Whole Exome sequencing of distant relatives in multiplex families implicates rare variants in candidate genes for oral clefts

Alexandre Bureau; Margaret M. Parker; Ingo Ruczinski; Margaret A. Taub; Mary L. Marazita; Jeffrey C. Murray; Elisabeth Mangold; Markus M. Noethen; Kirsten U. Ludwig; Jacqueline B. Hetmanski; Joan E. Bailey-Wilson; Cheryl D. Cropp; Qing Li; Silke Szymczak; Hasan Albacha-Hejazi; Khalid Alqosayer; L. Leigh Field; Yah Huei Wu-Chou; Kimberly F. Doheny; Hua Ling; Alan F. Scott; Terri H. Beaty

doi:10.1534/genetics.114.165225

Whole Exome sequencing of distant relatives in multiplex families implicates rare variants in candidate genes for oral clefts

Alexandre Bureau, Margaret M. Parker, Ingo Ruczinski, Margaret A. Taub, Mary L. Marazita, Jeffrey C. Murray, Elisabeth Mangold, Markus M. Noethen, Kirsten U. Ludwig, Jacqueline B. Hetmanski, Joan E. Bailey-Wilson, Cheryl D. Cropp, Qing Li, Silke Szymczak, Hasan Albacha-Hejazi, Khalid Alqosayer, L. Leigh Field, Yah Huei Wu-Chou, Kimberly F. Doheny, Hua LingAlan F. Scott, Terri H. Beaty

研究成果: 期刊稿件 › 文章 › 同行評審

72 引文斯高帕斯（Scopus）

摘要

A dozen genes/regions have been confirmed as genetic risk factors for oral clefts in human association and linkage studies, and animal models argue even more genes may be involved. Genomic sequencing studies should identify specific causal variants and may reveal additional genes as influencing risk to oral clefts, which have a complex and heterogeneous etiology. We conducted a whole exome sequencing (WES) study to search for potentially causal variants using affected relatives drawn from multiplex cleft families. Two or three affected second, third, and higher degree relatives from 55 multiplex families were sequenced. We examined rare single nucleotide variants (SNVs) shared by affected relatives in 348 recognized candidate genes. Exact probabilities that affected relatives would share these rare variants were calculated, given pedigree structures, and corrected for the number of variants tested. Five novel and potentially damaging SNVs shared by affected distant relatives were found and confirmed by Sanger sequencing. One damaging SNV in CDH1, shared by three affected second cousins from a single family, attained statistical significance (P = 0.02 after correcting for multiple tests). Family-based designs such as the one used in this WES study offer important advantages for identifying genes likely to be causing complex and heterogeneous disorders.

原文	英語
頁（從 - 到）	1039-1044
頁數	6
期刊	Genetics
卷	197
發行號	3
DOIs	https://doi.org/10.1534/genetics.114.165225
出版狀態	已出版 - 07 2014
對外發佈	是

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Bureau, A., Parker, M. M., Ruczinski, I., Taub, M. A., Marazita, M. L., Murray, J. C., Mangold, E., Noethen, M. M., Ludwig, K. U., Hetmanski, J. B., Bailey-Wilson, J. E., Cropp, C. D., Li, Q., Szymczak, S., Albacha-Hejazi, H., Alqosayer, K., Leigh Field, L., Wu-Chou, Y. H., Doheny, K. F., ... Beaty, T. H. (2014). Whole Exome sequencing of distant relatives in multiplex families implicates rare variants in candidate genes for oral clefts. Genetics, 197(3), 1039-1044. https://doi.org/10.1534/genetics.114.165225

@article{09a1df96b4504c92a535cc992ff6ef41,

title = "Whole Exome sequencing of distant relatives in multiplex families implicates rare variants in candidate genes for oral clefts",

abstract = "A dozen genes/regions have been confirmed as genetic risk factors for oral clefts in human association and linkage studies, and animal models argue even more genes may be involved. Genomic sequencing studies should identify specific causal variants and may reveal additional genes as influencing risk to oral clefts, which have a complex and heterogeneous etiology. We conducted a whole exome sequencing (WES) study to search for potentially causal variants using affected relatives drawn from multiplex cleft families. Two or three affected second, third, and higher degree relatives from 55 multiplex families were sequenced. We examined rare single nucleotide variants (SNVs) shared by affected relatives in 348 recognized candidate genes. Exact probabilities that affected relatives would share these rare variants were calculated, given pedigree structures, and corrected for the number of variants tested. Five novel and potentially damaging SNVs shared by affected distant relatives were found and confirmed by Sanger sequencing. One damaging SNV in CDH1, shared by three affected second cousins from a single family, attained statistical significance (P = 0.02 after correcting for multiple tests). Family-based designs such as the one used in this WES study offer important advantages for identifying genes likely to be causing complex and heterogeneous disorders.",

author = "Alexandre Bureau and Parker, {Margaret M.} and Ingo Ruczinski and Taub, {Margaret A.} and Marazita, {Mary L.} and Murray, {Jeffrey C.} and Elisabeth Mangold and Noethen, {Markus M.} and Ludwig, {Kirsten U.} and Hetmanski, {Jacqueline B.} and Bailey-Wilson, {Joan E.} and Cropp, {Cheryl D.} and Qing Li and Silke Szymczak and Hasan Albacha-Hejazi and Khalid Alqosayer and {Leigh Field}, L. and Wu-Chou, {Yah Huei} and Doheny, {Kimberly F.} and Hua Ling and Scott, {Alan F.} and Beaty, {Terri H.}",

year = "2014",

month = jul,

doi = "10.1534/genetics.114.165225",

language = "英语",

volume = "197",

pages = "1039--1044",

journal = "Genetics",

issn = "0016-6731",

publisher = "Oxford University Press",

number = "3",

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Bureau, A, Parker, MM, Ruczinski, I, Taub, MA, Marazita, ML, Murray, JC, Mangold, E, Noethen, MM, Ludwig, KU, Hetmanski, JB, Bailey-Wilson, JE, Cropp, CD, Li, Q, Szymczak, S, Albacha-Hejazi, H, Alqosayer, K, Leigh Field, L, Wu-Chou, YH, Doheny, KF, Ling, H, Scott, AF & Beaty, TH 2014, 'Whole Exome sequencing of distant relatives in multiplex families implicates rare variants in candidate genes for oral clefts', Genetics, 卷 197, 編號 3, 頁 1039-1044. https://doi.org/10.1534/genetics.114.165225

TY - JOUR

T1 - Whole Exome sequencing of distant relatives in multiplex families implicates rare variants in candidate genes for oral clefts

AU - Bureau, Alexandre

AU - Parker, Margaret M.

AU - Ruczinski, Ingo

AU - Taub, Margaret A.

AU - Marazita, Mary L.

AU - Murray, Jeffrey C.

AU - Mangold, Elisabeth

AU - Noethen, Markus M.

AU - Ludwig, Kirsten U.

AU - Hetmanski, Jacqueline B.

AU - Bailey-Wilson, Joan E.

AU - Cropp, Cheryl D.

AU - Li, Qing

AU - Szymczak, Silke

AU - Albacha-Hejazi, Hasan

AU - Alqosayer, Khalid

AU - Leigh Field, L.

AU - Wu-Chou, Yah Huei

AU - Doheny, Kimberly F.

AU - Ling, Hua

AU - Scott, Alan F.

AU - Beaty, Terri H.

PY - 2014/7

Y1 - 2014/7

N2 - A dozen genes/regions have been confirmed as genetic risk factors for oral clefts in human association and linkage studies, and animal models argue even more genes may be involved. Genomic sequencing studies should identify specific causal variants and may reveal additional genes as influencing risk to oral clefts, which have a complex and heterogeneous etiology. We conducted a whole exome sequencing (WES) study to search for potentially causal variants using affected relatives drawn from multiplex cleft families. Two or three affected second, third, and higher degree relatives from 55 multiplex families were sequenced. We examined rare single nucleotide variants (SNVs) shared by affected relatives in 348 recognized candidate genes. Exact probabilities that affected relatives would share these rare variants were calculated, given pedigree structures, and corrected for the number of variants tested. Five novel and potentially damaging SNVs shared by affected distant relatives were found and confirmed by Sanger sequencing. One damaging SNV in CDH1, shared by three affected second cousins from a single family, attained statistical significance (P = 0.02 after correcting for multiple tests). Family-based designs such as the one used in this WES study offer important advantages for identifying genes likely to be causing complex and heterogeneous disorders.

AB - A dozen genes/regions have been confirmed as genetic risk factors for oral clefts in human association and linkage studies, and animal models argue even more genes may be involved. Genomic sequencing studies should identify specific causal variants and may reveal additional genes as influencing risk to oral clefts, which have a complex and heterogeneous etiology. We conducted a whole exome sequencing (WES) study to search for potentially causal variants using affected relatives drawn from multiplex cleft families. Two or three affected second, third, and higher degree relatives from 55 multiplex families were sequenced. We examined rare single nucleotide variants (SNVs) shared by affected relatives in 348 recognized candidate genes. Exact probabilities that affected relatives would share these rare variants were calculated, given pedigree structures, and corrected for the number of variants tested. Five novel and potentially damaging SNVs shared by affected distant relatives were found and confirmed by Sanger sequencing. One damaging SNV in CDH1, shared by three affected second cousins from a single family, attained statistical significance (P = 0.02 after correcting for multiple tests). Family-based designs such as the one used in this WES study offer important advantages for identifying genes likely to be causing complex and heterogeneous disorders.

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U2 - 10.1534/genetics.114.165225

DO - 10.1534/genetics.114.165225

M3 - 文章

C2 - 24793288

AN - SCOPUS:84904246196

SN - 0016-6731

VL - 197

SP - 1039

EP - 1044

JO - Genetics

JF - Genetics

IS - 3

ER -

Whole Exome sequencing of distant relatives in multiplex families implicates rare variants in candidate genes for oral clefts

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