Dutch genome diagnostic laboratories accelerated and improved variant interpretation and increased accuracy by sharing data

Ivo F. A. C. Fokkema; Kasper J. van der Velde; Mariska K. Slofstra; Claudia A. L. Ruivenkamp; Maartje J. Vogel; Rolph Pfundt; Marinus J. Blok; Ronald H. Lekanne Deprez; Quinten Waisfisz; Kristin M. Abbott; Richard J. Sinke; Rubayte Rahman; Isaac J. Nijman; Bart de Koning; Gert Thijs; Nienke Wieskamp; Ruben J. G. Moritz; Bart Charbon; Jasper J. Saris; Johan T. den Dunnen; Jeroen F. J. Laros; Morris A. Swertz; Marielle E. van Gijn

doi:10.1002/humu.23896

Dutch genome diagnostic laboratories accelerated and improved variant interpretation and increased accuracy by sharing data

Ivo F. A. C. Fokkema, Kasper J. van der Velde, Mariska K. Slofstra, Claudia A. L. Ruivenkamp, Maartje J. Vogel, Rolph Pfundt, Marinus J. Blok, Ronald H. Lekanne Deprez, Quinten Waisfisz, Kristin M. Abbott, Richard J. Sinke, Rubayte Rahman, Isaac J. Nijman, Bart de Koning, Gert Thijs, Nienke Wieskamp, Ruben J. G. Moritz, Bart Charbon, Jasper J. Saris, Johan T. den DunnenJeroen F. J. Laros, Morris A. Swertz, Marielle E. van Gijn^*

^*Corresponding author for this work

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

Abstract

Each year diagnostic laboratories in the Netherlands profile thousands of individuals for heritable disease using next-generation sequencing (NGS). This requires pathogenicity classification of millions of DNA variants on the standard 5-tier scale. To reduce time spent on data interpretation and increase data quality and reliability, the nine Dutch labs decided to publicly share their classifications. Variant classifications of nearly 100,000 unique variants were catalogued and compared in a centralized MOLGENIS database. Variants classified by more than one center were labeled as "consensus" when classifications agreed, and shared internationally with LOVD and ClinVar. When classifications opposed (LB/B vs. LP/P), they were labeled "conflicting", while other nonconsensus observations were labeled "no consensus". We assessed our classifications using the InterVar software to compare to ACMG 2015 guidelines, showing 99.7% overall consistency with only 0.3% discrepancies. Differences in classifications between Dutch labs or between Dutch labs and ACMG were mainly present in genes with low penetrance or for late onset disorders and highlight limitations of the current 5-tier classification system. The data sharing boosted the quality of DNA diagnostics in Dutch labs, an initiative we hope will be followed internationally. Recently, a positive match with a case from outside our consortium resulted in a more definite disease diagnosis.

Original language	English
Pages (from-to)	2230-2238
Number of pages	9
Journal	Human Mutation
Volume	40
Issue number	12
DOIs	https://doi.org/10.1002/humu.23896
Publication status	Published - Dec 2019

Keywords

data sharing
database
diagnostics
NGS
whole-exome sequencing
SEQUENCE VARIANTS
RECOMMENDATIONS
CARDIOMYOPATHIES
CLASSIFICATION

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Fokkema, I. F. A. C., van der Velde, K. J., Slofstra, M. K., Ruivenkamp, C. A. L., Vogel, M. J., Pfundt, R., Blok, M. J., Deprez, R. H. L., Waisfisz, Q., Abbott, K. M., Sinke, R. J., Rahman, R., Nijman, I. J., de Koning, B., Thijs, G., Wieskamp, N., Moritz, R. J. G., Charbon, B., Saris, J. J., ... van Gijn, M. E. (2019). Dutch genome diagnostic laboratories accelerated and improved variant interpretation and increased accuracy by sharing data. Human Mutation, 40(12), 2230-2238. https://doi.org/10.1002/humu.23896

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title = "Dutch genome diagnostic laboratories accelerated and improved variant interpretation and increased accuracy by sharing data",

abstract = "Each year diagnostic laboratories in the Netherlands profile thousands of individuals for heritable disease using next-generation sequencing (NGS). This requires pathogenicity classification of millions of DNA variants on the standard 5-tier scale. To reduce time spent on data interpretation and increase data quality and reliability, the nine Dutch labs decided to publicly share their classifications. Variant classifications of nearly 100,000 unique variants were catalogued and compared in a centralized MOLGENIS database. Variants classified by more than one center were labeled as {"}consensus{"} when classifications agreed, and shared internationally with LOVD and ClinVar. When classifications opposed (LB/B vs. LP/P), they were labeled {"}conflicting{"}, while other nonconsensus observations were labeled {"}no consensus{"}. We assessed our classifications using the InterVar software to compare to ACMG 2015 guidelines, showing 99.7% overall consistency with only 0.3% discrepancies. Differences in classifications between Dutch labs or between Dutch labs and ACMG were mainly present in genes with low penetrance or for late onset disorders and highlight limitations of the current 5-tier classification system. The data sharing boosted the quality of DNA diagnostics in Dutch labs, an initiative we hope will be followed internationally. Recently, a positive match with a case from outside our consortium resulted in a more definite disease diagnosis.",

keywords = "data sharing, database, diagnostics, NGS, whole-exome sequencing, SEQUENCE VARIANTS, RECOMMENDATIONS, CARDIOMYOPATHIES, CLASSIFICATION",

author = "Fokkema, {Ivo F. A. C.} and {van der Velde}, {Kasper J.} and Slofstra, {Mariska K.} and Ruivenkamp, {Claudia A. L.} and Vogel, {Maartje J.} and Rolph Pfundt and Blok, {Marinus J.} and Deprez, {Ronald H. Lekanne} and Quinten Waisfisz and Abbott, {Kristin M.} and Sinke, {Richard J.} and Rubayte Rahman and Nijman, {Isaac J.} and {de Koning}, Bart and Gert Thijs and Nienke Wieskamp and Moritz, {Ruben J. G.} and Bart Charbon and Saris, {Jasper J.} and {den Dunnen}, {Johan T.} and Laros, {Jeroen F. J.} and Swertz, {Morris A.} and {van Gijn}, {Marielle E.}",

note = "Funding Information: We thank ZonMW GGG project “WGS-first: {\textquoteleft}One-test-fits-all{\textquoteright} to diagnose rare genetic disorders” (nr. 846002003), NWO VIDI Grant number 917.164.455, and BBMRI-NL for their voucher. BBMRI-NL is a research infrastructure financed by the Netherlands Organization for Scientific Research (NWO), Grant number 184.033.111. Funding Information: We thank ZonMW GGG project “WGS‐first: {\textquoteleft}One‐test‐fits‐all{\textquoteright} to diagnose rare genetic disorders” (nr. 846002003), NWO VIDI Grant number 917.164.455, and BBMRI‐NL for their voucher. BBMRI‐NL is a research infrastructure financed by the Netherlands Organization for Scientific Research (NWO), Grant number 184.033.111. Publisher Copyright: {\textcopyright} 2019 The Authors. Human Mutation Published by Wiley Periodicals, Inc.",

year = "2019",

month = dec,

doi = "10.1002/humu.23896",

language = "English",

volume = "40",

pages = "2230--2238",

journal = "Human Mutation",

issn = "1059-7794",

publisher = "Wiley",

number = "12",

}

Fokkema, IFAC, van der Velde, KJ, Slofstra, MK, Ruivenkamp, CAL, Vogel, MJ, Pfundt, R, Blok, MJ, Deprez, RHL, Waisfisz, Q, Abbott, KM, Sinke, RJ, Rahman, R, Nijman, IJ, de Koning, B, Thijs, G, Wieskamp, N, Moritz, RJG, Charbon, B, Saris, JJ, den Dunnen, JT, Laros, JFJ, Swertz, MA & van Gijn, ME 2019, 'Dutch genome diagnostic laboratories accelerated and improved variant interpretation and increased accuracy by sharing data', Human Mutation, vol. 40, no. 12, pp. 2230-2238. https://doi.org/10.1002/humu.23896

TY - JOUR

T1 - Dutch genome diagnostic laboratories accelerated and improved variant interpretation and increased accuracy by sharing data

AU - Fokkema, Ivo F. A. C.

AU - van der Velde, Kasper J.

AU - Slofstra, Mariska K.

AU - Ruivenkamp, Claudia A. L.

AU - Vogel, Maartje J.

AU - Pfundt, Rolph

AU - Blok, Marinus J.

AU - Deprez, Ronald H. Lekanne

AU - Waisfisz, Quinten

AU - Abbott, Kristin M.

AU - Sinke, Richard J.

AU - Rahman, Rubayte

AU - Nijman, Isaac J.

AU - de Koning, Bart

AU - Thijs, Gert

AU - Wieskamp, Nienke

AU - Moritz, Ruben J. G.

AU - Charbon, Bart

AU - Saris, Jasper J.

AU - den Dunnen, Johan T.

AU - Laros, Jeroen F. J.

AU - Swertz, Morris A.

AU - van Gijn, Marielle E.

N1 - Funding Information: We thank ZonMW GGG project “WGS-first: ‘One-test-fits-all’ to diagnose rare genetic disorders” (nr. 846002003), NWO VIDI Grant number 917.164.455, and BBMRI-NL for their voucher. BBMRI-NL is a research infrastructure financed by the Netherlands Organization for Scientific Research (NWO), Grant number 184.033.111. Funding Information: We thank ZonMW GGG project “WGS‐first: ‘One‐test‐fits‐all’ to diagnose rare genetic disorders” (nr. 846002003), NWO VIDI Grant number 917.164.455, and BBMRI‐NL for their voucher. BBMRI‐NL is a research infrastructure financed by the Netherlands Organization for Scientific Research (NWO), Grant number 184.033.111. Publisher Copyright: © 2019 The Authors. Human Mutation Published by Wiley Periodicals, Inc.

PY - 2019/12

Y1 - 2019/12

N2 - Each year diagnostic laboratories in the Netherlands profile thousands of individuals for heritable disease using next-generation sequencing (NGS). This requires pathogenicity classification of millions of DNA variants on the standard 5-tier scale. To reduce time spent on data interpretation and increase data quality and reliability, the nine Dutch labs decided to publicly share their classifications. Variant classifications of nearly 100,000 unique variants were catalogued and compared in a centralized MOLGENIS database. Variants classified by more than one center were labeled as "consensus" when classifications agreed, and shared internationally with LOVD and ClinVar. When classifications opposed (LB/B vs. LP/P), they were labeled "conflicting", while other nonconsensus observations were labeled "no consensus". We assessed our classifications using the InterVar software to compare to ACMG 2015 guidelines, showing 99.7% overall consistency with only 0.3% discrepancies. Differences in classifications between Dutch labs or between Dutch labs and ACMG were mainly present in genes with low penetrance or for late onset disorders and highlight limitations of the current 5-tier classification system. The data sharing boosted the quality of DNA diagnostics in Dutch labs, an initiative we hope will be followed internationally. Recently, a positive match with a case from outside our consortium resulted in a more definite disease diagnosis.

AB - Each year diagnostic laboratories in the Netherlands profile thousands of individuals for heritable disease using next-generation sequencing (NGS). This requires pathogenicity classification of millions of DNA variants on the standard 5-tier scale. To reduce time spent on data interpretation and increase data quality and reliability, the nine Dutch labs decided to publicly share their classifications. Variant classifications of nearly 100,000 unique variants were catalogued and compared in a centralized MOLGENIS database. Variants classified by more than one center were labeled as "consensus" when classifications agreed, and shared internationally with LOVD and ClinVar. When classifications opposed (LB/B vs. LP/P), they were labeled "conflicting", while other nonconsensus observations were labeled "no consensus". We assessed our classifications using the InterVar software to compare to ACMG 2015 guidelines, showing 99.7% overall consistency with only 0.3% discrepancies. Differences in classifications between Dutch labs or between Dutch labs and ACMG were mainly present in genes with low penetrance or for late onset disorders and highlight limitations of the current 5-tier classification system. The data sharing boosted the quality of DNA diagnostics in Dutch labs, an initiative we hope will be followed internationally. Recently, a positive match with a case from outside our consortium resulted in a more definite disease diagnosis.

KW - data sharing

KW - database

KW - diagnostics

KW - NGS

KW - whole-exome sequencing

KW - SEQUENCE VARIANTS

KW - RECOMMENDATIONS

KW - CARDIOMYOPATHIES

KW - CLASSIFICATION

U2 - 10.1002/humu.23896

DO - 10.1002/humu.23896

M3 - Article

C2 - 31433103

SN - 1059-7794

VL - 40

SP - 2230

EP - 2238

JO - Human Mutation

JF - Human Mutation

IS - 12

ER -