Litcius/Paper detail

Sphingomyelin maintains the cutaneous barrier via regulation of the STAT3 pathway

Mariko Komuro, Masaki Nagane, Tomoki Fukuyama, Xiaolin Luo, Shinobu Hiraki, Masakatsu Miyanabe, Miyuki Ishikawa, Chiaki Niwa, Hironobu Murakami, Mariko Okamoto, Tadashi Yamashita

2022The FASEB Journal16 citationsDOIOpen Access PDF

Abstract

Epidermal tissues play vital roles in maintaining homeostasis and preventing the dysregulation of the cutaneous barrier. Sphingomyelin (SM), a sphingolipid synthesized by sphingomyelin synthase (SMS) 1 and 2, is involved in signal transduction via modulation of lipid-raft functions. Though the implications of SMS on inflammatory diseases have been reported, its role in dermatitis has not been clarified. In this study, we investigated the role of SM in the cutaneous barrier using a dermatitis model established by employing Sgms1 and 2 deficient mice. SM deficiency impaired the cutaneous inflammation and upregulated signal transducer and activator of transcription 3 (STAT3) phosphorylation in epithelial tissues. Furthermore, using mouse embryonic fibroblast cells, the sensitivity of STAT3 to Interleukin-6 stimulation was increased in Sgms-deficient cells. Using tofacitinib, a clinical JAK inhibitor, the study showed that SM deficiency might participate in STAT3 phosphorylation via JAK activation. Overall, these results demonstrate that SM is essential for maintaining the cutaneous barrier via the STAT3 pathway, suggesting SM could be a potential therapeutic target for dermatitis treatment.

Topics & Concepts

STAT3STAT proteinPhosphorylationActivator (genetics)SphingolipidSignal transductionChemistryCell biologyDownregulation and upregulationSphingomyelinInflammationCancer researchJanus kinaseCeramideHippo signaling pathwayTranscription factorKinaseEmbryonic stem cellAtopic dermatitisDermal fibroblastSphingolipid Metabolism and SignalingDermatology and Skin DiseasesAdvancements in Transdermal Drug Delivery