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

Authors :
Flannick, J
Mercader, JM
Fuchsberger, C
Udler, MS
Mahajan, A
Wessel, J
Teslovich, TM
Caulkins, L
Koesterer, R
Barajas-Olmos, F
Blackwell, TW
Boerwinkle, E
Brody, JA
Centeno-Cruz, F
Chen, L
Chen, S
Contreras-Cubas, C
Córdova, E
Correa, A
Cortes, M
DeFronzo, RA
Dolan, L
Drews, KL
Elliott, A
Floyd, JS
Gabriel, S
Garay-Sevilla, ME
García-Ortiz, H
Gross, M
Han, S
Heard-Costa, NL
Jackson, AU
Jørgensen, ME
Kang, HM
Kelsey, M
Kim, B-J
Koistinen, HA
Kuusisto, J
Leader, JB
Linneberg, A
Liu, C-T
Liu, J
Lyssenko, V
Manning, AK
Marcketta, A
Malacara-Hernandez, JM
Martínez-Hernández, A
Matsuo, K
Mayer-Davis, E
Mendoza-Caamal, E
Mohlke, KL
Morrison, AC
Ndungu, A
Ng, MCY
O'Dushlaine, C
Payne, AJ
Pihoker, C
Broad Genomics Platform
Post, WS
Preuss, M
Psaty, BM
Vasan, RS
Rayner, NW
Reiner, AP
Revilla-Monsalve, C
Robertson, NR
Santoro, N
Schurmann, C
So, WY
Soberón, X
Stringham, HM
Strom, TM
Tam, CHT
Thameem, F
Tomlinson, B
Torres, JM
Tracy, RP
van Dam, RM
Vujkovic, M
Wang, S
Welch, RP
Witte, DR
Wong, T-Y
Atzmon, G
Barzilai, N
Blangero, J
Bonnycastle, LL
Bowden, DW
Chambers, JC
Chan, E
Cheng, C-Y
Cho, YS
Collins, FS
de Vries, PS
Duggirala, R
Glaser, B
Gonzalez, C
Gonzalez, ME
Groop, L
Kooner, JS
Kwak, SH
Laakso, M
Lehman, DM
Nilsson, P
Spector, TD
Tai, ES
Tuomi, T
Tuomilehto, J
Wilson, JG
Aguilar-Salinas, CA
Bottinger, E
Burke, B
Carey, DJ
Chan, JCN
Dupuis, J
Frossard, P
Heckbert, SR
Hwang, MY
Kim, YJ
Kirchner, HL
Lee, J-Y
Lee, J
Loos, RJF
Ma, RCW
Morris, AD
O'Donnell, CJ
Palmer, CNA
Pankow, J
Park, KS
Rasheed, A
Saleheen, D
Sim, X
Small, KS
Teo, YY
Haiman, C
Hanis, CL
Henderson, BE
Orozco, L
Tusié-Luna, T
Dewey, FE
Baras, A
Gieger, C
Meitinger, T
Strauch, K
Lange, L
Grarup, N
Hansen, T
Pedersen, O
Zeitler, P
Dabelea, D
Abecasis, G
Bell, GI
Cox, NJ
Seielstad, M
Sladek, R
Meigs, JB
Rich, SS
Rotter, JI
DiscovEHR Collaboration
CHARGE
LuCamp
ProDiGY
GoT2D
ESP
SIGMA-T2D
T2D-GENES
AMP-T2D-GENES
Altshuler, D
Burtt, NP
Scott, LJ
Morris, AP
Florez, JC
McCarthy, MI
Boehnke, M
Flannick, J
Mercader, JM
Fuchsberger, C
Udler, MS
Mahajan, A
Wessel, J
Teslovich, TM
Caulkins, L
Koesterer, R
Barajas-Olmos, F
Blackwell, TW
Boerwinkle, E
Brody, JA
Centeno-Cruz, F
Chen, L
Chen, S
Contreras-Cubas, C
Córdova, E
Correa, A
Cortes, M
DeFronzo, RA
Dolan, L
Drews, KL
Elliott, A
Floyd, JS
Gabriel, S
Garay-Sevilla, ME
García-Ortiz, H
Gross, M
Han, S
Heard-Costa, NL
Jackson, AU
Jørgensen, ME
Kang, HM
Kelsey, M
Kim, B-J
Koistinen, HA
Kuusisto, J
Leader, JB
Linneberg, A
Liu, C-T
Liu, J
Lyssenko, V
Manning, AK
Marcketta, A
Malacara-Hernandez, JM
Martínez-Hernández, A
Matsuo, K
Mayer-Davis, E
Mendoza-Caamal, E
Mohlke, KL
Morrison, AC
Ndungu, A
Ng, MCY
O'Dushlaine, C
Payne, AJ
Pihoker, C
Broad Genomics Platform
Post, WS
Preuss, M
Psaty, BM
Vasan, RS
Rayner, NW
Reiner, AP
Revilla-Monsalve, C
Robertson, NR
Santoro, N
Schurmann, C
So, WY
Soberón, X
Stringham, HM
Strom, TM
Tam, CHT
Thameem, F
Tomlinson, B
Torres, JM
Tracy, RP
van Dam, RM
Vujkovic, M
Wang, S
Welch, RP
Witte, DR
Wong, T-Y
Atzmon, G
Barzilai, N
Blangero, J
Bonnycastle, LL
Bowden, DW
Chambers, JC
Chan, E
Cheng, C-Y
Cho, YS
Collins, FS
de Vries, PS
Duggirala, R
Glaser, B
Gonzalez, C
Gonzalez, ME
Groop, L
Kooner, JS
Kwak, SH
Laakso, M
Lehman, DM
Nilsson, P
Spector, TD
Tai, ES
Tuomi, T
Tuomilehto, J
Wilson, JG
Aguilar-Salinas, CA
Bottinger, E
Burke, B
Carey, DJ
Chan, JCN
Dupuis, J
Frossard, P
Heckbert, SR
Hwang, MY
Kim, YJ
Kirchner, HL
Lee, J-Y
Lee, J
Loos, RJF
Ma, RCW
Morris, AD
O'Donnell, CJ
Palmer, CNA
Pankow, J
Park, KS
Rasheed, A
Saleheen, D
Sim, X
Small, KS
Teo, YY
Haiman, C
Hanis, CL
Henderson, BE
Orozco, L
Tusié-Luna, T
Dewey, FE
Baras, A
Gieger, C
Meitinger, T
Strauch, K
Lange, L
Grarup, N
Hansen, T
Pedersen, O
Zeitler, P
Dabelea, D
Abecasis, G
Bell, GI
Cox, NJ
Seielstad, M
Sladek, R
Meigs, JB
Rich, SS
Rotter, JI
DiscovEHR Collaboration
CHARGE
LuCamp
ProDiGY
GoT2D
ESP
SIGMA-T2D
T2D-GENES
AMP-T2D-GENES
Altshuler, D
Burtt, NP
Scott, LJ
Morris, AP
Florez, JC
McCarthy, MI
Boehnke, M
Publication Year :
2019

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.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1340013354
Document Type :
Electronic Resource

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