Subclinical immune responses to nickel in sensitized individuals—a dose–response study

Author:

Wennervaldt Michael1ORCID,Vaher Helen2ORCID,Ahlström Malin G.1ORCID,Bischofberger Nuno2ORCID,Menné Torkil1,Thyssen Jacob P.1ORCID,Johansen Jeanne D.1ORCID,Bonefeld Charlotte M.2ORCID

Affiliation:

1. Department of Dermatology and Allergy, National Allergy Research Centre Copenhagen University Hospital Herlev‐Gentofte Hellerup Denmark

2. Department of Immunology and Microbiology, Faculty of Health and Medical Sciences, The LEO Foundation Skin Immunology Research Center University of Copenhagen Copenhagen Denmark

Abstract

AbstractBackgroundNickel is the leading cause of contact allergy in Europe, with 14.5% of the adult population being sensitized. Despite regulations limiting nickel release from consumer items, the incidence and prevalence of nickel allergy remain high.ObjectiveTo investigate the clinical and subclinical immune response to low‐dose nickel exposure on nickel pre‐exposed skin to assess the adequacy of current regulatory limits.MethodNickel‐allergic and healthy controls were patch tested with nickel twice with a 3–4 weeks interval. The first exposure used the diagnostic concentration of 2000 μg/cm2 nickel sulphate, and the same skin areas were then re‐exposed to 0.2, 0.5, 12.8 and 370 μg/cm2 nickel sulphate. After 48 h, the patch reactions were examined for clinical signs of eczema, and skin biopsies were collected. The transcriptomic immune profile was analysed with Nanostring nCounter and quantitative polymerase chain reaction.ResultsTwo nickel‐allergic participants (15%) had clinical reactions to the regulatory limiting doses for nickel (0.2/0.5 μg/cm2) following re‐exposure. There was immune activation in all skin areas following re‐exposure to nickel, predominantly mediated by up‐regulation of cytokines and chemokines. In all nickel re‐exposed skin areas, 81 genes were up‐regulated independent from the clinical response. In skin areas exposed to 0.2 μg/cm2, 101 immune‐related genes were differentially expressed, even when no clinical response was observed. Healthy controls showed up‐regulation of three genes in response to nickel re‐exposures without any clinical reactions.ConclusionImmune activation can be induced in skin with local memory to nickel upon challenge with nickel doses within the regulatory limits. Our findings suggest that the regulatory limits in the European nickel regulation may not provide sufficient protection for consumers against low‐dose exposures.

Funder

LEO Fondet

Kongelig Hofbuntmager Aage Bangs Fond

Miljø- og Fødevareministeriet

Publisher

Wiley

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