Publications

Publications, Books, Book Chapters and Reviews by Prof. Marcus Maurer, MD

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Long-term reduction in local inflammation by a lipid raft molecule in atopic dermatitis

Filename 100. Dölle et al,Long-term reduction in local,Allergy2010.pdf
Filesize 429.62 KB
Version o.100
Date added May 28, 2020
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Category Original Work
Authors Dölle, S., Hoser, D., Rasche, C., Loddenkemper, C., Maurer, M. Zuberbier, T., and Worm, M.
Citation Dölle, S., Hoser, D., Rasche, C., Loddenkemper, C., Maurer, M. Zuberbier, T., and Worm, M.: Long-term reduction in local inflammation by a lipid raft molecule in atopic dermatitis. Allergy 2010: 65; 1158-1165. IF: 6.29
Corresponding authors Worm, M.
DocNum O.100
DocType PDF
Edition; Page 65; 1158-1165
IF 6.29
Publisher Allergy
ReleaseDate 2010

Background: The complex pathogenesis of atopic dermatitis (AD) is guided by cell surface receptor-mediated signal transduction regulated in lipid rafts. Miltefosine isa raft-modulating  study, the clinical and immunomodulatory efficacy of miltefosine was investigated in patients with AD in comparison with a topical corticosteroid treatment.

Methods: Sixteen patients with AD were treated topically with miltefosine and hydrocortisone localized on representative AD target lesions for 3 weeks. To assess the clinical efficacy, the three item severity (TIS) score was evaluated before, during and after treatment as well as after 4-week-follow-up period. To study the antiinflammatory effect of miltefosine on the cellular T cell pattern, skin biopsies were analysed before and after treatment.

Results: The TIS score dropped in both groups significantly after treatment. A carry-over effect was exclusively seen for miltefosine after discontinuing the treatment. These findings were substantiated by thermographic imaging with a significant decrease in the maximum temperature (Tmax) after miltefosine application (P = 0.034, DTmax = 1.7C [2.1–3.9]). Immunohistochemically, a reduction in lesional CD4+-infiltrating T cells was observed in both treatments. Moreover, increased FoxP3+ cells were present in the skin after miltefosine treatment (before 5.4% [1.9–9.8], after 6.2% [3.5–9.5]).

Conclusion: We demonstrate that miltefosine is locally active in patients with AD and led to a sustained clinical improvement in local skin inflammation. Moreover, the increased frequency of FoxP3+ cells in the skin of patients with AD suggests its immunomodulatory properties.

 

(Last update: 09.2024)

Number of original publications in peer-reviewed journals:626
Number of reviews in peer-reviewed journals:221
Number of publications (original work and reviews) in peer-reviewed journals:847
Cumulative IF for original publications in peer-reviewed journals:4432.59
Cumulative IF for reviews in peer-reviewed journals:1648.22
Cumulative IF of publications (original work & reviews) in peer-reviewed journals:6080.81
Total number of citations: 38,608, h-index: 99 (Web of Science September 2024)38,608

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