TY - JOUR
T1 - Variant Classification Concordance using the ACMG-AMP Variant Interpretation Guidelines across Nine Genomic Implementation Research Studies
AU - Amendola, Laura M.
AU - Muenzen, Kathleen
AU - Biesecker, Leslie G.
AU - Bowling, Kevin M.
AU - Cooper, Greg M.
AU - Dorschner, Michael O.
AU - Driscoll, Catherine
AU - Foreman, Ann Katherine M.
AU - Golden-Grant, Katie
AU - Greally, John M.
AU - Hindorff, Lucia
AU - Kanavy, Dona
AU - Jobanputra, Vaidehi
AU - Johnston, Jennifer J.
AU - Kenny, Eimear E.
AU - McNulty, Shannon
AU - Murali, Priyanka
AU - Ou, Jeffrey
AU - Powell, Bradford C.
AU - Rehm, Heidi L.
AU - Rolf, Bradley
AU - Roman, Tamara S.
AU - Van Ziffle, Jessica
AU - Guha, Saurav
AU - Abhyankar, Avinash
AU - Crosslin, David
AU - Venner, Eric
AU - Yuan, Bo
AU - Zouk, Hana
AU - Jarvik, Gail P.
N1 - Publisher Copyright:
© 2020 American Society of Human Genetics
PY - 2020/11/5
Y1 - 2020/11/5
N2 - Harmonization of variant pathogenicity classification across laboratories is important for advancing clinical genomics. The two CLIA-accredited Electronic Medical Record and Genomics Network sequencing centers and the six CLIA-accredited laboratories and one research laboratory performing genome or exome sequencing in the Clinical Sequencing Evidence-Generating Research Consortium collaborated to explore current sources of discordance in classification. Eight laboratories each submitted 20 classified variants in the ACMG secondary finding v.2.0 genes. After removing duplicates, each of the 158 variants was annotated and independently classified by two additional laboratories using the ACMG-AMP guidelines. Overall concordance across three laboratories was assessed and discordant variants were reviewed via teleconference and email. The submitted variant set included 28 P/LP variants, 96 VUS, and 34 LB/B variants, mostly in cancer (40%) and cardiac (27%) risk genes. Eighty-six (54%) variants reached complete five-category (i.e., P, LP, VUS, LB, B) concordance, and 17 (11%) had a discordance that could affect clinical recommendations (P/LP versus VUS/LB/B). 21% and 63% of variants submitted as P and LP, respectively, were discordant with VUS. Of the 54 originally discordant variants that underwent further review, 32 reached agreement, for a post-review concordance rate of 84% (118/140 variants). This project provides an updated estimate of variant concordance, identifies considerations for LP classified variants, and highlights ongoing sources of discordance. Continued and increased sharing of variant classifications and evidence across laboratories, and the ongoing work of ClinGen to provide general as well as gene- and disease-specific guidance, will lead to continued increases in concordance.
AB - Harmonization of variant pathogenicity classification across laboratories is important for advancing clinical genomics. The two CLIA-accredited Electronic Medical Record and Genomics Network sequencing centers and the six CLIA-accredited laboratories and one research laboratory performing genome or exome sequencing in the Clinical Sequencing Evidence-Generating Research Consortium collaborated to explore current sources of discordance in classification. Eight laboratories each submitted 20 classified variants in the ACMG secondary finding v.2.0 genes. After removing duplicates, each of the 158 variants was annotated and independently classified by two additional laboratories using the ACMG-AMP guidelines. Overall concordance across three laboratories was assessed and discordant variants were reviewed via teleconference and email. The submitted variant set included 28 P/LP variants, 96 VUS, and 34 LB/B variants, mostly in cancer (40%) and cardiac (27%) risk genes. Eighty-six (54%) variants reached complete five-category (i.e., P, LP, VUS, LB, B) concordance, and 17 (11%) had a discordance that could affect clinical recommendations (P/LP versus VUS/LB/B). 21% and 63% of variants submitted as P and LP, respectively, were discordant with VUS. Of the 54 originally discordant variants that underwent further review, 32 reached agreement, for a post-review concordance rate of 84% (118/140 variants). This project provides an updated estimate of variant concordance, identifies considerations for LP classified variants, and highlights ongoing sources of discordance. Continued and increased sharing of variant classifications and evidence across laboratories, and the ongoing work of ClinGen to provide general as well as gene- and disease-specific guidance, will lead to continued increases in concordance.
KW - ACMG-AMP recommendations
KW - genomic implementation
KW - germline variant classification
UR - http://www.scopus.com/inward/record.url?scp=85094949817&partnerID=8YFLogxK
U2 - 10.1016/j.ajhg.2020.09.011
DO - 10.1016/j.ajhg.2020.09.011
M3 - Article
C2 - 33108757
AN - SCOPUS:85094949817
SN - 0002-9297
VL - 107
SP - 932
EP - 941
JO - American journal of human genetics
JF - American journal of human genetics
IS - 5
ER -