Filaggrin null alleles are not associated with psoriasis

Yiwei Zhao; Ana Terron-Kwiatkowski; Haihui Liao; Simon P. Lee; Michael H. Allen; Peter R. Hull; Linda E. Campbell; Richard C. Trembath; Francesca Capon; Christopher E.M. Griffiths; David Burden; Ross McManus; Rosalind Hughes; Brian Kirby; Sarah F. Rogers; Oliver Fitzgerald; David Kane; Jonathan N.W.N. Barker; Colin N.A. Palmer; Alan D. Irvine; W. H. Irwin McLean

doi:10.1038/sj.jid.5700817

Filaggrin null alleles are not associated with psoriasis

Yiwei Zhao, Ana Terron-Kwiatkowski, Haihui Liao, Simon P. Lee, Michael H. Allen, Peter R. Hull, Linda E. Campbell, Richard C. Trembath, Francesca Capon, Christopher E.M. Griffiths, David Burden, Ross McManus, Rosalind Hughes, Brian Kirby, Sarah F. Rogers, Oliver Fitzgerald, David Kane, Jonathan N.W.N. Barker, Colin N.A. Palmer, Alan D. IrvineW. H. Irwin McLean

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37 Citations (Scopus)

Résumé

Psoriasis is a common skin disease with an etiology consistent with a multifactorial trait. Several psoriasis susceptibility loci are known, a number of which are also implicated in a predisposition to atopic dermatitis (AD), including the epidermal differentiation complex on chromosome 1q21. It has recently been shown in several replicate studies that prevalent null alleles for the filaggrin gene (FLG) on 1q21 are an important genetic factor in AD. Here, we examined the role of these FLG variants in psoriasis using case:control association studies comparing Irish and UK psoriasis cohorts (combined n=691) to ethnically matched populations (combined n=2117). No association was present for the two common European FLG mutations R501X and 2282del4 (combined χ² P=0.989). In addition, the 3′ end of the FLG open-reading frame was sequenced in a number of patients with differing types of psoriasis (plaque, guttate, palmoplantar, and late-onset), which excluded the possibility of a gain-of-function frameshift mutation such as those found in loricrin or certain keratin genes. These data suggest that FLG mutations are unlikely to be involved in genetic susceptibility to psoriasis and implies that there may be within-locus heterogeneity in chromosomal regions involved in both AD and psoriasis.

Langue d'origine	English
Pages (de-à)	1878-1882
Nombre de pages	5
Journal	Journal of Investigative Dermatology
Volume	127
Numéro de publication	8
DOI	https://doi.org/10.1038/sj.jid.5700817
Statut de publication	Published - août 2007
Publié à l'externe	Oui

Note bibliographique

Funding Information:
We thank the patients and their families for their participation, which made this research possible. We also thank to Jayne Mcfarlane, Epithelial Genetics Group for clerical assistance. The Barker group was supported by The British Skin Foundation (N.J.R. and J.N.B.), The Wellcome Trust (R.C.T. and J.N.B.), and the Psoriasis Association (J.N.W.N.B, C.E.M.G., and D.B.). The McLean group is supported by grants from The Dystrophic Epidermolysis Bullosa Research Association, The Pachyonychia Congenita Project, the British Skin Foundation/National Eczema Society (W.H.I.M and Frances J.D. Smith). Filaggrin research in Dundee is supported by a donation from an anonymous family from Tayside, Scotland. The Palmer group is supported by the Biotechnology and Biological Sciences Research Council (award D13460), Scottish Enterprise Tayside and the Gannochy Trust, and the Scottish Executive Genetic Health Initiative. We acknowledge the following clinicians for their support: Louise Barnes and Rosemarie Watson, St James Hospital, Dublin; Paul Collins, Barry Bresnihan, and Doug Veale, St Vincent's University Hospital, Dublin.

ASJC Scopus Subject Areas

Biochemistry
Molecular Biology
Dermatology
Cell Biology

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10.1038/sj.jid.5700817

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Zhao, Y., Terron-Kwiatkowski, A., Liao, H., Lee, S. P., Allen, M. H., Hull, P. R., Campbell, L. E., Trembath, R. C., Capon, F., Griffiths, C. E. M., Burden, D., McManus, R., Hughes, R., Kirby, B., Rogers, S. F., Fitzgerald, O., Kane, D., Barker, J. N. W. N., Palmer, C. N. A., ... Irwin McLean, W. H. (2007). Filaggrin null alleles are not associated with psoriasis. Journal of Investigative Dermatology, 127(8), 1878-1882. https://doi.org/10.1038/sj.jid.5700817

Zhao, Y, Terron-Kwiatkowski, A, Liao, H, Lee, SP, Allen, MH, Hull, PR, Campbell, LE, Trembath, RC, Capon, F, Griffiths, CEM, Burden, D, McManus, R, Hughes, R, Kirby, B, Rogers, SF, Fitzgerald, O, Kane, D, Barker, JNWN, Palmer, CNA, Irvine, AD & Irwin McLean, WH 2007, 'Filaggrin null alleles are not associated with psoriasis', Journal of Investigative Dermatology, vol. 127, n° 8, pp. 1878-1882. https://doi.org/10.1038/sj.jid.5700817

@article{731511316fc54d4ea65b1585a2215592,

title = "Filaggrin null alleles are not associated with psoriasis",

abstract = "Psoriasis is a common skin disease with an etiology consistent with a multifactorial trait. Several psoriasis susceptibility loci are known, a number of which are also implicated in a predisposition to atopic dermatitis (AD), including the epidermal differentiation complex on chromosome 1q21. It has recently been shown in several replicate studies that prevalent null alleles for the filaggrin gene (FLG) on 1q21 are an important genetic factor in AD. Here, we examined the role of these FLG variants in psoriasis using case:control association studies comparing Irish and UK psoriasis cohorts (combined n=691) to ethnically matched populations (combined n=2117). No association was present for the two common European FLG mutations R501X and 2282del4 (combined χ2 P=0.989). In addition, the 3′ end of the FLG open-reading frame was sequenced in a number of patients with differing types of psoriasis (plaque, guttate, palmoplantar, and late-onset), which excluded the possibility of a gain-of-function frameshift mutation such as those found in loricrin or certain keratin genes. These data suggest that FLG mutations are unlikely to be involved in genetic susceptibility to psoriasis and implies that there may be within-locus heterogeneity in chromosomal regions involved in both AD and psoriasis.",

author = "Yiwei Zhao and Ana Terron-Kwiatkowski and Haihui Liao and Lee, {Simon P.} and Allen, {Michael H.} and Hull, {Peter R.} and Campbell, {Linda E.} and Trembath, {Richard C.} and Francesca Capon and Griffiths, {Christopher E.M.} and David Burden and Ross McManus and Rosalind Hughes and Brian Kirby and Rogers, {Sarah F.} and Oliver Fitzgerald and David Kane and Barker, {Jonathan N.W.N.} and Palmer, {Colin N.A.} and Irvine, {Alan D.} and {Irwin McLean}, {W. H.}",

note = "Funding Information: We thank the patients and their families for their participation, which made this research possible. We also thank to Jayne Mcfarlane, Epithelial Genetics Group for clerical assistance. The Barker group was supported by The British Skin Foundation (N.J.R. and J.N.B.), The Wellcome Trust (R.C.T. and J.N.B.), and the Psoriasis Association (J.N.W.N.B, C.E.M.G., and D.B.). The McLean group is supported by grants from The Dystrophic Epidermolysis Bullosa Research Association, The Pachyonychia Congenita Project, the British Skin Foundation/National Eczema Society (W.H.I.M and Frances J.D. Smith). Filaggrin research in Dundee is supported by a donation from an anonymous family from Tayside, Scotland. The Palmer group is supported by the Biotechnology and Biological Sciences Research Council (award D13460), Scottish Enterprise Tayside and the Gannochy Trust, and the Scottish Executive Genetic Health Initiative. We acknowledge the following clinicians for their support: Louise Barnes and Rosemarie Watson, St James Hospital, Dublin; Paul Collins, Barry Bresnihan, and Doug Veale, St Vincent's University Hospital, Dublin.",

year = "2007",

month = aug,

doi = "10.1038/sj.jid.5700817",

language = "English",

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T1 - Filaggrin null alleles are not associated with psoriasis

AU - Zhao, Yiwei

AU - Terron-Kwiatkowski, Ana

AU - Liao, Haihui

AU - Lee, Simon P.

AU - Allen, Michael H.

AU - Hull, Peter R.

AU - Campbell, Linda E.

AU - Trembath, Richard C.

AU - Capon, Francesca

AU - Griffiths, Christopher E.M.

AU - Burden, David

AU - McManus, Ross

AU - Hughes, Rosalind

AU - Kirby, Brian

AU - Rogers, Sarah F.

AU - Fitzgerald, Oliver

AU - Kane, David

AU - Barker, Jonathan N.W.N.

AU - Palmer, Colin N.A.

AU - Irvine, Alan D.

AU - Irwin McLean, W. H.

N1 - Funding Information: We thank the patients and their families for their participation, which made this research possible. We also thank to Jayne Mcfarlane, Epithelial Genetics Group for clerical assistance. The Barker group was supported by The British Skin Foundation (N.J.R. and J.N.B.), The Wellcome Trust (R.C.T. and J.N.B.), and the Psoriasis Association (J.N.W.N.B, C.E.M.G., and D.B.). The McLean group is supported by grants from The Dystrophic Epidermolysis Bullosa Research Association, The Pachyonychia Congenita Project, the British Skin Foundation/National Eczema Society (W.H.I.M and Frances J.D. Smith). Filaggrin research in Dundee is supported by a donation from an anonymous family from Tayside, Scotland. The Palmer group is supported by the Biotechnology and Biological Sciences Research Council (award D13460), Scottish Enterprise Tayside and the Gannochy Trust, and the Scottish Executive Genetic Health Initiative. We acknowledge the following clinicians for their support: Louise Barnes and Rosemarie Watson, St James Hospital, Dublin; Paul Collins, Barry Bresnihan, and Doug Veale, St Vincent's University Hospital, Dublin.

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N2 - Psoriasis is a common skin disease with an etiology consistent with a multifactorial trait. Several psoriasis susceptibility loci are known, a number of which are also implicated in a predisposition to atopic dermatitis (AD), including the epidermal differentiation complex on chromosome 1q21. It has recently been shown in several replicate studies that prevalent null alleles for the filaggrin gene (FLG) on 1q21 are an important genetic factor in AD. Here, we examined the role of these FLG variants in psoriasis using case:control association studies comparing Irish and UK psoriasis cohorts (combined n=691) to ethnically matched populations (combined n=2117). No association was present for the two common European FLG mutations R501X and 2282del4 (combined χ2 P=0.989). In addition, the 3′ end of the FLG open-reading frame was sequenced in a number of patients with differing types of psoriasis (plaque, guttate, palmoplantar, and late-onset), which excluded the possibility of a gain-of-function frameshift mutation such as those found in loricrin or certain keratin genes. These data suggest that FLG mutations are unlikely to be involved in genetic susceptibility to psoriasis and implies that there may be within-locus heterogeneity in chromosomal regions involved in both AD and psoriasis.

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Filaggrin null alleles are not associated with psoriasis

Résumé

Note bibliographique

ASJC Scopus Subject Areas

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