Whole-genome analysis of sporadic amyotrophic lateral sclerosis

Travis Dunckley; Matthew J. Huentelman; David W. Craig; John V. Pearson; Szabolcs Szelinger; Keta Joshipura; Rebecca F. Halperin; Chelsea Stamper; Kendall R. Jensen; David Letizia; Sharon E. Hesterlee; Alan Pestronk; Todd Levine; Tulio Bertorini; Michael C. Graves; Tahseen Mozaffar; Carlayne E. Jackson; Peter Bosch; April McVey; Arthur Dick; Richard Barohn; Catherine Lomen-Hoerth; Jeffrey Rosenfeld; Daniel T. O'Connor; Kuixing Zhang; Richard Crook; Henrik Ryberg; Michael Hutton; Jonathan Katz; Ericka P. Simpson; Hiroshi Mitsumoto; Robert Bowser; Robert G. Miller; Stanley H. Appel; Dietrich A. Stephan

doi:10.1056/NEJMoa070174

Whole-genome analysis of sporadic amyotrophic lateral sclerosis

Travis Dunckley, Matthew J. Huentelman, David W. Craig, John V. Pearson, Szabolcs Szelinger, Keta Joshipura, Rebecca F. Halperin, Chelsea Stamper, Kendall R. Jensen, David Letizia, Sharon E. Hesterlee, Alan Pestronk, Todd Levine, Tulio Bertorini, Michael C. Graves, Tahseen Mozaffar, Carlayne E. Jackson, Peter Bosch, April McVey, Arthur DickRichard Barohn, Catherine Lomen-Hoerth, Jeffrey Rosenfeld, Daniel T. O'Connor, Kuixing Zhang, Richard Crook, Henrik Ryberg, Michael Hutton, Jonathan Katz, Ericka P. Simpson, Hiroshi Mitsumoto, Robert Bowser, Robert G. Miller, Stanley H. Appel, Dietrich A. Stephan

Neurology

Research output: Contribution to journal › Article › peer-review

196 Scopus citations

Abstract

Background: Approximately 90% of persons with amyotrophic lateral sclerosis (ALS) have the sporadic form, which may be caused by the interaction of multiple environmental factors and previously unknown genes. Methods: We performed a genomewide association analysis using 766,955 single-nucleotide polymorphisms (SNPs) found in 386 white patients with sporadic ALS and 542 neurologically normal white controls (the discovery series). Associations of SNPs with sporadic ALS were confirmed in two independent replication populations: replication series 1, with 766 case patients with the disease and 750 neurologically normal controls, and replication series 2, with 135 case patients and 275 controls. Results: We identified 10 genetic loci that are significantly associated (P<0.05) with sporadic ALS in three independent series of case patients and controls and an additional 41 loci that had significant associations in two of the three series. The most significant association with disease in white case patients as compared with controls was found for a SNP near an uncharacterized gene known as FLJ10986 (P = 3.0 x 10^-4; odds ratio for having the genotype in patients vs. controls, 1.35; 95% confidence interval, 1.13 to 1.62). The FLJ10986 protein was found to be expressed in the spinal cord and cerebrospinal fluid of patients and of controls. Specific SNPs seem to be associated with sex, age at onset, and site of onset of sporadic ALS. Conclusions: Variants of FLJ10986 may confer susceptibility to sporadic ALS. FLJ10986 and 50 other candidate loci warrant further investigation for their potential role in conferring susceptibility to the disease.

Original language	English (US)
Pages (from-to)	775-788
Number of pages	14
Journal	New England Journal of Medicine
Volume	357
Issue number	8
DOIs	https://doi.org/10.1056/NEJMoa070174
State	Published - Aug 23 2007

ASJC Scopus subject areas

General Medicine

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Dunckley, T., Huentelman, M. J., Craig, D. W., Pearson, J. V., Szelinger, S., Joshipura, K., Halperin, R. F., Stamper, C., Jensen, K. R., Letizia, D., Hesterlee, S. E., Pestronk, A., Levine, T., Bertorini, T., Graves, M. C., Mozaffar, T., Jackson, C. E., Bosch, P., McVey, A., ... Stephan, D. A. (2007). Whole-genome analysis of sporadic amyotrophic lateral sclerosis. New England Journal of Medicine, 357(8), 775-788. https://doi.org/10.1056/NEJMoa070174

Dunckley, T, Huentelman, MJ, Craig, DW, Pearson, JV, Szelinger, S, Joshipura, K, Halperin, RF, Stamper, C, Jensen, KR, Letizia, D, Hesterlee, SE, Pestronk, A, Levine, T, Bertorini, T, Graves, MC, Mozaffar, T, Jackson, CE, Bosch, P, McVey, A, Dick, A, Barohn, R, Lomen-Hoerth, C, Rosenfeld, J, O'Connor, DT, Zhang, K, Crook, R, Ryberg, H, Hutton, M, Katz, J, Simpson, EP, Mitsumoto, H, Bowser, R, Miller, RG, Appel, SH & Stephan, DA 2007, 'Whole-genome analysis of sporadic amyotrophic lateral sclerosis', New England Journal of Medicine, vol. 357, no. 8, pp. 775-788. https://doi.org/10.1056/NEJMoa070174

@article{ac14ecff29c24357994c200f77e72096,

title = "Whole-genome analysis of sporadic amyotrophic lateral sclerosis",

abstract = "Background: Approximately 90% of persons with amyotrophic lateral sclerosis (ALS) have the sporadic form, which may be caused by the interaction of multiple environmental factors and previously unknown genes. Methods: We performed a genomewide association analysis using 766,955 single-nucleotide polymorphisms (SNPs) found in 386 white patients with sporadic ALS and 542 neurologically normal white controls (the discovery series). Associations of SNPs with sporadic ALS were confirmed in two independent replication populations: replication series 1, with 766 case patients with the disease and 750 neurologically normal controls, and replication series 2, with 135 case patients and 275 controls. Results: We identified 10 genetic loci that are significantly associated (P<0.05) with sporadic ALS in three independent series of case patients and controls and an additional 41 loci that had significant associations in two of the three series. The most significant association with disease in white case patients as compared with controls was found for a SNP near an uncharacterized gene known as FLJ10986 (P = 3.0 x 10-4; odds ratio for having the genotype in patients vs. controls, 1.35; 95% confidence interval, 1.13 to 1.62). The FLJ10986 protein was found to be expressed in the spinal cord and cerebrospinal fluid of patients and of controls. Specific SNPs seem to be associated with sex, age at onset, and site of onset of sporadic ALS. Conclusions: Variants of FLJ10986 may confer susceptibility to sporadic ALS. FLJ10986 and 50 other candidate loci warrant further investigation for their potential role in conferring susceptibility to the disease.",

author = "Travis Dunckley and Huentelman, {Matthew J.} and Craig, {David W.} and Pearson, {John V.} and Szabolcs Szelinger and Keta Joshipura and Halperin, {Rebecca F.} and Chelsea Stamper and Jensen, {Kendall R.} and David Letizia and Hesterlee, {Sharon E.} and Alan Pestronk and Todd Levine and Tulio Bertorini and Graves, {Michael C.} and Tahseen Mozaffar and Jackson, {Carlayne E.} and Peter Bosch and April McVey and Arthur Dick and Richard Barohn and Catherine Lomen-Hoerth and Jeffrey Rosenfeld and O'Connor, {Daniel T.} and Kuixing Zhang and Richard Crook and Henrik Ryberg and Michael Hutton and Jonathan Katz and Simpson, {Ericka P.} and Hiroshi Mitsumoto and Robert Bowser and Miller, {Robert G.} and Appel, {Stanley H.} and Stephan, {Dietrich A.}",

year = "2007",

month = aug,

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doi = "10.1056/NEJMoa070174",

language = "English (US)",

volume = "357",

pages = "775--788",

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T1 - Whole-genome analysis of sporadic amyotrophic lateral sclerosis

AU - Dunckley, Travis

AU - Huentelman, Matthew J.

AU - Craig, David W.

AU - Pearson, John V.

AU - Szelinger, Szabolcs

AU - Joshipura, Keta

AU - Halperin, Rebecca F.

AU - Stamper, Chelsea

AU - Jensen, Kendall R.

AU - Letizia, David

AU - Hesterlee, Sharon E.

AU - Pestronk, Alan

AU - Levine, Todd

AU - Bertorini, Tulio

AU - Graves, Michael C.

AU - Mozaffar, Tahseen

AU - Jackson, Carlayne E.

AU - Bosch, Peter

AU - McVey, April

AU - Dick, Arthur

AU - Barohn, Richard

AU - Lomen-Hoerth, Catherine

AU - Rosenfeld, Jeffrey

AU - O'Connor, Daniel T.

AU - Zhang, Kuixing

AU - Crook, Richard

AU - Ryberg, Henrik

AU - Hutton, Michael

AU - Katz, Jonathan

AU - Simpson, Ericka P.

AU - Mitsumoto, Hiroshi

AU - Bowser, Robert

AU - Miller, Robert G.

AU - Appel, Stanley H.

AU - Stephan, Dietrich A.

PY - 2007/8/23

Y1 - 2007/8/23

N2 - Background: Approximately 90% of persons with amyotrophic lateral sclerosis (ALS) have the sporadic form, which may be caused by the interaction of multiple environmental factors and previously unknown genes. Methods: We performed a genomewide association analysis using 766,955 single-nucleotide polymorphisms (SNPs) found in 386 white patients with sporadic ALS and 542 neurologically normal white controls (the discovery series). Associations of SNPs with sporadic ALS were confirmed in two independent replication populations: replication series 1, with 766 case patients with the disease and 750 neurologically normal controls, and replication series 2, with 135 case patients and 275 controls. Results: We identified 10 genetic loci that are significantly associated (P<0.05) with sporadic ALS in three independent series of case patients and controls and an additional 41 loci that had significant associations in two of the three series. The most significant association with disease in white case patients as compared with controls was found for a SNP near an uncharacterized gene known as FLJ10986 (P = 3.0 x 10-4; odds ratio for having the genotype in patients vs. controls, 1.35; 95% confidence interval, 1.13 to 1.62). The FLJ10986 protein was found to be expressed in the spinal cord and cerebrospinal fluid of patients and of controls. Specific SNPs seem to be associated with sex, age at onset, and site of onset of sporadic ALS. Conclusions: Variants of FLJ10986 may confer susceptibility to sporadic ALS. FLJ10986 and 50 other candidate loci warrant further investigation for their potential role in conferring susceptibility to the disease.

AB - Background: Approximately 90% of persons with amyotrophic lateral sclerosis (ALS) have the sporadic form, which may be caused by the interaction of multiple environmental factors and previously unknown genes. Methods: We performed a genomewide association analysis using 766,955 single-nucleotide polymorphisms (SNPs) found in 386 white patients with sporadic ALS and 542 neurologically normal white controls (the discovery series). Associations of SNPs with sporadic ALS were confirmed in two independent replication populations: replication series 1, with 766 case patients with the disease and 750 neurologically normal controls, and replication series 2, with 135 case patients and 275 controls. Results: We identified 10 genetic loci that are significantly associated (P<0.05) with sporadic ALS in three independent series of case patients and controls and an additional 41 loci that had significant associations in two of the three series. The most significant association with disease in white case patients as compared with controls was found for a SNP near an uncharacterized gene known as FLJ10986 (P = 3.0 x 10-4; odds ratio for having the genotype in patients vs. controls, 1.35; 95% confidence interval, 1.13 to 1.62). The FLJ10986 protein was found to be expressed in the spinal cord and cerebrospinal fluid of patients and of controls. Specific SNPs seem to be associated with sex, age at onset, and site of onset of sporadic ALS. Conclusions: Variants of FLJ10986 may confer susceptibility to sporadic ALS. FLJ10986 and 50 other candidate loci warrant further investigation for their potential role in conferring susceptibility to the disease.

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DO - 10.1056/NEJMoa070174

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AN - SCOPUS:34548083742

SN - 0028-4793

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JO - New England Journal of Medicine

JF - New England Journal of Medicine

IS - 8

ER -

Whole-genome analysis of sporadic amyotrophic lateral sclerosis

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