Refining the role of de novo protein-truncating variants in neurodevelopmental disorders by using population reference samples

Jack A. Kosmicki; Kaitlin E. Samocha; Daniel P. Howrigan; Stephan J. Sanders; Kamil Slowikowski; Monkol Lek; Konrad J. Karczewski; David J. Cutler; Bernie Devlin; Kathryn Roeder; Joseph D. Buxbaum; Benjamin M. Neale; Daniel G. Macarthur; Dennis P. Wall; Elise B. Robinson; Mark J. Daly

doi:10.1038/ng.3789

Refining the role of de novo protein-truncating variants in neurodevelopmental disorders by using population reference samples

Jack A. Kosmicki, Kaitlin E. Samocha, Daniel P. Howrigan, Stephan J. Sanders, Kamil Slowikowski, Monkol Lek, Konrad J. Karczewski, David J. Cutler, Bernie Devlin, Kathryn Roeder, Joseph D. Buxbaum, Benjamin M. Neale, Daniel G. Macarthur, Dennis P. Wall, Elise B. Robinson, Mark J. Daly

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Abstract

Recent research has uncovered an important role for de novo variation in neurodevelopmental disorders. Using aggregated data from 9,246 families with autism spectrum disorder, intellectual disability, or developmental delay, we found that ∼41/3 of de novo variants are independently present as standing variation in the Exome Aggregation Consortium's cohort of 60,706 adults, and these de novo variants do not contribute to neurodevelopmental risk. We further used a loss-of-function (LoF)-intolerance metric, pLI, to identify a subset of LoF-intolerant genes containing the observed signal of associated de novo protein-truncating variants (PTVs) in neurodevelopmental disorders. LoF-intolerant genes also carry a modest excess of inherited PTVs, although the strongest de novo-affected genes contribute little to this excess, thus suggesting that the excess of inherited risk resides in lower-penetrant genes. These findings illustrate the importance of population-based reference cohorts for the interpretation of candidate pathogenic variants, even for analyses of complex diseases and de novo variation.

Original language	English
Pages (from-to)	504-510
Number of pages	7
Journal	Nature Genetics
Volume	49
Issue number	4
DOIs	https://doi.org/10.1038/ng.3789
State	Published - 30 Mar 2017

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Kosmicki, J. A., Samocha, K. E., Howrigan, D. P., Sanders, S. J., Slowikowski, K., Lek, M., Karczewski, K. J., Cutler, D. J., Devlin, B., Roeder, K., Buxbaum, J. D., Neale, B. M., Macarthur, D. G., Wall, D. P., Robinson, E. B., & Daly, M. J. (2017). Refining the role of de novo protein-truncating variants in neurodevelopmental disorders by using population reference samples. Nature Genetics, 49(4), 504-510. https://doi.org/10.1038/ng.3789

@article{11c71fb6d32a44188e9d79612c19ac9d,

title = "Refining the role of de novo protein-truncating variants in neurodevelopmental disorders by using population reference samples",

abstract = "Recent research has uncovered an important role for de novo variation in neurodevelopmental disorders. Using aggregated data from 9,246 families with autism spectrum disorder, intellectual disability, or developmental delay, we found that ∼41/3 of de novo variants are independently present as standing variation in the Exome Aggregation Consortium's cohort of 60,706 adults, and these de novo variants do not contribute to neurodevelopmental risk. We further used a loss-of-function (LoF)-intolerance metric, pLI, to identify a subset of LoF-intolerant genes containing the observed signal of associated de novo protein-truncating variants (PTVs) in neurodevelopmental disorders. LoF-intolerant genes also carry a modest excess of inherited PTVs, although the strongest de novo-affected genes contribute little to this excess, thus suggesting that the excess of inherited risk resides in lower-penetrant genes. These findings illustrate the importance of population-based reference cohorts for the interpretation of candidate pathogenic variants, even for analyses of complex diseases and de novo variation.",

author = "Kosmicki, \{Jack A.\} and Samocha, \{Kaitlin E.\} and Howrigan, \{Daniel P.\} and Sanders, \{Stephan J.\} and Kamil Slowikowski and Monkol Lek and Karczewski, \{Konrad J.\} and Cutler, \{David J.\} and Bernie Devlin and Kathryn Roeder and Buxbaum, \{Joseph D.\} and Neale, \{Benjamin M.\} and Macarthur, \{Daniel G.\} and Wall, \{Dennis P.\} and Robinson, \{Elise B.\} and Daly, \{Mark J.\}",

note = "Funding Information: This work was supported by NIH grants U01MH100233, U01MH100209, U01MH100229, and U01MH100239 to the Autism Sequencing Consortium (ASC), and R56 MH097849 and R01 MH097849 to the Population-based Autism Genetics and Environment Study (PAGES).",

year = "2017",

month = mar,

day = "30",

doi = "10.1038/ng.3789",

language = "English",

volume = "49",

pages = "504--510",

journal = "Nature Genetics",

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number = "4",

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Kosmicki, JA, Samocha, KE, Howrigan, DP, Sanders, SJ, Slowikowski, K, Lek, M, Karczewski, KJ, Cutler, DJ, Devlin, B, Roeder, K, Buxbaum, JD, Neale, BM, Macarthur, DG, Wall, DP, Robinson, EB & Daly, MJ 2017, 'Refining the role of de novo protein-truncating variants in neurodevelopmental disorders by using population reference samples', Nature Genetics, vol. 49, no. 4, pp. 504-510. https://doi.org/10.1038/ng.3789

TY - JOUR

T1 - Refining the role of de novo protein-truncating variants in neurodevelopmental disorders by using population reference samples

AU - Kosmicki, Jack A.

AU - Samocha, Kaitlin E.

AU - Howrigan, Daniel P.

AU - Sanders, Stephan J.

AU - Slowikowski, Kamil

AU - Lek, Monkol

AU - Karczewski, Konrad J.

AU - Cutler, David J.

AU - Devlin, Bernie

AU - Roeder, Kathryn

AU - Buxbaum, Joseph D.

AU - Neale, Benjamin M.

AU - Macarthur, Daniel G.

AU - Wall, Dennis P.

AU - Robinson, Elise B.

AU - Daly, Mark J.

N1 - Funding Information: This work was supported by NIH grants U01MH100233, U01MH100209, U01MH100229, and U01MH100239 to the Autism Sequencing Consortium (ASC), and R56 MH097849 and R01 MH097849 to the Population-based Autism Genetics and Environment Study (PAGES).

PY - 2017/3/30

Y1 - 2017/3/30

N2 - Recent research has uncovered an important role for de novo variation in neurodevelopmental disorders. Using aggregated data from 9,246 families with autism spectrum disorder, intellectual disability, or developmental delay, we found that ∼41/3 of de novo variants are independently present as standing variation in the Exome Aggregation Consortium's cohort of 60,706 adults, and these de novo variants do not contribute to neurodevelopmental risk. We further used a loss-of-function (LoF)-intolerance metric, pLI, to identify a subset of LoF-intolerant genes containing the observed signal of associated de novo protein-truncating variants (PTVs) in neurodevelopmental disorders. LoF-intolerant genes also carry a modest excess of inherited PTVs, although the strongest de novo-affected genes contribute little to this excess, thus suggesting that the excess of inherited risk resides in lower-penetrant genes. These findings illustrate the importance of population-based reference cohorts for the interpretation of candidate pathogenic variants, even for analyses of complex diseases and de novo variation.

AB - Recent research has uncovered an important role for de novo variation in neurodevelopmental disorders. Using aggregated data from 9,246 families with autism spectrum disorder, intellectual disability, or developmental delay, we found that ∼41/3 of de novo variants are independently present as standing variation in the Exome Aggregation Consortium's cohort of 60,706 adults, and these de novo variants do not contribute to neurodevelopmental risk. We further used a loss-of-function (LoF)-intolerance metric, pLI, to identify a subset of LoF-intolerant genes containing the observed signal of associated de novo protein-truncating variants (PTVs) in neurodevelopmental disorders. LoF-intolerant genes also carry a modest excess of inherited PTVs, although the strongest de novo-affected genes contribute little to this excess, thus suggesting that the excess of inherited risk resides in lower-penetrant genes. These findings illustrate the importance of population-based reference cohorts for the interpretation of candidate pathogenic variants, even for analyses of complex diseases and de novo variation.

UR - https://www.scopus.com/pages/publications/85012277777

U2 - 10.1038/ng.3789

DO - 10.1038/ng.3789

M3 - Article

C2 - 28191890

AN - SCOPUS:85012277777

SN - 1061-4036

VL - 49

SP - 504

EP - 510

JO - Nature Genetics

JF - Nature Genetics

IS - 4

ER -

Refining the role of de novo protein-truncating variants in neurodevelopmental disorders by using population reference samples

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