Complement factor H genetic variant and age-related macular degeneration: effect size, modifiers and relationship to disease subtype

Reecha Sofat; Juan P. Casas; Andrew R. Webster; Alan C. Bird; Samantha S. Mann; John R. W. Yates; Anthony T. Moore; Tiina Sepp; Valentina Cipriani; Catey Bunce; Jane C. Khan; Humma Shahid; Anand Swaroop; Gonçalo Abecasis; Kari E. H. Branham; Sepideh Zareparsi; Arthur A. Bergen; Caroline C. W. Klaver; Dominique C. Baas; Kang Zhang; Yuhong Chen; Daniel Gibbs; Bernhard H. F. Weber; Claudia N. Keilhauer; Lars G. Fritsche; Andrew Lotery; Angela J. Cree; Helen L. Griffiths; Shomi S. Bhattacharya; Li L. Chen; Sharon A. Jenkins; Tunde Peto; Mark Lathrop; Thierry Leveillard; Michael B. Gorin; Daniel E. Weeks; Maria Carolina Ortube; Robert E. Ferrell; Johanna Jakobsdottir; Yvette P. Conley; Mati Rahu; Johan H. Seland; Gisele Soubrane; Fotis Topouzis; Jesus Vioque; Laura Tomazzoli; Ian Young; John Whittaker; Usha Chakravarthy; Paulus T. V. M. de Jong; Liam Smeeth; Astrid Fletcher; Aroon D. Hingorani

doi:https://doi.org/10.1093/ije/dyr204

Complement factor H genetic variant and age-related macular degeneration: effect size, modifiers and relationship to disease subtype

Reecha Sofat, Juan P. Casas, Andrew R. Webster, Alan C. Bird, Samantha S. Mann, John R. W. Yates, Anthony T. Moore, Tiina Sepp, Valentina Cipriani, Catey Bunce, Jane C. Khan, Humma Shahid, Anand Swaroop, Gonçalo Abecasis, Kari E. H. Branham, Sepideh Zareparsi, Arthur A. Bergen, Caroline C. W. Klaver, Dominique C. Baas, Kang ZhangYuhong Chen, Daniel Gibbs, Bernhard H. F. Weber, Claudia N. Keilhauer, Lars G. Fritsche, Andrew Lotery, Angela J. Cree, Helen L. Griffiths, Shomi S. Bhattacharya, Li L. Chen, Sharon A. Jenkins, Tunde Peto, Mark Lathrop, Thierry Leveillard, Michael B. Gorin, Daniel E. Weeks, Maria Carolina Ortube, Robert E. Ferrell, Johanna Jakobsdottir, Yvette P. Conley, Mati Rahu, Johan H. Seland, Gisele Soubrane, Fotis Topouzis, Jesus Vioque, Laura Tomazzoli, Ian Young, John Whittaker, Usha Chakravarthy, Paulus T. V. M. de Jong, Liam Smeeth, Astrid Fletcher, Aroon D. Hingorani

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Abstract

Variation in the complement factor H gene (CFH) is associated with risk of late age-related macular degeneration (AMD). Previous studies have been case-control studies in populations of European ancestry with little differentiation in AMD subtype, and insufficient power to confirm or refute effect modification by smoking. To precisely quantify the association of the single nucleotide polymorphism (SNP rs1061170, 'Y402H') with risk of AMD among studies with differing study designs, participant ancestry and AMD grade and to investigate effect modification by smoking, we report two unpublished genetic association studies (n = 2759) combined with data from 24 published studies (26 studies, 26,494 individuals, including 14,174 cases of AMD) of European ancestry, 10 of which provided individual-level data used to test gene-smoking interaction; and 16 published studies from non-European ancestry. In individuals of European ancestry, there was a significant association between Y402H and late-AMD with a per-allele odds ratio (OR) of 2.27 [95% confidence interval (CI) 2.10-2.45; P = 1.1 x 10(-161)]. There was no evidence of effect modification by smoking (P = 0.75). The frequency of Y402H varied by ancestral origin and the association with AMD in non-Europeans was less clear, limited by paucity of studies. The Y402H variant confers a 2-fold higher risk of late-AMD per copy in individuals of European descent. This was stable to stratification by study design and AMD classification and not modified by smoking. The lack of association in non-Europeans requires further verification. These findings are of direct relevance for disease prediction. New research is needed to ascertain if differences in circulating levels, expression or activity of factor H protein explain the genetic association

Original language	English
Pages (from-to)	250-262
Journal	International journal of epidemiology
Volume	41
Issue number	1
DOIs	https://doi.org/10.1093/ije/dyr204
Publication status	Published - 2012

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Sofat, R., Casas, J. P., Webster, A. R., Bird, A. C., Mann, S. S., Yates, J. R. W., Moore, A. T., Sepp, T., Cipriani, V., Bunce, C., Khan, J. C., Shahid, H., Swaroop, A., Abecasis, G., Branham, K. E. H., Zareparsi, S., Bergen, A. A., Klaver, C. C. W., Baas, D. C., ... Hingorani, A. D. (2012). Complement factor H genetic variant and age-related macular degeneration: effect size, modifiers and relationship to disease subtype. International journal of epidemiology, 41(1), 250-262. https://doi.org/10.1093/ije/dyr204

@article{925b6bfa3d5047adbd95b10da6b88394,

title = "Complement factor H genetic variant and age-related macular degeneration: effect size, modifiers and relationship to disease subtype",

abstract = "Variation in the complement factor H gene (CFH) is associated with risk of late age-related macular degeneration (AMD). Previous studies have been case-control studies in populations of European ancestry with little differentiation in AMD subtype, and insufficient power to confirm or refute effect modification by smoking. To precisely quantify the association of the single nucleotide polymorphism (SNP rs1061170, 'Y402H') with risk of AMD among studies with differing study designs, participant ancestry and AMD grade and to investigate effect modification by smoking, we report two unpublished genetic association studies (n = 2759) combined with data from 24 published studies (26 studies, 26,494 individuals, including 14,174 cases of AMD) of European ancestry, 10 of which provided individual-level data used to test gene-smoking interaction; and 16 published studies from non-European ancestry. In individuals of European ancestry, there was a significant association between Y402H and late-AMD with a per-allele odds ratio (OR) of 2.27 [95% confidence interval (CI) 2.10-2.45; P = 1.1 x 10(-161)]. There was no evidence of effect modification by smoking (P = 0.75). The frequency of Y402H varied by ancestral origin and the association with AMD in non-Europeans was less clear, limited by paucity of studies. The Y402H variant confers a 2-fold higher risk of late-AMD per copy in individuals of European descent. This was stable to stratification by study design and AMD classification and not modified by smoking. The lack of association in non-Europeans requires further verification. These findings are of direct relevance for disease prediction. New research is needed to ascertain if differences in circulating levels, expression or activity of factor H protein explain the genetic association",

author = "Reecha Sofat and Casas, {Juan P.} and Webster, {Andrew R.} and Bird, {Alan C.} and Mann, {Samantha S.} and Yates, {John R. W.} and Moore, {Anthony T.} and Tiina Sepp and Valentina Cipriani and Catey Bunce and Khan, {Jane C.} and Humma Shahid and Anand Swaroop and Gon{\c c}alo Abecasis and Branham, {Kari E. H.} and Sepideh Zareparsi and Bergen, {Arthur A.} and Klaver, {Caroline C. W.} and Baas, {Dominique C.} and Kang Zhang and Yuhong Chen and Daniel Gibbs and Weber, {Bernhard H. F.} and Keilhauer, {Claudia N.} and Fritsche, {Lars G.} and Andrew Lotery and Cree, {Angela J.} and Griffiths, {Helen L.} and Bhattacharya, {Shomi S.} and Chen, {Li L.} and Jenkins, {Sharon A.} and Tunde Peto and Mark Lathrop and Thierry Leveillard and Gorin, {Michael B.} and Weeks, {Daniel E.} and Ortube, {Maria Carolina} and Ferrell, {Robert E.} and Johanna Jakobsdottir and Conley, {Yvette P.} and Mati Rahu and Seland, {Johan H.} and Gisele Soubrane and Fotis Topouzis and Jesus Vioque and Laura Tomazzoli and Ian Young and John Whittaker and Usha Chakravarthy and {de Jong}, {Paulus T. V. M.} and Liam Smeeth and Astrid Fletcher and Hingorani, {Aroon D.}",

year = "2012",

doi = "https://doi.org/10.1093/ije/dyr204",

language = "English",

volume = "41",

pages = "250--262",

journal = "International journal of epidemiology",

issn = "0300-5771",

publisher = "Oxford University Press",

number = "1",

}

Sofat, R, Casas, JP, Webster, AR, Bird, AC, Mann, SS, Yates, JRW, Moore, AT, Sepp, T, Cipriani, V, Bunce, C, Khan, JC, Shahid, H, Swaroop, A, Abecasis, G, Branham, KEH, Zareparsi, S, Bergen, AA, Klaver, CCW, Baas, DC, Zhang, K, Chen, Y, Gibbs, D, Weber, BHF, Keilhauer, CN, Fritsche, LG, Lotery, A, Cree, AJ, Griffiths, HL, Bhattacharya, SS, Chen, LL, Jenkins, SA, Peto, T, Lathrop, M, Leveillard, T, Gorin, MB, Weeks, DE, Ortube, MC, Ferrell, RE, Jakobsdottir, J, Conley, YP, Rahu, M, Seland, JH, Soubrane, G, Topouzis, F, Vioque, J, Tomazzoli, L, Young, I, Whittaker, J, Chakravarthy, U, de Jong, PTVM, Smeeth, L, Fletcher, A & Hingorani, AD 2012, 'Complement factor H genetic variant and age-related macular degeneration: effect size, modifiers and relationship to disease subtype', International journal of epidemiology, vol. 41, no. 1, pp. 250-262. https://doi.org/10.1093/ije/dyr204

TY - JOUR

T1 - Complement factor H genetic variant and age-related macular degeneration: effect size, modifiers and relationship to disease subtype

AU - Sofat, Reecha

AU - Casas, Juan P.

AU - Webster, Andrew R.

AU - Bird, Alan C.

AU - Mann, Samantha S.

AU - Yates, John R. W.

AU - Moore, Anthony T.

AU - Sepp, Tiina

AU - Cipriani, Valentina

AU - Bunce, Catey

AU - Khan, Jane C.

AU - Shahid, Humma

AU - Swaroop, Anand

AU - Abecasis, Gonçalo

AU - Branham, Kari E. H.

AU - Zareparsi, Sepideh

AU - Bergen, Arthur A.

AU - Klaver, Caroline C. W.

AU - Baas, Dominique C.

AU - Zhang, Kang

AU - Chen, Yuhong

AU - Gibbs, Daniel

AU - Weber, Bernhard H. F.

AU - Keilhauer, Claudia N.

AU - Fritsche, Lars G.

AU - Lotery, Andrew

AU - Cree, Angela J.

AU - Griffiths, Helen L.

AU - Bhattacharya, Shomi S.

AU - Chen, Li L.

AU - Jenkins, Sharon A.

AU - Peto, Tunde

AU - Lathrop, Mark

AU - Leveillard, Thierry

AU - Gorin, Michael B.

AU - Weeks, Daniel E.

AU - Ortube, Maria Carolina

AU - Ferrell, Robert E.

AU - Jakobsdottir, Johanna

AU - Conley, Yvette P.

AU - Rahu, Mati

AU - Seland, Johan H.

AU - Soubrane, Gisele

AU - Topouzis, Fotis

AU - Vioque, Jesus

AU - Tomazzoli, Laura

AU - Young, Ian

AU - Whittaker, John

AU - Chakravarthy, Usha

AU - de Jong, Paulus T. V. M.

AU - Smeeth, Liam

AU - Fletcher, Astrid

AU - Hingorani, Aroon D.

PY - 2012

Y1 - 2012

N2 - Variation in the complement factor H gene (CFH) is associated with risk of late age-related macular degeneration (AMD). Previous studies have been case-control studies in populations of European ancestry with little differentiation in AMD subtype, and insufficient power to confirm or refute effect modification by smoking. To precisely quantify the association of the single nucleotide polymorphism (SNP rs1061170, 'Y402H') with risk of AMD among studies with differing study designs, participant ancestry and AMD grade and to investigate effect modification by smoking, we report two unpublished genetic association studies (n = 2759) combined with data from 24 published studies (26 studies, 26,494 individuals, including 14,174 cases of AMD) of European ancestry, 10 of which provided individual-level data used to test gene-smoking interaction; and 16 published studies from non-European ancestry. In individuals of European ancestry, there was a significant association between Y402H and late-AMD with a per-allele odds ratio (OR) of 2.27 [95% confidence interval (CI) 2.10-2.45; P = 1.1 x 10(-161)]. There was no evidence of effect modification by smoking (P = 0.75). The frequency of Y402H varied by ancestral origin and the association with AMD in non-Europeans was less clear, limited by paucity of studies. The Y402H variant confers a 2-fold higher risk of late-AMD per copy in individuals of European descent. This was stable to stratification by study design and AMD classification and not modified by smoking. The lack of association in non-Europeans requires further verification. These findings are of direct relevance for disease prediction. New research is needed to ascertain if differences in circulating levels, expression or activity of factor H protein explain the genetic association

AB - Variation in the complement factor H gene (CFH) is associated with risk of late age-related macular degeneration (AMD). Previous studies have been case-control studies in populations of European ancestry with little differentiation in AMD subtype, and insufficient power to confirm or refute effect modification by smoking. To precisely quantify the association of the single nucleotide polymorphism (SNP rs1061170, 'Y402H') with risk of AMD among studies with differing study designs, participant ancestry and AMD grade and to investigate effect modification by smoking, we report two unpublished genetic association studies (n = 2759) combined with data from 24 published studies (26 studies, 26,494 individuals, including 14,174 cases of AMD) of European ancestry, 10 of which provided individual-level data used to test gene-smoking interaction; and 16 published studies from non-European ancestry. In individuals of European ancestry, there was a significant association between Y402H and late-AMD with a per-allele odds ratio (OR) of 2.27 [95% confidence interval (CI) 2.10-2.45; P = 1.1 x 10(-161)]. There was no evidence of effect modification by smoking (P = 0.75). The frequency of Y402H varied by ancestral origin and the association with AMD in non-Europeans was less clear, limited by paucity of studies. The Y402H variant confers a 2-fold higher risk of late-AMD per copy in individuals of European descent. This was stable to stratification by study design and AMD classification and not modified by smoking. The lack of association in non-Europeans requires further verification. These findings are of direct relevance for disease prediction. New research is needed to ascertain if differences in circulating levels, expression or activity of factor H protein explain the genetic association

U2 - https://doi.org/10.1093/ije/dyr204

DO - https://doi.org/10.1093/ije/dyr204

M3 - Article

C2 - 22253316

SN - 0300-5771

VL - 41

SP - 250

EP - 262

JO - International journal of epidemiology

JF - International journal of epidemiology

IS - 1

ER -