Guselkumab treatment normalizes the stratum corneum ceramide profile and alleviates barrier dysfunction in psoriasis: results of a randomized controlled trial

The epidermal inflammation associated with psoriasis drives skin barrier perturbations. The skin barrier is primarily located in stratum corneum (SC). Its function depends on the SC lipid matrix of which ceramides constitute important components. Changes in the ceramide profile directly correlate to...

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Published inJournal of lipid research Vol. 65; no. 8; p. 100591
Main Authors Rousel, Jannik, Mergen, Catherine, Bergmans, Menthe E., Bruijnincx, Lisa J., de Kam, Marieke L., Klarenbeek, Naomi B., Niemeyer-van der Kolk, Tessa, van Doorn, Martijn B.A., Bouwstra, Joke A., Rissmann, Robert
Format Journal Article
LanguageEnglish
Published Elsevier Inc 01.08.2024
Subjects
Barrier
Ceramides
Clinical trials
Lipidomics
Psoriasis
Skin
Stratum Corneum
TEWL
PASI
AD
IL
Psoriasis
Clinical trials
Lipidomics
Barrier
MUCer
CCL
LSS
SC
DES
Ceramides
Skin
Stratum Corneum
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Summary:The epidermal inflammation associated with psoriasis drives skin barrier perturbations. The skin barrier is primarily located in stratum corneum (SC). Its function depends on the SC lipid matrix of which ceramides constitute important components. Changes in the ceramide profile directly correlate to barrier function. In this study, we characterized the dynamics of the barrier function and ceramide profile of psoriatic skin during anti-Interleukin-23 therapy with guselkumab. We conducted a double-blind, randomized controlled trial in which 26 mild-to-severe plaque psoriasis patients were randomization 3:1–100 mg guselkumab or placebo for 16 weeks and barrier dynamics monitored throughout. Barrier function was measured by trans-epidermal water loss measurements. Untargeted ceramide profiling was performed using liquid chromatography-mass spectrometry after SC was harvested using tape-stripping. The barrier function and ceramide profile of lesional skin normalized to that of controls during treatment with guselkumab, but not placebo. This resulted in significant differences compared to placebo at the end of the treatment. Changes in the lesional ceramide profile during treatment correlated with barrier function and target lesion severity. Nonlesional skin remained similar throughout treatment. Guselkumab therapy restored the skin barrier in psoriasis. Concomitant correlations between skin barrier function, the ceramide profile, and disease severity demonstrate their interdependency.
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ISSN:0022-2275
1539-7262
1539-7262
DOI:10.1016/j.jlr.2024.100591