Resequencing candidate genes implicates rare variants in asthma susceptibility

Dara G. Torgerson; Daniel Capurso; Rasika A. Mathias; Penelope E. Graves; Ryan D. Hernandez; Terri H. Beaty; Eugene R. Bleecker; Benjamin A. Raby; Deborah A. Meyers; Kathleen C. Barnes; Scott T. Weiss; Fernando D. Martinez; Dan L. Nicolae; Carole Ober

doi:10.1016/j.ajhg.2012.01.008

Resequencing candidate genes implicates rare variants in asthma susceptibility

Dara G. Torgerson, Daniel Capurso, Rasika A. Mathias, Penelope E. Graves, Ryan D. Hernandez, Terri H. Beaty, Eugene R. Bleecker, Benjamin A. Raby, Deborah A. Meyers, Kathleen C. Barnes, Scott T. Weiss, Fernando D. Martinez, Dan L. Nicolae, Carole Ober

School of Medicine

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46 Scopus citations

Abstract

Common variation in over 100 genes has been implicated in the risk of developing asthma, but the contribution of rare variants to asthma susceptibility remains largely unexplored. We selected nine genes that showed the strongest signatures of weak purifying selection from among 53 candidate asthma-associated genes, and we sequenced the coding exons and flanking noncoding regions in 450 asthmatic cases and 515 nonasthmatic controls. We observed an overall excess of p values <0.05 (p = 0.02), and rare variants in four genes (AGT, DPP10, IKBKAP, and IL12RB1) contributed to asthma susceptibility among African Americans. Rare variants in IL12RB1 were also associated with asthma susceptibility among European Americans, despite the fact that the majority of rare variants in IL12RB1 were specific to either one of the populations. The combined evidence of association with rare noncoding variants in IL12RB1 remained significant (p = 3.7 × 10 ^-4) after correcting for multiple testing. Overall, the contribution of rare variants to asthma susceptibility was predominantly due to noncoding variants in sequences flanking the exons, although nonsynonymous rare variants in DPP10 and in IL12RB1 were associated with asthma in African Americans and European Americans, respectively. This study provides evidence that rare variants contribute to asthma susceptibility. Additional studies are required for testing whether prioritizing genes for resequencing on the basis of signatures of purifying selection is an efficient means of identifying novel rare variants that contribute to complex disease.

Original language	English (US)
Pages (from-to)	273-281
Number of pages	9
Journal	American journal of human genetics
Volume	90
Issue number	2
DOIs	https://doi.org/10.1016/j.ajhg.2012.01.008
State	Published - Feb 10 2012

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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10.1016/j.ajhg.2012.01.008

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Torgerson, D. G., Capurso, D., Mathias, R. A., Graves, P. E., Hernandez, R. D., Beaty, T. H., Bleecker, E. R., Raby, B. A., Meyers, D. A., Barnes, K. C., Weiss, S. T., Martinez, F. D., Nicolae, D. L., & Ober, C. (2012). Resequencing candidate genes implicates rare variants in asthma susceptibility. American journal of human genetics, 90(2), 273-281. https://doi.org/10.1016/j.ajhg.2012.01.008

@article{655090d9185346b79546b029de4627aa,

title = "Resequencing candidate genes implicates rare variants in asthma susceptibility",

abstract = "Common variation in over 100 genes has been implicated in the risk of developing asthma, but the contribution of rare variants to asthma susceptibility remains largely unexplored. We selected nine genes that showed the strongest signatures of weak purifying selection from among 53 candidate asthma-associated genes, and we sequenced the coding exons and flanking noncoding regions in 450 asthmatic cases and 515 nonasthmatic controls. We observed an overall excess of p values <0.05 (p = 0.02), and rare variants in four genes (AGT, DPP10, IKBKAP, and IL12RB1) contributed to asthma susceptibility among African Americans. Rare variants in IL12RB1 were also associated with asthma susceptibility among European Americans, despite the fact that the majority of rare variants in IL12RB1 were specific to either one of the populations. The combined evidence of association with rare noncoding variants in IL12RB1 remained significant (p = 3.7 × 10 -4) after correcting for multiple testing. Overall, the contribution of rare variants to asthma susceptibility was predominantly due to noncoding variants in sequences flanking the exons, although nonsynonymous rare variants in DPP10 and in IL12RB1 were associated with asthma in African Americans and European Americans, respectively. This study provides evidence that rare variants contribute to asthma susceptibility. Additional studies are required for testing whether prioritizing genes for resequencing on the basis of signatures of purifying selection is an efficient means of identifying novel rare variants that contribute to complex disease.",

author = "Torgerson, {Dara G.} and Daniel Capurso and Mathias, {Rasika A.} and Graves, {Penelope E.} and Hernandez, {Ryan D.} and Beaty, {Terri H.} and Bleecker, {Eugene R.} and Raby, {Benjamin A.} and Meyers, {Deborah A.} and Barnes, {Kathleen C.} and Weiss, {Scott T.} and Martinez, {Fernando D.} and Nicolae, {Dan L.} and Carole Ober",

note = "Funding Information: The authors gratefully acknowledge Dana Busam and Ewen Kirkness at the J. Craig Venter Institute (JCVI), the National Heart, Lung, and Blood Institute (NHLBI)-funded Resequencing and Genotyping Service at the JCVI, and all of the patients, investigators, coordinators, and research teams for the CAMP (Childhood Asthma Management Program) Genetic Ancillary Study, the Childhood Asthma Research and Education network, the Severe Asthma Research Program network, the Collaborative Studies on the Genetics of Asthma study, and the Genomic Research on Asthma in the African Diaspora study. These studies were supported by U01 HL49596 and R01 HL072414 to C.O.; RC2 HL101651 to C.O. and D.L.N.; R01 HL087665 to D.L.N.; U10 HL064307, U10 HL064288, U10 HL064295, U10 HL064287, U10 HL064305, and U10 HL064313 to F.D.M.; U01 HL075419, U01 HL65899, P01 HL083069, R01 HL086601, and RC2 HL101651 to S.T.W.; R01 HL69167 and HL101487 to D.A.M. and E.R.B.; and R01 HL087699, U01 HL49612, R01 AI50024, and R01 AI44840 to K.C.B. K.C.B. was supported in part by the Mary Beryl Patch Turnbull Scholar Program. Resequencing services were provided by the JCVI under U.S. Federal Government contract number N01-HV-48196 from the NHLBI. ",

year = "2012",

month = feb,

day = "10",

doi = "10.1016/j.ajhg.2012.01.008",

language = "English (US)",

volume = "90",

pages = "273--281",

journal = "American journal of human genetics",

issn = "0002-9297",

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TY - JOUR

T1 - Resequencing candidate genes implicates rare variants in asthma susceptibility

AU - Torgerson, Dara G.

AU - Capurso, Daniel

AU - Mathias, Rasika A.

AU - Graves, Penelope E.

AU - Hernandez, Ryan D.

AU - Beaty, Terri H.

AU - Bleecker, Eugene R.

AU - Raby, Benjamin A.

AU - Meyers, Deborah A.

AU - Barnes, Kathleen C.

AU - Weiss, Scott T.

AU - Martinez, Fernando D.

AU - Nicolae, Dan L.

AU - Ober, Carole

N1 - Funding Information: The authors gratefully acknowledge Dana Busam and Ewen Kirkness at the J. Craig Venter Institute (JCVI), the National Heart, Lung, and Blood Institute (NHLBI)-funded Resequencing and Genotyping Service at the JCVI, and all of the patients, investigators, coordinators, and research teams for the CAMP (Childhood Asthma Management Program) Genetic Ancillary Study, the Childhood Asthma Research and Education network, the Severe Asthma Research Program network, the Collaborative Studies on the Genetics of Asthma study, and the Genomic Research on Asthma in the African Diaspora study. These studies were supported by U01 HL49596 and R01 HL072414 to C.O.; RC2 HL101651 to C.O. and D.L.N.; R01 HL087665 to D.L.N.; U10 HL064307, U10 HL064288, U10 HL064295, U10 HL064287, U10 HL064305, and U10 HL064313 to F.D.M.; U01 HL075419, U01 HL65899, P01 HL083069, R01 HL086601, and RC2 HL101651 to S.T.W.; R01 HL69167 and HL101487 to D.A.M. and E.R.B.; and R01 HL087699, U01 HL49612, R01 AI50024, and R01 AI44840 to K.C.B. K.C.B. was supported in part by the Mary Beryl Patch Turnbull Scholar Program. Resequencing services were provided by the JCVI under U.S. Federal Government contract number N01-HV-48196 from the NHLBI.

PY - 2012/2/10

Y1 - 2012/2/10

N2 - Common variation in over 100 genes has been implicated in the risk of developing asthma, but the contribution of rare variants to asthma susceptibility remains largely unexplored. We selected nine genes that showed the strongest signatures of weak purifying selection from among 53 candidate asthma-associated genes, and we sequenced the coding exons and flanking noncoding regions in 450 asthmatic cases and 515 nonasthmatic controls. We observed an overall excess of p values <0.05 (p = 0.02), and rare variants in four genes (AGT, DPP10, IKBKAP, and IL12RB1) contributed to asthma susceptibility among African Americans. Rare variants in IL12RB1 were also associated with asthma susceptibility among European Americans, despite the fact that the majority of rare variants in IL12RB1 were specific to either one of the populations. The combined evidence of association with rare noncoding variants in IL12RB1 remained significant (p = 3.7 × 10 -4) after correcting for multiple testing. Overall, the contribution of rare variants to asthma susceptibility was predominantly due to noncoding variants in sequences flanking the exons, although nonsynonymous rare variants in DPP10 and in IL12RB1 were associated with asthma in African Americans and European Americans, respectively. This study provides evidence that rare variants contribute to asthma susceptibility. Additional studies are required for testing whether prioritizing genes for resequencing on the basis of signatures of purifying selection is an efficient means of identifying novel rare variants that contribute to complex disease.

AB - Common variation in over 100 genes has been implicated in the risk of developing asthma, but the contribution of rare variants to asthma susceptibility remains largely unexplored. We selected nine genes that showed the strongest signatures of weak purifying selection from among 53 candidate asthma-associated genes, and we sequenced the coding exons and flanking noncoding regions in 450 asthmatic cases and 515 nonasthmatic controls. We observed an overall excess of p values <0.05 (p = 0.02), and rare variants in four genes (AGT, DPP10, IKBKAP, and IL12RB1) contributed to asthma susceptibility among African Americans. Rare variants in IL12RB1 were also associated with asthma susceptibility among European Americans, despite the fact that the majority of rare variants in IL12RB1 were specific to either one of the populations. The combined evidence of association with rare noncoding variants in IL12RB1 remained significant (p = 3.7 × 10 -4) after correcting for multiple testing. Overall, the contribution of rare variants to asthma susceptibility was predominantly due to noncoding variants in sequences flanking the exons, although nonsynonymous rare variants in DPP10 and in IL12RB1 were associated with asthma in African Americans and European Americans, respectively. This study provides evidence that rare variants contribute to asthma susceptibility. Additional studies are required for testing whether prioritizing genes for resequencing on the basis of signatures of purifying selection is an efficient means of identifying novel rare variants that contribute to complex disease.

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SP - 273

EP - 281

JO - American journal of human genetics

JF - American journal of human genetics

IS - 2

ER -

Resequencing candidate genes implicates rare variants in asthma susceptibility

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