Comparison of the ABC and ACMG systems for variant classification

Gunnar Houge; Eirik Bratland; Ingvild Aukrust; Kristian Tveten; Gabrielė Žukauskaitė; Ivona Sansovic; Alejandro J. Brea-Fernández; Karin Mayer; Teija Paakkola; Caoimhe McKenna; William Wright; Milica Keckarevic Markovic; Dorte L. Lildballe; Michal Konecny; Thomas Smol; Pia Alhopuro; Estelle Arnaud Gouttenoire; Katharina Obeid; Albena Todorova; Milena Jankovic; Joanna M. Lubieniecka; Maja Stojiljkovic; Marie Pierre Buisine; Bjørn Ivar Haukanes; Marie Lorans; Hanno Roomere; François M. Petit; Maria K. Haanpää; Claire Beneteau; Belén Pérez; Dijana Plaseska-Karanfilska; Matthias Rath; Nico Fuhrmann; Bibiana I. Ferreira; Coralea Stephanou; Wenche Sjursen; Aleš Maver; Cécile Rouzier; Adela Chirita-Emandi; João Gonçalves; Wei Cheng David Kuek; Martin Broly; Lonneke Haer-Wigman; Meow Keong Thong; Sok Kun Tae; Michaela Hyblova; Johan T. den Dunnen; Andreas Laner

doi:10.1038/s41431-024-01617-8

Comparison of the ABC and ACMG systems for variant classification

Gunnar Houge, Eirik Bratland, Ingvild Aukrust, Kristian Tveten, Gabrielė Žukauskaitė, Ivona Sansovic, Alejandro J. Brea-Fernández, Karin Mayer, Teija Paakkola, Caoimhe McKenna, William Wright, Milica Keckarevic Markovic, Dorte L. Lildballe, Michal Konecny, Thomas Smol, Pia Alhopuro, Estelle Arnaud Gouttenoire, Katharina Obeid, Albena Todorova, Milena JankovicJoanna M. Lubieniecka, Maja Stojiljkovic, Marie Pierre Buisine, Bjørn Ivar Haukanes, Marie Lorans, Hanno Roomere, François M. Petit, Maria K. Haanpää, Claire Beneteau, Belén Pérez, Dijana Plaseska-Karanfilska, Matthias Rath, Nico Fuhrmann, Bibiana I. Ferreira, Coralea Stephanou, Wenche Sjursen, Aleš Maver, Cécile Rouzier, Adela Chirita-Emandi, João Gonçalves, Wei Cheng David Kuek, Martin Broly, Lonneke Haer-Wigman, Meow Keong Thong, Sok Kun Tae, Michaela Hyblova, Johan T. den Dunnen, Andreas Laner

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Sammanfattning

The ABC and ACMG variant classification systems were compared by asking mainly European clinical laboratories to classify variants in 10 challenging cases using both systems, and to state if the variant in question would be reported as a relevant result or not as a measure of clinical utility. In contrast to the ABC system, the ACMG system was not made to guide variant reporting but to determine the likelihood of pathogenicity. Nevertheless, this comparison is justified since the ACMG class determines variant reporting in many laboratories. Forty-three laboratories participated in the survey. In seven cases, the classification system used did not influence the reporting likelihood when variants labeled as “maybe report” after ACMG-based classification were included. In three cases of population frequent but disease-associated variants, there was a difference in favor of reporting after ABC classification. A possible reason is that ABC step C (standard variant comments) allows a variant to be reported in one clinical setting but not another, e.g., based on Bayesian-based likelihood calculation of clinical relevance. Finally, the selection of ACMG criteria was compared between 36 laboratories. When excluding criteria used by less than four laboratories (<10%), the average concordance rate was 46%. Taken together, ABC-based classification is more clear-cut than ACMG-based classification since molecular and clinical information is handled separately, and variant reporting can be adapted to the clinical question and phenotype. Furthermore, variants do not get a clinically inappropriate label, like pathogenic when not pathogenic in a clinical context, or variant of unknown significance when the significance is known.

Originalspråk	engelska
Tidskrift	European Journal of Human Genetics
Volym	32
Sidor (från-till)	858-863
Antal sidor	6
ISSN	1018-4813
DOI	https://doi.org/10.1038/s41431-024-01617-8
Status	Publicerad - 2024
MoE-publikationstyp	A1 Tidskriftsartikel-refererad

Bibliografisk information

Publisher Copyright:
© The Author(s) 2024.

Vetenskapsgrenar

3111 Biomedicinska vetenskaper
1184 Genetik, utvecklingsbiologi, fysiologi

Åtkomst av dokument

10.1038/s41431-024-01617-8

s41431-024-01617-8Slutlig publicerad version, 995 KBLicens: CC BY

Citera det här

Houge, G., Bratland, E., Aukrust, I., Tveten, K., Žukauskaitė, G., Sansovic, I., Brea-Fernández, A. J., Mayer, K., Paakkola, T., McKenna, C., Wright, W., Markovic, M. K., Lildballe, D. L., Konecny, M., Smol, T., Alhopuro, P., Gouttenoire, E. A., Obeid, K., Todorova, A., ... Laner, A. (2024). Comparison of the ABC and ACMG systems for variant classification. European Journal of Human Genetics, 32, 858-863. https://doi.org/10.1038/s41431-024-01617-8

@article{ef25d969aa25439ba6a94bd90ec5d772,

title = "Comparison of the ABC and ACMG systems for variant classification",

abstract = "The ABC and ACMG variant classification systems were compared by asking mainly European clinical laboratories to classify variants in 10 challenging cases using both systems, and to state if the variant in question would be reported as a relevant result or not as a measure of clinical utility. In contrast to the ABC system, the ACMG system was not made to guide variant reporting but to determine the likelihood of pathogenicity. Nevertheless, this comparison is justified since the ACMG class determines variant reporting in many laboratories. Forty-three laboratories participated in the survey. In seven cases, the classification system used did not influence the reporting likelihood when variants labeled as “maybe report” after ACMG-based classification were included. In three cases of population frequent but disease-associated variants, there was a difference in favor of reporting after ABC classification. A possible reason is that ABC step C (standard variant comments) allows a variant to be reported in one clinical setting but not another, e.g., based on Bayesian-based likelihood calculation of clinical relevance. Finally, the selection of ACMG criteria was compared between 36 laboratories. When excluding criteria used by less than four laboratories (<10%), the average concordance rate was 46%. Taken together, ABC-based classification is more clear-cut than ACMG-based classification since molecular and clinical information is handled separately, and variant reporting can be adapted to the clinical question and phenotype. Furthermore, variants do not get a clinically inappropriate label, like pathogenic when not pathogenic in a clinical context, or variant of unknown significance when the significance is known.",

keywords = "3111 Biomedicine, 1184 Genetics, developmental biology, physiology",

author = "Gunnar Houge and Eirik Bratland and Ingvild Aukrust and Kristian Tveten and Gabrielė {\v Z}ukauskaitė and Ivona Sansovic and Brea-Fern{\'a}ndez, {Alejandro J.} and Karin Mayer and Teija Paakkola and Caoimhe McKenna and William Wright and Markovic, {Milica Keckarevic} and Lildballe, {Dorte L.} and Michal Konecny and Thomas Smol and Pia Alhopuro and Gouttenoire, {Estelle Arnaud} and Katharina Obeid and Albena Todorova and Milena Jankovic and Lubieniecka, {Joanna M.} and Maja Stojiljkovic and Buisine, {Marie Pierre} and Haukanes, {Bj{\o}rn Ivar} and Marie Lorans and Hanno Roomere and Petit, {Fran{\c c}ois M.} and Haanp{\"a}{\"a}, {Maria K.} and Claire Beneteau and Bel{\'e}n P{\'e}rez and Dijana Plaseska-Karanfilska and Matthias Rath and Nico Fuhrmann and Ferreira, {Bibiana I.} and Coralea Stephanou and Wenche Sjursen and Ale{\v s} Maver and C{\'e}cile Rouzier and Adela Chirita-Emandi and Jo{\~a}o Gon{\c c}alves and Kuek, {Wei Cheng David} and Martin Broly and Lonneke Haer-Wigman and Thong, {Meow Keong} and Tae, {Sok Kun} and Michaela Hyblova and {den Dunnen}, {Johan T.} and Andreas Laner",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2024",

doi = "10.1038/s41431-024-01617-8",

language = "English",

volume = "32",

pages = "858--863",

journal = "European Journal of Human Genetics",

issn = "1018-4813",

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Houge, G, Bratland, E, Aukrust, I, Tveten, K, Žukauskaitė, G, Sansovic, I, Brea-Fernández, AJ, Mayer, K, Paakkola, T, McKenna, C, Wright, W, Markovic, MK, Lildballe, DL, Konecny, M, Smol, T, Alhopuro, P, Gouttenoire, EA, Obeid, K, Todorova, A, Jankovic, M, Lubieniecka, JM, Stojiljkovic, M, Buisine, MP, Haukanes, BI, Lorans, M, Roomere, H, Petit, FM, Haanpää, MK, Beneteau, C, Pérez, B, Plaseska-Karanfilska, D, Rath, M, Fuhrmann, N, Ferreira, BI, Stephanou, C, Sjursen, W, Maver, A, Rouzier, C, Chirita-Emandi, A, Gonçalves, J, Kuek, WCD, Broly, M, Haer-Wigman, L, Thong, MK, Tae, SK, Hyblova, M, den Dunnen, JT & Laner, A 2024, 'Comparison of the ABC and ACMG systems for variant classification', European Journal of Human Genetics, vol. 32, s. 858-863. https://doi.org/10.1038/s41431-024-01617-8

TY - JOUR

T1 - Comparison of the ABC and ACMG systems for variant classification

AU - Houge, Gunnar

AU - Bratland, Eirik

AU - Aukrust, Ingvild

AU - Tveten, Kristian

AU - Žukauskaitė, Gabrielė

AU - Sansovic, Ivona

AU - Brea-Fernández, Alejandro J.

AU - Mayer, Karin

AU - Paakkola, Teija

AU - McKenna, Caoimhe

AU - Wright, William

AU - Markovic, Milica Keckarevic

AU - Lildballe, Dorte L.

AU - Konecny, Michal

AU - Smol, Thomas

AU - Alhopuro, Pia

AU - Gouttenoire, Estelle Arnaud

AU - Obeid, Katharina

AU - Todorova, Albena

AU - Jankovic, Milena

AU - Lubieniecka, Joanna M.

AU - Stojiljkovic, Maja

AU - Buisine, Marie Pierre

AU - Haukanes, Bjørn Ivar

AU - Lorans, Marie

AU - Roomere, Hanno

AU - Petit, François M.

AU - Haanpää, Maria K.

AU - Beneteau, Claire

AU - Pérez, Belén

AU - Plaseska-Karanfilska, Dijana

AU - Rath, Matthias

AU - Fuhrmann, Nico

AU - Ferreira, Bibiana I.

AU - Stephanou, Coralea

AU - Sjursen, Wenche

AU - Maver, Aleš

AU - Rouzier, Cécile

AU - Chirita-Emandi, Adela

AU - Gonçalves, João

AU - Kuek, Wei Cheng David

AU - Broly, Martin

AU - Haer-Wigman, Lonneke

AU - Thong, Meow Keong

AU - Tae, Sok Kun

AU - Hyblova, Michaela

AU - den Dunnen, Johan T.

AU - Laner, Andreas

PY - 2024

Y1 - 2024

N2 - The ABC and ACMG variant classification systems were compared by asking mainly European clinical laboratories to classify variants in 10 challenging cases using both systems, and to state if the variant in question would be reported as a relevant result or not as a measure of clinical utility. In contrast to the ABC system, the ACMG system was not made to guide variant reporting but to determine the likelihood of pathogenicity. Nevertheless, this comparison is justified since the ACMG class determines variant reporting in many laboratories. Forty-three laboratories participated in the survey. In seven cases, the classification system used did not influence the reporting likelihood when variants labeled as “maybe report” after ACMG-based classification were included. In three cases of population frequent but disease-associated variants, there was a difference in favor of reporting after ABC classification. A possible reason is that ABC step C (standard variant comments) allows a variant to be reported in one clinical setting but not another, e.g., based on Bayesian-based likelihood calculation of clinical relevance. Finally, the selection of ACMG criteria was compared between 36 laboratories. When excluding criteria used by less than four laboratories (<10%), the average concordance rate was 46%. Taken together, ABC-based classification is more clear-cut than ACMG-based classification since molecular and clinical information is handled separately, and variant reporting can be adapted to the clinical question and phenotype. Furthermore, variants do not get a clinically inappropriate label, like pathogenic when not pathogenic in a clinical context, or variant of unknown significance when the significance is known.

AB - The ABC and ACMG variant classification systems were compared by asking mainly European clinical laboratories to classify variants in 10 challenging cases using both systems, and to state if the variant in question would be reported as a relevant result or not as a measure of clinical utility. In contrast to the ABC system, the ACMG system was not made to guide variant reporting but to determine the likelihood of pathogenicity. Nevertheless, this comparison is justified since the ACMG class determines variant reporting in many laboratories. Forty-three laboratories participated in the survey. In seven cases, the classification system used did not influence the reporting likelihood when variants labeled as “maybe report” after ACMG-based classification were included. In three cases of population frequent but disease-associated variants, there was a difference in favor of reporting after ABC classification. A possible reason is that ABC step C (standard variant comments) allows a variant to be reported in one clinical setting but not another, e.g., based on Bayesian-based likelihood calculation of clinical relevance. Finally, the selection of ACMG criteria was compared between 36 laboratories. When excluding criteria used by less than four laboratories (<10%), the average concordance rate was 46%. Taken together, ABC-based classification is more clear-cut than ACMG-based classification since molecular and clinical information is handled separately, and variant reporting can be adapted to the clinical question and phenotype. Furthermore, variants do not get a clinically inappropriate label, like pathogenic when not pathogenic in a clinical context, or variant of unknown significance when the significance is known.

KW - 3111 Biomedicine

KW - 1184 Genetics, developmental biology, physiology

U2 - 10.1038/s41431-024-01617-8

DO - 10.1038/s41431-024-01617-8

M3 - Article

AN - SCOPUS:85193793451

SN - 1018-4813

VL - 32

SP - 858

EP - 863

JO - European Journal of Human Genetics

JF - European Journal of Human Genetics

ER -