Exome sequencing of 20,791 cases of type 2 diabetes and 24,440 controls

Broad Genomics Platform; DiscovEHR Collaboration; CHARGE; LuCamp; ProDiGY; GoT2D; ESP; SIGMA-T2D; T2D-GENES; AMP-T2D-GENES

doi:10.1038/s41586-019-1231-2

Exome sequencing of 20,791 cases of type 2 diabetes and 24,440 controls

Broad Genomics Platform, DiscovEHR Collaboration, CHARGE, LuCamp, ProDiGY, GoT2D, ESP, SIGMA-T2D, T2D-GENES, AMP-T2D-GENES

Producción científica: Article › revisión exhaustiva

209 Citas (Scopus)

Resumen

Protein-coding genetic variants that strongly affect disease risk can yield relevant clues to disease pathogenesis. Here we report exome-sequencing analyses of 20,791 individuals with type 2 diabetes (T2D) and 24,440 non-diabetic control participants from 5 ancestries. We identify gene-level associations of rare variants (with minor allele frequencies of less than 0.5%) in 4 genes at exome-wide significance, including a series of more than 30 SLC30A8 alleles that conveys protection against T2D, and in 12 gene sets, including those corresponding to T2D drug targets (P = 6.1 × 10⁻³) and candidate genes from knockout mice (P = 5.2 × 10⁻³). Within our study, the strongest T2D gene-level signals for rare variants explain at most 25% of the heritability of the strongest common single-variant signals, and the gene-level effect sizes of the rare variants that we observed in established T2D drug targets will require 75,000–185,000 sequenced cases to achieve exome-wide significance. We propose a method to interpret these modest rare-variant associations and to incorporate these associations into future target or gene prioritization efforts.

Idioma original	English (US)
Páginas (desde-hasta)	71-76
Número de páginas	6
Publicación	Nature
Volumen	570
N.º	7759
DOI	https://doi.org/10.1038/s41586-019-1231-2
Estado	Published - jun 6 2019

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10.1038/s41586-019-1231-2

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@article{a4a9e01c512041ab98ae09f8e767c850,

title = "Exome sequencing of 20,791 cases of type 2 diabetes and 24,440 controls",

abstract = "Protein-coding genetic variants that strongly affect disease risk can yield relevant clues to disease pathogenesis. Here we report exome-sequencing analyses of 20,791 individuals with type 2 diabetes (T2D) and 24,440 non-diabetic control participants from 5 ancestries. We identify gene-level associations of rare variants (with minor allele frequencies of less than 0.5%) in 4 genes at exome-wide significance, including a series of more than 30 SLC30A8 alleles that conveys protection against T2D, and in 12 gene sets, including those corresponding to T2D drug targets (P = 6.1 × 10−3) and candidate genes from knockout mice (P = 5.2 × 10−3). Within our study, the strongest T2D gene-level signals for rare variants explain at most 25% of the heritability of the strongest common single-variant signals, and the gene-level effect sizes of the rare variants that we observed in established T2D drug targets will require 75,000–185,000 sequenced cases to achieve exome-wide significance. We propose a method to interpret these modest rare-variant associations and to incorporate these associations into future target or gene prioritization efforts.",

author = "{Broad Genomics Platform} and {DiscovEHR Collaboration} and CHARGE and LuCamp and ProDiGY and GoT2D and ESP and SIGMA-T2D and T2D-GENES and AMP-T2D-GENES and Jason Flannick and Mercader, {Josep M.} and Christian Fuchsberger and Udler, {Miriam S.} and Anubha Mahajan and Jennifer Wessel and Teslovich, {Tanya M.} and Lizz Caulkins and Ryan Koesterer and Francisco Barajas-Olmos and Blackwell, {Thomas W.} and Eric Boerwinkle and Brody, {Jennifer A.} and Federico Centeno-Cruz and Ling Chen and Siying Chen and Cecilia Contreras-Cubas and Emilio C{\'o}rdova and Adolfo Correa and Maria Cortes and DeFronzo, {Ralph A.} and Lawrence Dolan and Drews, {Kimberly L.} and Amanda Elliott and Floyd, {James S.} and Stacey Gabriel and Garay-Sevilla, {Maria Eugenia} and Humberto Garc{\'i}a-Ortiz and Myron Gross and Sohee Han and Heard-Costa, {Nancy L.} and Jackson, {Anne U.} and J{\o}rgensen, {Marit E.} and Kang, {Hyun Min} and Megan Kelsey and Kim, {Bong Jo} and Koistinen, {Heikki A.} and Johanna Kuusisto and Leader, {Joseph B.} and Allan Linneberg and Liu, {Ching Ti} and Jianjun Liu and Valeriya Lyssenko and Manning, {Alisa K.} and Anthony Marcketta and Vasan, {Ramachandran S.} and Farook Thameem and John Blangero and Ravindranath Duggirala and Lehman, {Donna M.}",

note = "Publisher Copyright: {\textcopyright} 2019, The Author(s), under exclusive licence to Springer Nature Limited.",

year = "2019",

month = jun,

day = "6",

doi = "10.1038/s41586-019-1231-2",

language = "English (US)",

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pages = "71--76",

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TY - JOUR

T1 - Exome sequencing of 20,791 cases of type 2 diabetes and 24,440 controls

AU - Broad Genomics Platform

AU - DiscovEHR Collaboration

AU - CHARGE

AU - LuCamp

AU - ProDiGY

AU - GoT2D

AU - ESP

AU - SIGMA-T2D

AU - T2D-GENES

AU - AMP-T2D-GENES

AU - Flannick, Jason

AU - Mercader, Josep M.

AU - Fuchsberger, Christian

AU - Udler, Miriam S.

AU - Mahajan, Anubha

AU - Wessel, Jennifer

AU - Teslovich, Tanya M.

AU - Caulkins, Lizz

AU - Koesterer, Ryan

AU - Barajas-Olmos, Francisco

AU - Blackwell, Thomas W.

AU - Boerwinkle, Eric

AU - Brody, Jennifer A.

AU - Centeno-Cruz, Federico

AU - Chen, Ling

AU - Chen, Siying

AU - Contreras-Cubas, Cecilia

AU - Córdova, Emilio

AU - Correa, Adolfo

AU - Cortes, Maria

AU - DeFronzo, Ralph A.

AU - Dolan, Lawrence

AU - Drews, Kimberly L.

AU - Elliott, Amanda

AU - Floyd, James S.

AU - Gabriel, Stacey

AU - Garay-Sevilla, Maria Eugenia

AU - García-Ortiz, Humberto

AU - Gross, Myron

AU - Han, Sohee

AU - Heard-Costa, Nancy L.

AU - Jackson, Anne U.

AU - Jørgensen, Marit E.

AU - Kang, Hyun Min

AU - Kelsey, Megan

AU - Kim, Bong Jo

AU - Koistinen, Heikki A.

AU - Kuusisto, Johanna

AU - Leader, Joseph B.

AU - Linneberg, Allan

AU - Liu, Ching Ti

AU - Liu, Jianjun

AU - Lyssenko, Valeriya

AU - Manning, Alisa K.

AU - Marcketta, Anthony

AU - Vasan, Ramachandran S.

AU - Thameem, Farook

AU - Blangero, John

AU - Duggirala, Ravindranath

AU - Lehman, Donna M.

PY - 2019/6/6

Y1 - 2019/6/6

N2 - Protein-coding genetic variants that strongly affect disease risk can yield relevant clues to disease pathogenesis. Here we report exome-sequencing analyses of 20,791 individuals with type 2 diabetes (T2D) and 24,440 non-diabetic control participants from 5 ancestries. We identify gene-level associations of rare variants (with minor allele frequencies of less than 0.5%) in 4 genes at exome-wide significance, including a series of more than 30 SLC30A8 alleles that conveys protection against T2D, and in 12 gene sets, including those corresponding to T2D drug targets (P = 6.1 × 10−3) and candidate genes from knockout mice (P = 5.2 × 10−3). Within our study, the strongest T2D gene-level signals for rare variants explain at most 25% of the heritability of the strongest common single-variant signals, and the gene-level effect sizes of the rare variants that we observed in established T2D drug targets will require 75,000–185,000 sequenced cases to achieve exome-wide significance. We propose a method to interpret these modest rare-variant associations and to incorporate these associations into future target or gene prioritization efforts.

AB - Protein-coding genetic variants that strongly affect disease risk can yield relevant clues to disease pathogenesis. Here we report exome-sequencing analyses of 20,791 individuals with type 2 diabetes (T2D) and 24,440 non-diabetic control participants from 5 ancestries. We identify gene-level associations of rare variants (with minor allele frequencies of less than 0.5%) in 4 genes at exome-wide significance, including a series of more than 30 SLC30A8 alleles that conveys protection against T2D, and in 12 gene sets, including those corresponding to T2D drug targets (P = 6.1 × 10−3) and candidate genes from knockout mice (P = 5.2 × 10−3). Within our study, the strongest T2D gene-level signals for rare variants explain at most 25% of the heritability of the strongest common single-variant signals, and the gene-level effect sizes of the rare variants that we observed in established T2D drug targets will require 75,000–185,000 sequenced cases to achieve exome-wide significance. We propose a method to interpret these modest rare-variant associations and to incorporate these associations into future target or gene prioritization efforts.

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U2 - 10.1038/s41586-019-1231-2

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C2 - 31118516

AN - SCOPUS:85066251977

SN - 0028-0836

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JO - Nature

JF - Nature

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