Further evidence for an association of ABCR alleles with age-related macular degeneration

R. Allikmets; J. Tammur; A. Hutchinson; R. A. Lewis; N. F. Shroyer; K. Dalakishvili; J. R. Lupski; K. Steiner; D. Pauleikhoff; F. G. Holz; B. H.F. Weber; M. Dean; A. Atkinson; M. H. Gail; P. S. Bernstein; N. Singh; N. Zabriskie; A. Peiffer; M. Leppert; J. M. Seddon; K. Zhang; J. S. Sunness; N. S. Udar; S. Yelchits; R. Silva-Garcia; K. W. Small; F. Simonelli; F. Testa; M. D'Urso; R. Brancato; E. Rinaldi; S. Ingvast; A. Taube; C. Wadelius; E. Souied; D. Ducroq; J. Kaplan; J. J.M. Assink; J. B. Ten Brink; P. T.V.M. De Jong; A. A.B. Bergen; A. Maugeri; M. A. Van Driel; C. B. Hoyng; F. P.M. Cremers; E. Paloma; R. Coco; S. Balcells; R. Gonzalez- Duarte; S. Kermani

doi:https://doi.org/10.1086/303018

Further evidence for an association of ABCR alleles with age-related macular degeneration

R. Allikmets, J. Tammur, A. Hutchinson, R. A. Lewis, N. F. Shroyer, K. Dalakishvili, J. R. Lupski, K. Steiner, D. Pauleikhoff, F. G. Holz, B. H.F. Weber, M. Dean, A. Atkinson, M. H. Gail, P. S. Bernstein, N. Singh, N. Zabriskie, A. Peiffer, M. Leppert, J. M. SeddonK. Zhang, J. S. Sunness, N. S. Udar, S. Yelchits, R. Silva-Garcia, K. W. Small, F. Simonelli, F. Testa, M. D'Urso, R. Brancato, E. Rinaldi, S. Ingvast, A. Taube, C. Wadelius, E. Souied, D. Ducroq, J. Kaplan, J. J.M. Assink, J. B. Ten Brink, P. T.V.M. De Jong, A. A.B. Bergen, A. Maugeri, M. A. Van Driel, C. B. Hoyng, F. P.M. Cremers, E. Paloma, R. Coco, S. Balcells, R. Gonzalez- Duarte, S. Kermani

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

265 Citations (Scopus)

Abstract

Age-related macular degeneration (AMD) accounts for >50% of the registered visual disability among North American and Western European populations and has been associated both with environmental factors, such as smoking, and with genetic factors. Previously we have reported disease- associated variants in the ABCR (also called ABCA4) gene in a subset of patients affected with this complex disorder. We have now tested our original hypothesis, that ABCR is a dominant susceptibility locus for AMD, by screening 1,218 unrelated AMD patients of North American and Western European origin and 1,258 comparison individuals from 15 centers in North America and Europe for the two most frequent AMD-associated variants found in ABCR. These two sequence changes, G1961E and D2177N, were found in one allele of ABCR in 40 patients ~3.4%), and in 13 control subjects (~0.95%). Fisher's two-sided exact test confirmed that these two variants are associated with AMD at a statistically significant level (P < .0001). The risk of AMD is elevated approximately threefold in D2177N carriers and approximately fivefold in G1961E carriers. The identification of a gene that confers risk of AMD is an important step in unraveling this complex disorder.

Original language	English
Pages (from-to)	487-491
Number of pages	5
Journal	American journal of human genetics
Volume	67
Issue number	2
DOIs	https://doi.org/10.1086/303018
Publication status	Published - 2000

Access to Document

https://doi.org/10.1086/303018

Cite this

Allikmets, R., Tammur, J., Hutchinson, A., Lewis, R. A., Shroyer, N. F., Dalakishvili, K., Lupski, J. R., Steiner, K., Pauleikhoff, D., Holz, F. G., Weber, B. H. F., Dean, M., Atkinson, A., Gail, M. H., Bernstein, P. S., Singh, N., Zabriskie, N., Peiffer, A., Leppert, M., ... Kermani, S. (2000). Further evidence for an association of ABCR alleles with age-related macular degeneration. American journal of human genetics, 67(2), 487-491. https://doi.org/10.1086/303018

@article{39a303b8bad840dbadbaddc2adc568d9,

title = "Further evidence for an association of ABCR alleles with age-related macular degeneration",

abstract = "Age-related macular degeneration (AMD) accounts for >50% of the registered visual disability among North American and Western European populations and has been associated both with environmental factors, such as smoking, and with genetic factors. Previously we have reported disease- associated variants in the ABCR (also called ABCA4) gene in a subset of patients affected with this complex disorder. We have now tested our original hypothesis, that ABCR is a dominant susceptibility locus for AMD, by screening 1,218 unrelated AMD patients of North American and Western European origin and 1,258 comparison individuals from 15 centers in North America and Europe for the two most frequent AMD-associated variants found in ABCR. These two sequence changes, G1961E and D2177N, were found in one allele of ABCR in 40 patients ~3.4%), and in 13 control subjects (~0.95%). Fisher's two-sided exact test confirmed that these two variants are associated with AMD at a statistically significant level (P < .0001). The risk of AMD is elevated approximately threefold in D2177N carriers and approximately fivefold in G1961E carriers. The identification of a gene that confers risk of AMD is an important step in unraveling this complex disorder.",

author = "R. Allikmets and J. Tammur and A. Hutchinson and Lewis, {R. A.} and Shroyer, {N. F.} and K. Dalakishvili and Lupski, {J. R.} and K. Steiner and D. Pauleikhoff and Holz, {F. G.} and Weber, {B. H.F.} and M. Dean and A. Atkinson and Gail, {M. H.} and Bernstein, {P. S.} and N. Singh and N. Zabriskie and A. Peiffer and M. Leppert and Seddon, {J. M.} and K. Zhang and Sunness, {J. S.} and Udar, {N. S.} and S. Yelchits and R. Silva-Garcia and Small, {K. W.} and F. Simonelli and F. Testa and M. D'Urso and R. Brancato and E. Rinaldi and S. Ingvast and A. Taube and C. Wadelius and E. Souied and D. Ducroq and J. Kaplan and Assink, {J. J.M.} and {Ten Brink}, {J. B.} and {De Jong}, {P. T.V.M.} and Bergen, {A. A.B.} and A. Maugeri and {Van Driel}, {M. A.} and Hoyng, {C. B.} and Cremers, {F. P.M.} and E. Paloma and R. Coco and S. Balcells and {Gonzalez- Duarte}, R. and S. Kermani",

year = "2000",

doi = "https://doi.org/10.1086/303018",

language = "English",

volume = "67",

pages = "487--491",

journal = "American journal of human genetics",

issn = "0002-9297",

publisher = "Cell Press",

number = "2",

}

Allikmets, R, Tammur, J, Hutchinson, A, Lewis, RA, Shroyer, NF, Dalakishvili, K, Lupski, JR, Steiner, K, Pauleikhoff, D, Holz, FG, Weber, BHF, Dean, M, Atkinson, A, Gail, MH, Bernstein, PS, Singh, N, Zabriskie, N, Peiffer, A, Leppert, M, Seddon, JM, Zhang, K, Sunness, JS, Udar, NS, Yelchits, S, Silva-Garcia, R, Small, KW, Simonelli, F, Testa, F, D'Urso, M, Brancato, R, Rinaldi, E, Ingvast, S, Taube, A, Wadelius, C, Souied, E, Ducroq, D, Kaplan, J, Assink, JJM, Ten Brink, JB, De Jong, PTVM, Bergen, AAB, Maugeri, A, Van Driel, MA, Hoyng, CB, Cremers, FPM, Paloma, E, Coco, R, Balcells, S, Gonzalez- Duarte, R & Kermani, S 2000, 'Further evidence for an association of ABCR alleles with age-related macular degeneration', American journal of human genetics, vol. 67, no. 2, pp. 487-491. https://doi.org/10.1086/303018

TY - JOUR

T1 - Further evidence for an association of ABCR alleles with age-related macular degeneration

AU - Allikmets, R.

AU - Tammur, J.

AU - Hutchinson, A.

AU - Lewis, R. A.

AU - Shroyer, N. F.

AU - Dalakishvili, K.

AU - Lupski, J. R.

AU - Steiner, K.

AU - Pauleikhoff, D.

AU - Holz, F. G.

AU - Weber, B. H.F.

AU - Dean, M.

AU - Atkinson, A.

AU - Gail, M. H.

AU - Bernstein, P. S.

AU - Singh, N.

AU - Zabriskie, N.

AU - Peiffer, A.

AU - Leppert, M.

AU - Seddon, J. M.

AU - Zhang, K.

AU - Sunness, J. S.

AU - Udar, N. S.

AU - Yelchits, S.

AU - Silva-Garcia, R.

AU - Small, K. W.

AU - Simonelli, F.

AU - Testa, F.

AU - D'Urso, M.

AU - Brancato, R.

AU - Rinaldi, E.

AU - Ingvast, S.

AU - Taube, A.

AU - Wadelius, C.

AU - Souied, E.

AU - Ducroq, D.

AU - Kaplan, J.

AU - Assink, J. J.M.

AU - Ten Brink, J. B.

AU - De Jong, P. T.V.M.

AU - Bergen, A. A.B.

AU - Maugeri, A.

AU - Van Driel, M. A.

AU - Hoyng, C. B.

AU - Cremers, F. P.M.

AU - Paloma, E.

AU - Coco, R.

AU - Balcells, S.

AU - Gonzalez- Duarte, R.

AU - Kermani, S.

PY - 2000

Y1 - 2000

N2 - Age-related macular degeneration (AMD) accounts for >50% of the registered visual disability among North American and Western European populations and has been associated both with environmental factors, such as smoking, and with genetic factors. Previously we have reported disease- associated variants in the ABCR (also called ABCA4) gene in a subset of patients affected with this complex disorder. We have now tested our original hypothesis, that ABCR is a dominant susceptibility locus for AMD, by screening 1,218 unrelated AMD patients of North American and Western European origin and 1,258 comparison individuals from 15 centers in North America and Europe for the two most frequent AMD-associated variants found in ABCR. These two sequence changes, G1961E and D2177N, were found in one allele of ABCR in 40 patients ~3.4%), and in 13 control subjects (~0.95%). Fisher's two-sided exact test confirmed that these two variants are associated with AMD at a statistically significant level (P < .0001). The risk of AMD is elevated approximately threefold in D2177N carriers and approximately fivefold in G1961E carriers. The identification of a gene that confers risk of AMD is an important step in unraveling this complex disorder.

AB - Age-related macular degeneration (AMD) accounts for >50% of the registered visual disability among North American and Western European populations and has been associated both with environmental factors, such as smoking, and with genetic factors. Previously we have reported disease- associated variants in the ABCR (also called ABCA4) gene in a subset of patients affected with this complex disorder. We have now tested our original hypothesis, that ABCR is a dominant susceptibility locus for AMD, by screening 1,218 unrelated AMD patients of North American and Western European origin and 1,258 comparison individuals from 15 centers in North America and Europe for the two most frequent AMD-associated variants found in ABCR. These two sequence changes, G1961E and D2177N, were found in one allele of ABCR in 40 patients ~3.4%), and in 13 control subjects (~0.95%). Fisher's two-sided exact test confirmed that these two variants are associated with AMD at a statistically significant level (P < .0001). The risk of AMD is elevated approximately threefold in D2177N carriers and approximately fivefold in G1961E carriers. The identification of a gene that confers risk of AMD is an important step in unraveling this complex disorder.

UR - http://www.scopus.com/inward/record.url?scp=0033859128&partnerID=8YFLogxK

U2 - https://doi.org/10.1086/303018

DO - https://doi.org/10.1086/303018

M3 - Article

C2 - 10880298

SN - 0002-9297

VL - 67

SP - 487

EP - 491

JO - American journal of human genetics

JF - American journal of human genetics

IS - 2

ER -

Further evidence for an association of ABCR alleles with age-related macular degeneration

Abstract

Access to Document

Other files and links

Cite this