Biomarkers in atopic dermatitis

Publication date

2017-09-20

Authors

Thijs, Judith L.

Editors

Advisors

Supervisors

Bruijnzeel-Koomen, Carla A.ISNI 0000000043719227
Hijnen, D. J.ISNI 0000000395833381
Nierkens, StefanORCID 0000-0003-3406-817XISNI 0000000395421272

DOI

Document Type

Dissertation

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Abstract

Main findings of this thesis · A meta-analysis including 222 studies showed that serum TARC level is the best biomarker for disease severity currently available (chapter 2). · Immunoglobulin free light chains have been shown to correlate with disease severity in paediatric AD. However, they do not correlate with disease severity in adult AD (chapter 6). · A pilot study in 17 AD patients showed that a combination of serum biomarkers is better in assessing disease severity than a single biomarker (chapter 3). · In a prospective cohort of 200 patients it was shown that combining serum TARC, IL-22 and sIL-2R levels in an algorithm accurately predicts clinically measured disease severity (predicted EASI) in 90% of AD patient treated with topical steroids (chapter 4). · The p-EASI also predicts disease severity in patients treated with cyclosporin A (chapter 5). · The p-EASI offers an objective outcome measure for disease severity in prospective AD studies (chapter 4 and 5). Biomarkers enabling precision medicine in atopic dermatitis · High expression levels of circulating inflammatory biomarkers suggest that AD is a systemic disease. Recently described comorbidities may be the result of this systemic inflammation, and emphasize the need for a multidisciplinary approach for optimal management of AD and its comorbidities (chapter 9) · AD is a heterogeneous disease both clinically and biologically. We have identified four clusters of AD patients based on specific serum biomarker profiles, implying that each of these clusters is driven by a distinct underlying pathway and these clusters may represent different endotypes (chapter 7). · UGT1A9 polymorphisms can be used to identify patients with non-responsiveness to mycophenolic acid therapy, thereby showing the potential of pharmacodynamic biomarkers in AD (chapter 8). Improving practical aspects of biomarker measurement · The biomarkers studied in this thesis are measured in serum. However, multiple other sources for biomarker measurement exist, for instance saliva and dried blood spots (chapter 10). · A disadvantage of the use of serum biomarkers is the need for a venipuncture. TARC levels measured in dried blood spots also highly correlate with disease severity and significantly decrease during effective treatment. Therefore, dried blood spots may offer a simple and minimally invasive method for measurement of biomarkers in AD (chapter 11).

Keywords

atopic dermatitis, eczema, biomarkers, dried blood spots, endotypes, personalised medicine

Citation

Thijs, J L 2017, 'Biomarkers in atopic dermatitis', UMC Utrecht.