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Interplay of filaggrin loss-of-function variants, allergic sensitization, and eczema in a longitudinal study covering infancy to 18 years of age

Interplay of filaggrin loss-of-function variants, allergic sensitization, and eczema in a longitudinal study covering infancy to 18 years of age
Interplay of filaggrin loss-of-function variants, allergic sensitization, and eczema in a longitudinal study covering infancy to 18 years of age
Background

Immune specific genes as well as genes regulating the formation of skin barrier are major determinants for eczema manifestation. There is a debate as to whether allergic sensitization and filaggrin gene (FLG) variants lead to eczema or FLG variants and eczema increase the risk of allergic sensitization. To investigate the time-order between eczema and allergic sensitization with respect to FLG variants, data from a large prospective study covering infancy to late adolescence were analyzed.

Methodology/Principal Findings
Repeated measurements of eczema and allergic sensitization (documented by skin prick tests) at ages 1, 2, 4, 10, and 18 years were ascertained in the Isle of Wight birth cohort (n = 1,456). Three transition periods were analyzed: age 1-or-2 to 4, 4 to 10, and 10 to 18 years. FLG variants were genotyped in 1,150 participants. Over the three transition periods, in temporal sequence analyses of initially eczema-free participants, the combined effect of FLG variants and allergic sensitization showed a 2.92-fold (95% CI: 1.47–5.77) increased risk ratio (RR) of eczema in subsequent examinations. This overall risk was more pronounced at a younger age (transition period 1-or-2 to 4, RR = 6.47, 95% CI: 1.96–21.33). In contrast, FLG variants in combination with eczema showed a weaker, but significant, risk ratio for subsequent allergic sensitization only up to 10 years of age.

Conclusions/Significance
Taking the time order into account, this prospective study demonstrates for the first time, that a combination of FLG variants and allergic sensitization increased the risk of eczema in subsequent years. Also FLG variants interacted with eczema and increased the risk of subsequent allergic sensitization, which, was limited to the younger age. Hence, early restoration of defective skin barrier could prevent allergic sensitization and subsequently reduce the risk of eczema development.

1932-6203
e32721
Ziyab, Ali H.
12905e44-3fd1-47c2-98e5-35320e89815b
Karmaus, Wilfried
281d0e53-6b5d-4d38-9732-3981b07cd853
Yousefi, Mitra
9d5d6aa8-bba4-40b0-861e-0b60ceaea587
Ewart, Susan
28667421-3cf7-43d7-b1c3-ca27564938f7
Schauberger, Eric
465a4658-a065-470e-b7dc-0b713f911922
Holloway, John W.
4bbd77e6-c095-445d-a36b-a50a72f6fe1a
Zhang, Hongmei
9f774048-54d6-4321-a252-3887b2c76db0
Arshad, Syed Hasan
917e246d-2e60-472f-8d30-94b01ef28958
Ziyab, Ali H.
12905e44-3fd1-47c2-98e5-35320e89815b
Karmaus, Wilfried
281d0e53-6b5d-4d38-9732-3981b07cd853
Yousefi, Mitra
9d5d6aa8-bba4-40b0-861e-0b60ceaea587
Ewart, Susan
28667421-3cf7-43d7-b1c3-ca27564938f7
Schauberger, Eric
465a4658-a065-470e-b7dc-0b713f911922
Holloway, John W.
4bbd77e6-c095-445d-a36b-a50a72f6fe1a
Zhang, Hongmei
9f774048-54d6-4321-a252-3887b2c76db0
Arshad, Syed Hasan
917e246d-2e60-472f-8d30-94b01ef28958

Ziyab, Ali H., Karmaus, Wilfried, Yousefi, Mitra, Ewart, Susan, Schauberger, Eric, Holloway, John W., Zhang, Hongmei and Arshad, Syed Hasan (2012) Interplay of filaggrin loss-of-function variants, allergic sensitization, and eczema in a longitudinal study covering infancy to 18 years of age. PLoS ONE, 7 (3), e32721. (doi:10.1371/journal.pone.0032721). (PMID:22403702)

Record type: Article

Abstract

Background

Immune specific genes as well as genes regulating the formation of skin barrier are major determinants for eczema manifestation. There is a debate as to whether allergic sensitization and filaggrin gene (FLG) variants lead to eczema or FLG variants and eczema increase the risk of allergic sensitization. To investigate the time-order between eczema and allergic sensitization with respect to FLG variants, data from a large prospective study covering infancy to late adolescence were analyzed.

Methodology/Principal Findings
Repeated measurements of eczema and allergic sensitization (documented by skin prick tests) at ages 1, 2, 4, 10, and 18 years were ascertained in the Isle of Wight birth cohort (n = 1,456). Three transition periods were analyzed: age 1-or-2 to 4, 4 to 10, and 10 to 18 years. FLG variants were genotyped in 1,150 participants. Over the three transition periods, in temporal sequence analyses of initially eczema-free participants, the combined effect of FLG variants and allergic sensitization showed a 2.92-fold (95% CI: 1.47–5.77) increased risk ratio (RR) of eczema in subsequent examinations. This overall risk was more pronounced at a younger age (transition period 1-or-2 to 4, RR = 6.47, 95% CI: 1.96–21.33). In contrast, FLG variants in combination with eczema showed a weaker, but significant, risk ratio for subsequent allergic sensitization only up to 10 years of age.

Conclusions/Significance
Taking the time order into account, this prospective study demonstrates for the first time, that a combination of FLG variants and allergic sensitization increased the risk of eczema in subsequent years. Also FLG variants interacted with eczema and increased the risk of subsequent allergic sensitization, which, was limited to the younger age. Hence, early restoration of defective skin barrier could prevent allergic sensitization and subsequently reduce the risk of eczema development.

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Published date: 5 March 2012
Organisations: Human Development & Health, Clinical & Experimental Sciences

Identifiers

Local EPrints ID: 336323
URI: http://eprints.soton.ac.uk/id/eprint/336323
ISSN: 1932-6203
PURE UUID: 69a34578-9e61-410c-828f-04547e4f3f9e
ORCID for John W. Holloway: ORCID iD orcid.org/0000-0001-9998-0464

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Date deposited: 22 Mar 2012 10:06
Last modified: 15 Mar 2024 02:56

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Contributors

Author: Ali H. Ziyab
Author: Wilfried Karmaus
Author: Mitra Yousefi
Author: Susan Ewart
Author: Eric Schauberger
Author: Hongmei Zhang

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