Bias in association studies of systemic lupus erythematosus susceptibility due to geographical variation in the frequency of a programmed cell death 1 polymorphism across Europe

I. Ferreiros-Vidal; S. D'Alfonso; C. Papasteriades; F. N. Skopouli; M. Marchini; R. Scorza; S. Migliaresi; G. D. Sebastiani; E. Endreffy; M. Mavromati; I. Kappou-Rigatou; S. Ruzickova; C. Dostal; R. E. Schmidt; T. Witte; J. J. Gomez-Reino; A. Gonzalez

doi:10.1038/sj.gene.6364370

Bias in association studies of systemic lupus erythematosus susceptibility due to geographical variation in the frequency of a programmed cell death 1 polymorphism across Europe

I. Ferreiros-Vidal, S. D'Alfonso, C. Papasteriades, F. N. Skopouli, M. Marchini, R. Scorza, S. Migliaresi, G. D. Sebastiani, E. Endreffy, M. Mavromati, I. Kappou-Rigatou, S. Ruzickova, C. Dostal, R. E. Schmidt, T. Witte, J. J. Gomez-Reino, A. Gonzalez

Dipartimento di Scienze della Salute

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

Abstract

We obtained eight collections of DNA samples from ethnically matched systemic lupus erythematosus (SLE) patients and controls from five European countries totaling 783 patients and 1210 controls. A highly significant cline in the frequency of the PD1.3 A allele was found among controls but not among SLE patients. The frequency of the PD1.3 A allele increased from the Northeast to the Southwest of Europe. The cline was clearly apparent (P=1.2 × 10^-6) when data from controls of other five SLE susceptibility studies were included in the analysis. This variation has severely biased SLE association studies owing to the lack of parallel changes in SLE patients. As a consequence, the PD1.3 A allele was more common in SLE patients than in controls in the Northeast and Center of Europe, similar to controls in Southeast Europe, and less frequent than in the controls in the Southwest of the Continent. This dissociation in allele frequencies between SLE patients and controls in different subpopulations indicated that programmed cell death 1 variation and disease susceptibility are not independent but the type of relationship is currently unclear. As allele frequency clines are common in other polymorphisms their impact in genetic epidemiology studies should be carefully considered.

Lingua originale	Inglese
pagine (da-a)	138-146
Numero di pagine	9
Rivista	Genes and Immunity
Volume	8
Numero di pubblicazione	2
DOI	https://doi.org/10.1038/sj.gene.6364370
Stato di pubblicazione	Pubblicato - mar 2007

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Ferreiros-Vidal, I., D'Alfonso, S., Papasteriades, C., Skopouli, F. N., Marchini, M., Scorza, R., Migliaresi, S., Sebastiani, G. D., Endreffy, E., Mavromati, M., Kappou-Rigatou, I., Ruzickova, S., Dostal, C., Schmidt, R. E., Witte, T., Gomez-Reino, J. J., & Gonzalez, A. (2007). Bias in association studies of systemic lupus erythematosus susceptibility due to geographical variation in the frequency of a programmed cell death 1 polymorphism across Europe. Genes and Immunity, 8(2), 138-146. https://doi.org/10.1038/sj.gene.6364370

@article{ea63498ea5bc4a23a3fcf2778c407169,

title = "Bias in association studies of systemic lupus erythematosus susceptibility due to geographical variation in the frequency of a programmed cell death 1 polymorphism across Europe",

abstract = "We obtained eight collections of DNA samples from ethnically matched systemic lupus erythematosus (SLE) patients and controls from five European countries totaling 783 patients and 1210 controls. A highly significant cline in the frequency of the PD1.3 A allele was found among controls but not among SLE patients. The frequency of the PD1.3 A allele increased from the Northeast to the Southwest of Europe. The cline was clearly apparent (P=1.2 × 10-6) when data from controls of other five SLE susceptibility studies were included in the analysis. This variation has severely biased SLE association studies owing to the lack of parallel changes in SLE patients. As a consequence, the PD1.3 A allele was more common in SLE patients than in controls in the Northeast and Center of Europe, similar to controls in Southeast Europe, and less frequent than in the controls in the Southwest of the Continent. This dissociation in allele frequencies between SLE patients and controls in different subpopulations indicated that programmed cell death 1 variation and disease susceptibility are not independent but the type of relationship is currently unclear. As allele frequency clines are common in other polymorphisms their impact in genetic epidemiology studies should be carefully considered.",

author = "I. Ferreiros-Vidal and S. D'Alfonso and C. Papasteriades and Skopouli, \{F. N.\} and M. Marchini and R. Scorza and S. Migliaresi and Sebastiani, \{G. D.\} and E. Endreffy and M. Mavromati and I. Kappou-Rigatou and S. Ruzickova and C. Dostal and Schmidt, \{R. E.\} and T. Witte and Gomez-Reino, \{J. J.\} and A. Gonzalez",

note = "Funding Information: We acknowledge Harry M Moutsopoulos for his collaboration and comments, Snaevar Sigurdsson and Ann-Christine Syv{\"a}nen for sharing data and Manuel Calaza, Marta Alarcon and Javier Costas for their comments. Cristina Fernandez-Lopez and Marta Picado have provided outstanding technical support. This work has been supported by Fondo de Investigacion Sanitaria, Instituto de Salud Carlos III (Spain), Grants 01/3138, 02/0713, 04/ 1651 that are partially financed by the FEDER program of the EU and by grants from the Xunta de Galicia. IF-V is supported by a BEFI fellowship of the Fondo de Investigacion Sanitaria, Instituto de Salud Carlos III (Spain). SR and CD were supported by Grant 00023728 of the Ministry of Health of the Czech Republic. RES and TW were supported by BMBF, KN Rheuma C2.12. Work by SD{\textquoteright}A was supported by Telethon (Grant E1221) and the CARIPLO Foundation.",

year = "2007",

month = mar,

doi = "10.1038/sj.gene.6364370",

language = "English",

volume = "8",

pages = "138--146",

journal = "Genes and Immunity",

issn = "1466-4879",

publisher = "Springer Nature",

number = "2",

}

Ferreiros-Vidal, I, D'Alfonso, S, Papasteriades, C, Skopouli, FN, Marchini, M, Scorza, R, Migliaresi, S, Sebastiani, GD, Endreffy, E, Mavromati, M, Kappou-Rigatou, I, Ruzickova, S, Dostal, C, Schmidt, RE, Witte, T, Gomez-Reino, JJ & Gonzalez, A 2007, 'Bias in association studies of systemic lupus erythematosus susceptibility due to geographical variation in the frequency of a programmed cell death 1 polymorphism across Europe', Genes and Immunity, vol. 8, n. 2, pagg. 138-146. https://doi.org/10.1038/sj.gene.6364370

Bias in association studies of systemic lupus erythematosus susceptibility due to geographical variation in the frequency of a programmed cell death 1 polymorphism across Europe. / Ferreiros-Vidal, I.; D'Alfonso, S.; Papasteriades, C. et al.
In: Genes and Immunity, Vol. 8, N. 2, 03.2007, pag. 138-146.

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

TY - JOUR

T1 - Bias in association studies of systemic lupus erythematosus susceptibility due to geographical variation in the frequency of a programmed cell death 1 polymorphism across Europe

AU - Ferreiros-Vidal, I.

AU - D'Alfonso, S.

AU - Papasteriades, C.

AU - Skopouli, F. N.

AU - Marchini, M.

AU - Scorza, R.

AU - Migliaresi, S.

AU - Sebastiani, G. D.

AU - Endreffy, E.

AU - Mavromati, M.

AU - Kappou-Rigatou, I.

AU - Ruzickova, S.

AU - Dostal, C.

AU - Schmidt, R. E.

AU - Witte, T.

AU - Gomez-Reino, J. J.

AU - Gonzalez, A.

N1 - Funding Information: We acknowledge Harry M Moutsopoulos for his collaboration and comments, Snaevar Sigurdsson and Ann-Christine Syvänen for sharing data and Manuel Calaza, Marta Alarcon and Javier Costas for their comments. Cristina Fernandez-Lopez and Marta Picado have provided outstanding technical support. This work has been supported by Fondo de Investigacion Sanitaria, Instituto de Salud Carlos III (Spain), Grants 01/3138, 02/0713, 04/ 1651 that are partially financed by the FEDER program of the EU and by grants from the Xunta de Galicia. IF-V is supported by a BEFI fellowship of the Fondo de Investigacion Sanitaria, Instituto de Salud Carlos III (Spain). SR and CD were supported by Grant 00023728 of the Ministry of Health of the Czech Republic. RES and TW were supported by BMBF, KN Rheuma C2.12. Work by SD’A was supported by Telethon (Grant E1221) and the CARIPLO Foundation.

PY - 2007/3

Y1 - 2007/3

N2 - We obtained eight collections of DNA samples from ethnically matched systemic lupus erythematosus (SLE) patients and controls from five European countries totaling 783 patients and 1210 controls. A highly significant cline in the frequency of the PD1.3 A allele was found among controls but not among SLE patients. The frequency of the PD1.3 A allele increased from the Northeast to the Southwest of Europe. The cline was clearly apparent (P=1.2 × 10-6) when data from controls of other five SLE susceptibility studies were included in the analysis. This variation has severely biased SLE association studies owing to the lack of parallel changes in SLE patients. As a consequence, the PD1.3 A allele was more common in SLE patients than in controls in the Northeast and Center of Europe, similar to controls in Southeast Europe, and less frequent than in the controls in the Southwest of the Continent. This dissociation in allele frequencies between SLE patients and controls in different subpopulations indicated that programmed cell death 1 variation and disease susceptibility are not independent but the type of relationship is currently unclear. As allele frequency clines are common in other polymorphisms their impact in genetic epidemiology studies should be carefully considered.

AB - We obtained eight collections of DNA samples from ethnically matched systemic lupus erythematosus (SLE) patients and controls from five European countries totaling 783 patients and 1210 controls. A highly significant cline in the frequency of the PD1.3 A allele was found among controls but not among SLE patients. The frequency of the PD1.3 A allele increased from the Northeast to the Southwest of Europe. The cline was clearly apparent (P=1.2 × 10-6) when data from controls of other five SLE susceptibility studies were included in the analysis. This variation has severely biased SLE association studies owing to the lack of parallel changes in SLE patients. As a consequence, the PD1.3 A allele was more common in SLE patients than in controls in the Northeast and Center of Europe, similar to controls in Southeast Europe, and less frequent than in the controls in the Southwest of the Continent. This dissociation in allele frequencies between SLE patients and controls in different subpopulations indicated that programmed cell death 1 variation and disease susceptibility are not independent but the type of relationship is currently unclear. As allele frequency clines are common in other polymorphisms their impact in genetic epidemiology studies should be carefully considered.

UR - https://www.scopus.com/pages/publications/33847779224

U2 - 10.1038/sj.gene.6364370

DO - 10.1038/sj.gene.6364370

M3 - Article

SN - 1466-4879

VL - 8

SP - 138

EP - 146

JO - Genes and Immunity

JF - Genes and Immunity

IS - 2

ER -

Bias in association studies of systemic lupus erythematosus susceptibility due to geographical variation in the frequency of a programmed cell death 1 polymorphism across Europe

Abstract

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