| Literature DB >> 35279741 |
Mark G Lebwohl1, Emma Guttman-Yassky1, Hee J Kim2, Ester Del Duca1, Ana B Pavel1,3, Giselle K Singer1, Brian J Abittan1, Margot A Chima1, Grace Kimmel1, Jennifer Bares1, Danielle Baum1, Matthew Gagliotti1, Jordan Genece1, Justin Chu1.
Abstract
Improved repigmentation of generalized vitiligo in skin types IV-VI has been reported in clinical response to combined therapy with apremilast and narrowband (NB)-UVB; however, tissue responses to combined therapy versus NB-UVB monotherapy have not been elucidated. We compared the change from baseline in cellular and molecular markers in vitiligo skin after combined therapy versus NB-UVB monotherapy. We assessed lesional and nonlesional skin samples from enrolled subjects and evaluated for immune infiltrates, inflammatory, and melanogenesis-related markers which were compared across different treatment groups. Combined therapy resulted in significant reduction of CD8+T cells and CD11c+ dendritic cells, downregulation of PDE4B and Th17-related markers, and upregulation of melanogenesis markers. This study was limited to small sample size, skin types IV-VI, and high dropout rate. Our molecular findings support the clinical analysis that apremilast may potentiate NB-UVB in repigmentation of generalized vitiligo in skin types IV-VI.Entities:
Keywords: Anti-inflammatory; Apremilast; IFNγ pathway; Innate immune system; Narrowband UVB; Phosphodiesterase-4 inhibitor; Split-body study; Th17 axis; Vitiligo
Year: 2022 PMID: 35279741 DOI: 10.1007/s00403-022-02343-1
Source DB: PubMed Journal: Arch Dermatol Res ISSN: 0340-3696 Impact factor: 3.017