2 - 38234100

AN - SCOPUS:85182849171

SN - 2198-3844

VL - 11

SP - e2308141

JO - Advanced Science

JF - Advanced Science

IS - 27

M1 - 2308141

ER -

Analysis of Clinical Samples of Pancreatic Cyst's Lesions with A Multi-Analyte Bioelectronic Simot Array Benchmarked Against Ultrasensitive Chemiluminescent Immunoassay

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