Secukinumab and Dead Sea Climatotherapy Impact Resolved Psoriasis Skin Differently Potentially Affecting Disease Memory.
Thomas EmmanuelBorislav IgnatovTrine BertelsenThomas LitmanMorten Muhlig NielsenMikkel Bo BrentToke TouborgAnders Benjamin RønsholdtAnnita PetersenMette BoyeIda KaaberDaniel SortebechDorte LybækTorben SteinicheAnne BregnhøjLiv EidsmoLars IversenClaus JohansenPublished in: International journal of molecular sciences (2024)
Secukinumab and Dead Sea treatment result in clear skin for many psoriasis patients, through distinct mechanisms. However, recurrence in the same areas after treatments suggests the existence of a molecular scar. We aimed to compare the molecular and genetic differences in psoriasis patients who achieved complete response from secukinumab and Dead Sea climatotherapy treatments. We performed quantitative immunohistochemical and transcriptomic analysis, in addition to digital spatial profiling of skin punch biopsies. Histologically, both treatments resulted in a normalization of the lesional skin to a level resembling nonlesional skin. Interestingly, the transcriptome was not normalized by either treatments. We revealed 479 differentially expressed genes between secukinumab and Dead Sea climatotherapy at the end of treatment, with a psoriasis panel identifying SERPINB4 , SERPINB13 , IL36G , IL36RN , and AKR1B10 as upregulated in Dead Sea climatotherapy compared with secukinumab. Using digital spatial profiling, pan-RAS was observed to be differentially expressed in the microenvironment surrounding CD103 + cells, and IDO1 was differentially expressed in the dermis when comparing the two treatments. The differences observed between secukinumab and Dead Sea climatotherapy suggest the presence of a molecular scar, which may stem from mechanistically different pathways and potentially contribute to disease recurrence. This may be important for determining treatment response duration and disease memory.
Keyphrases
- ankylosing spondylitis
- wound healing
- soft tissue
- single cell
- end stage renal disease
- genome wide
- chronic kidney disease
- ejection fraction
- rheumatoid arthritis
- stem cells
- gene expression
- induced apoptosis
- newly diagnosed
- working memory
- disease activity
- rna seq
- atopic dermatitis
- prognostic factors
- single molecule
- high resolution
- combination therapy
- cell death
- mass spectrometry