Multi-center real-world comparison of the fully automated Idylla™ microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer

Ana Velasco; Fatma Tokat; Jesper Bonde; Nicola Trim; Elisabeth Bauer; Adam Meeney; Wendy de Leng; George Chong; Véronique Dalstein; Lorand L. Kis; Jon A. Lorentzen; Snjezana Tomić; Keeley Thwaites; Martina Putzová; Astrid Birnbaum; Romena Qazi; Vanessa Primmer; Barbara Dockhorn-Dworniczak; Javier Hernández-Losa; Fernando A. Soares; Asaf A. Gertler; Michal Kalman; Chris Wong; Dirce M. Carraro; Ana C. Sousa; Rui M. Reis; Stephen B. Fox; Matteo Fassan; Marie Brevet; Sabine Merkelbach-Bruse; Richard Colling; Elizabeth Soilleux; Ryan Yee Wei Teo; Nicky D’Haene; Serge Nolet; Ari Ristimäki; Timo Väisänen; Caroline Chapusot; Afsaneh Soruri; Tina Unger; Johanna Wecgowiec; Michele Biscuola; Milo Frattini; Anna Long; Paulo V. Campregher; Xavier Matias-Guiu

doi:10.1007/s00428-020-02962-x

Multi-center real-world comparison of the fully automated Idylla™ microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer

Ana Velasco^*, Fatma Tokat, Jesper Bonde, Nicola Trim, Elisabeth Bauer, Adam Meeney, Wendy de Leng, George Chong, Véronique Dalstein, Lorand L. Kis, Jon A. Lorentzen, Snjezana Tomić, Keeley Thwaites, Martina Putzová, Astrid Birnbaum, Romena Qazi, Vanessa Primmer, Barbara Dockhorn-Dworniczak, Javier Hernández-Losa, Fernando A. SoaresAsaf A. Gertler, Michal Kalman, Chris Wong, Dirce M. Carraro, Ana C. Sousa, Rui M. Reis, Stephen B. Fox, Matteo Fassan, Marie Brevet, Sabine Merkelbach-Bruse, Richard Colling, Elizabeth Soilleux, Ryan Yee Wei Teo, Nicky D’Haene, Serge Nolet, Ari Ristimäki, Timo Väisänen, Caroline Chapusot, Afsaneh Soruri, Tina Unger, Johanna Wecgowiec, Michele Biscuola, Milo Frattini, Anna Long, Paulo V. Campregher, Xavier Matias-Guiu

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

Abstract

Microsatellite instability (MSI) is present in 15–20% of primary colorectal cancers. MSI status is assessed to detect Lynch syndrome, guide adjuvant chemotherapy, determine prognosis, and use as a companion test for checkpoint blockade inhibitors. Traditionally, MSI status is determined by immunohistochemistry or molecular methods. The Idylla™ MSI Assay is a fully automated molecular method (including automated result interpretation), using seven novel MSI biomarkers (ACVR2A, BTBD7, DIDO1, MRE11, RYR3, SEC31A, SULF2) and not requiring matched normal tissue. In this real-world global study, 44 clinical centers performed Idylla™ testing on a total of 1301 archived colorectal cancer formalin-fixed, paraffin-embedded (FFPE) tissue sections and compared Idylla™ results against available results from routine diagnostic testing in those sites. MSI mutations detected with the Idylla™ MSI Assay were equally distributed over the seven biomarkers, and 84.48% of the MSI-high samples had ≥ 5 mutated biomarkers, while 98.25% of the microsatellite-stable samples had zero mutated biomarkers. The concordance level between the Idylla™ MSI Assay and immunohistochemistry was 96.39% (988/1025); 17/37 discordant samples were found to be concordant when a third method was used. Compared with routine molecular methods, the concordance level was 98.01% (789/805); third-method analysis found concordance for 8/16 discordant samples. The failure rate of the Idylla™ MSI Assay (0.23%; 3/1301) was lower than that of referenced immunohistochemistry (4.37%; 47/1075) or molecular assays (0.86%; 7/812). In conclusion, lower failure rates and high concordance levels were found between the Idylla™ MSI Assay and routine tests.

Original language	English
Pages (from-to)	851-863
Number of pages	13
Journal	Virchows Archiv
Volume	478
Issue number	5
DOIs	https://doi.org/10.1007/s00428-020-02962-x
Publication status	Published - May 2021
Externally published	Yes

ASJC Scopus subject areas

Pathology and Forensic Medicine
Molecular Biology
Cell Biology

Keywords

Colorectal cancer
FFPE clinical tissue samples
Idylla™ MSI assay
Microsatellite instability
Multi-center study

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1007/s00428-020-02962-x

Fingerprint

Dive into the research topics of 'Multi-center real-world comparison of the fully automated Idylla™ microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer'. Together they form a unique fingerprint.

Cite this

Velasco, A., Tokat, F., Bonde, J., Trim, N., Bauer, E., Meeney, A., de Leng, W., Chong, G., Dalstein, V., Kis, L. L., Lorentzen, J. A., Tomić, S., Thwaites, K., Putzová, M., Birnbaum, A., Qazi, R., Primmer, V., Dockhorn-Dworniczak, B., Hernández-Losa, J., ... Matias-Guiu, X. (2021). Multi-center real-world comparison of the fully automated Idylla™ microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer. Virchows Archiv, 478(5), 851-863. https://doi.org/10.1007/s00428-020-02962-x

@article{3377731a90ae4a42a3e13e0afde179c0,

title = "Multi-center real-world comparison of the fully automated Idylla{\texttrademark} microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer",

abstract = "Microsatellite instability (MSI) is present in 15–20\% of primary colorectal cancers. MSI status is assessed to detect Lynch syndrome, guide adjuvant chemotherapy, determine prognosis, and use as a companion test for checkpoint blockade inhibitors. Traditionally, MSI status is determined by immunohistochemistry or molecular methods. The Idylla{\texttrademark} MSI Assay is a fully automated molecular method (including automated result interpretation), using seven novel MSI biomarkers (ACVR2A, BTBD7, DIDO1, MRE11, RYR3, SEC31A, SULF2) and not requiring matched normal tissue. In this real-world global study, 44 clinical centers performed Idylla{\texttrademark} testing on a total of 1301 archived colorectal cancer formalin-fixed, paraffin-embedded (FFPE) tissue sections and compared Idylla{\texttrademark} results against available results from routine diagnostic testing in those sites. MSI mutations detected with the Idylla{\texttrademark} MSI Assay were equally distributed over the seven biomarkers, and 84.48\% of the MSI-high samples had ≥ 5 mutated biomarkers, while 98.25\% of the microsatellite-stable samples had zero mutated biomarkers. The concordance level between the Idylla{\texttrademark} MSI Assay and immunohistochemistry was 96.39\% (988/1025); 17/37 discordant samples were found to be concordant when a third method was used. Compared with routine molecular methods, the concordance level was 98.01\% (789/805); third-method analysis found concordance for 8/16 discordant samples. The failure rate of the Idylla{\texttrademark} MSI Assay (0.23\%; 3/1301) was lower than that of referenced immunohistochemistry (4.37\%; 47/1075) or molecular assays (0.86\%; 7/812). In conclusion, lower failure rates and high concordance levels were found between the Idylla{\texttrademark} MSI Assay and routine tests.",

keywords = "Colorectal cancer, FFPE clinical tissue samples, Idylla{\texttrademark} MSI assay, Microsatellite instability, Multi-center study",

author = "Ana Velasco and Fatma Tokat and Jesper Bonde and Nicola Trim and Elisabeth Bauer and Adam Meeney and \{de Leng\}, Wendy and George Chong and V{\'e}ronique Dalstein and Kis, \{Lorand L.\} and Lorentzen, \{Jon A.\} and Snjezana Tomi{\'c} and Keeley Thwaites and Martina Putzov{\'a} and Astrid Birnbaum and Romena Qazi and Vanessa Primmer and Barbara Dockhorn-Dworniczak and Javier Hern{\'a}ndez-Losa and Soares, \{Fernando A.\} and Gertler, \{Asaf A.\} and Michal Kalman and Chris Wong and Carraro, \{Dirce M.\} and Sousa, \{Ana C.\} and Reis, \{Rui M.\} and Fox, \{Stephen B.\} and Matteo Fassan and Marie Brevet and Sabine Merkelbach-Bruse and Richard Colling and Elizabeth Soilleux and Teo, \{Ryan Yee Wei\} and Nicky D{\textquoteright}Haene and Serge Nolet and Ari Ristim{\"a}ki and Timo V{\"a}is{\"a}nen and Caroline Chapusot and Afsaneh Soruri and Tina Unger and Johanna Wecgowiec and Michele Biscuola and Milo Frattini and Anna Long and Campregher, \{Paulo V.\} and Xavier Matias-Guiu",

note = "Publisher Copyright: {\textcopyright} 2020, The Author(s).",

year = "2021",

month = may,

doi = "10.1007/s00428-020-02962-x",

language = "English",

volume = "478",

pages = "851--863",

journal = "Virchows Archiv",

issn = "0945-6317",

publisher = "Springer Science and Business Media Deutschland GmbH",

number = "5",

}

Velasco, A, Tokat, F, Bonde, J, Trim, N, Bauer, E, Meeney, A, de Leng, W, Chong, G, Dalstein, V, Kis, LL, Lorentzen, JA, Tomić, S, Thwaites, K, Putzová, M, Birnbaum, A, Qazi, R, Primmer, V, Dockhorn-Dworniczak, B, Hernández-Losa, J, Soares, FA, Gertler, AA, Kalman, M, Wong, C, Carraro, DM, Sousa, AC, Reis, RM, Fox, SB, Fassan, M, Brevet, M, Merkelbach-Bruse, S, Colling, R, Soilleux, E, Teo, RYW, D’Haene, N, Nolet, S, Ristimäki, A, Väisänen, T, Chapusot, C, Soruri, A, Unger, T, Wecgowiec, J, Biscuola, M, Frattini, M, Long, A, Campregher, PV & Matias-Guiu, X 2021, 'Multi-center real-world comparison of the fully automated Idylla™ microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer', Virchows Archiv, vol. 478, no. 5, pp. 851-863. https://doi.org/10.1007/s00428-020-02962-x

Multi-center real-world comparison of the fully automated Idylla™ microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer. / Velasco, Ana; Tokat, Fatma; Bonde, Jesper et al.
In: Virchows Archiv, Vol. 478, No. 5, 05.2021, p. 851-863.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - Multi-center real-world comparison of the fully automated Idylla™ microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer

AU - Velasco, Ana

AU - Tokat, Fatma

AU - Bonde, Jesper

AU - Trim, Nicola

AU - Bauer, Elisabeth

AU - Meeney, Adam

AU - de Leng, Wendy

AU - Chong, George

AU - Dalstein, Véronique

AU - Kis, Lorand L.

AU - Lorentzen, Jon A.

AU - Tomić, Snjezana

AU - Thwaites, Keeley

AU - Putzová, Martina

AU - Birnbaum, Astrid

AU - Qazi, Romena

AU - Primmer, Vanessa

AU - Dockhorn-Dworniczak, Barbara

AU - Hernández-Losa, Javier

AU - Soares, Fernando A.

AU - Gertler, Asaf A.

AU - Kalman, Michal

AU - Wong, Chris

AU - Carraro, Dirce M.

AU - Sousa, Ana C.

AU - Reis, Rui M.

AU - Fox, Stephen B.

AU - Fassan, Matteo

AU - Brevet, Marie

AU - Merkelbach-Bruse, Sabine

AU - Colling, Richard

AU - Soilleux, Elizabeth

AU - Teo, Ryan Yee Wei

AU - D’Haene, Nicky

AU - Nolet, Serge

AU - Ristimäki, Ari

AU - Väisänen, Timo

AU - Chapusot, Caroline

AU - Soruri, Afsaneh

AU - Unger, Tina

AU - Wecgowiec, Johanna

AU - Biscuola, Michele

AU - Frattini, Milo

AU - Long, Anna

AU - Campregher, Paulo V.

AU - Matias-Guiu, Xavier

PY - 2021/5

Y1 - 2021/5

N2 - Microsatellite instability (MSI) is present in 15–20% of primary colorectal cancers. MSI status is assessed to detect Lynch syndrome, guide adjuvant chemotherapy, determine prognosis, and use as a companion test for checkpoint blockade inhibitors. Traditionally, MSI status is determined by immunohistochemistry or molecular methods. The Idylla™ MSI Assay is a fully automated molecular method (including automated result interpretation), using seven novel MSI biomarkers (ACVR2A, BTBD7, DIDO1, MRE11, RYR3, SEC31A, SULF2) and not requiring matched normal tissue. In this real-world global study, 44 clinical centers performed Idylla™ testing on a total of 1301 archived colorectal cancer formalin-fixed, paraffin-embedded (FFPE) tissue sections and compared Idylla™ results against available results from routine diagnostic testing in those sites. MSI mutations detected with the Idylla™ MSI Assay were equally distributed over the seven biomarkers, and 84.48% of the MSI-high samples had ≥ 5 mutated biomarkers, while 98.25% of the microsatellite-stable samples had zero mutated biomarkers. The concordance level between the Idylla™ MSI Assay and immunohistochemistry was 96.39% (988/1025); 17/37 discordant samples were found to be concordant when a third method was used. Compared with routine molecular methods, the concordance level was 98.01% (789/805); third-method analysis found concordance for 8/16 discordant samples. The failure rate of the Idylla™ MSI Assay (0.23%; 3/1301) was lower than that of referenced immunohistochemistry (4.37%; 47/1075) or molecular assays (0.86%; 7/812). In conclusion, lower failure rates and high concordance levels were found between the Idylla™ MSI Assay and routine tests.

AB - Microsatellite instability (MSI) is present in 15–20% of primary colorectal cancers. MSI status is assessed to detect Lynch syndrome, guide adjuvant chemotherapy, determine prognosis, and use as a companion test for checkpoint blockade inhibitors. Traditionally, MSI status is determined by immunohistochemistry or molecular methods. The Idylla™ MSI Assay is a fully automated molecular method (including automated result interpretation), using seven novel MSI biomarkers (ACVR2A, BTBD7, DIDO1, MRE11, RYR3, SEC31A, SULF2) and not requiring matched normal tissue. In this real-world global study, 44 clinical centers performed Idylla™ testing on a total of 1301 archived colorectal cancer formalin-fixed, paraffin-embedded (FFPE) tissue sections and compared Idylla™ results against available results from routine diagnostic testing in those sites. MSI mutations detected with the Idylla™ MSI Assay were equally distributed over the seven biomarkers, and 84.48% of the MSI-high samples had ≥ 5 mutated biomarkers, while 98.25% of the microsatellite-stable samples had zero mutated biomarkers. The concordance level between the Idylla™ MSI Assay and immunohistochemistry was 96.39% (988/1025); 17/37 discordant samples were found to be concordant when a third method was used. Compared with routine molecular methods, the concordance level was 98.01% (789/805); third-method analysis found concordance for 8/16 discordant samples. The failure rate of the Idylla™ MSI Assay (0.23%; 3/1301) was lower than that of referenced immunohistochemistry (4.37%; 47/1075) or molecular assays (0.86%; 7/812). In conclusion, lower failure rates and high concordance levels were found between the Idylla™ MSI Assay and routine tests.

KW - Colorectal cancer

KW - FFPE clinical tissue samples

KW - Idylla™ MSI assay

KW - Microsatellite instability

KW - Multi-center study

UR - http://www.scopus.com/inward/record.url?scp=85095824973&partnerID=8YFLogxK

U2 - 10.1007/s00428-020-02962-x

DO - 10.1007/s00428-020-02962-x

M3 - Article

C2 - 33170334

AN - SCOPUS:85095824973

SN - 0945-6317

VL - 478

SP - 851

EP - 863

JO - Virchows Archiv

JF - Virchows Archiv

IS - 5

ER -

Multi-center real-world comparison of the fully automated Idylla™ microsatellite instability assay with routine molecular methods and immunohistochemistry on formalin-fixed paraffin-embedded tissue of colorectal cancer

Abstract

ASJC Scopus subject areas

Keywords

UN SDGs

Access to Document

Other files and links

Fingerprint

Cite this