Literature DB >> 36008138

KLF5 governs sphingolipid metabolism and barrier function of the skin.

Ying Lyu1, Yinglu Guan1, Lisa Deliu1, Ericka Humphrey1, Joanna K Frontera1, Youn Joo Yang1, Daniel Zamler1, Kun Hee Kim2, Vakul Mohanty1,3, Kevin Jin1,3, Vakul Mohanty1,3, Virginia Liu1,3, Jinzhuang Dou2, Lucas J Veillon2, Shwetha V Kumar2, Philip L Lorenzi2, Yang Chen1, Kathleen M McAndrews1, Sergei Grivennikov4,5, Xingzhi Song6, Jianhua Zhang6, Yuanxin Xi2, Jing Wang2, Ken Chen2, Priyadharsini Nagarajan7, Yejing Ge1.   

Abstract

Stem cells are fundamental units of tissue remodeling whose functions are dictated by lineage-specific transcription factors. Home to epidermal stem cells and their upward-stratifying progenies, skin relies on its secretory functions to form the outermost protective barrier, of which a transcriptional orchestrator has been elusive. KLF5 is a Krüppel-like transcription factor broadly involved in development and regeneration whose lineage specificity, if any, remains unclear. Here we report KLF5 specifically marks the epidermis, and its deletion leads to skin barrier dysfunction in vivo. Lipid envelopes and secretory lamellar bodies are defective in KLF5-deficient skin, accompanied by preferential loss of complex sphingolipids. KLF5 binds to and transcriptionally regulates genes encoding rate-limiting sphingolipid metabolism enzymes. Remarkably, skin barrier defects elicited by KLF5 ablation can be rescued by dietary interventions. Finally, we found that KLF5 is widely suppressed in human diseases with disrupted epidermal secretion, and its regulation of sphingolipid metabolism is conserved in human skin. Altogether, we established KLF5 as a disease-relevant transcription factor governing sphingolipid metabolism and barrier function in the skin, likely representing a long-sought secretory lineage-defining factor across tissue types.
© 2022 Lyu et al.; Published by Cold Spring Harbor Laboratory Press.

Entities:  

Keywords:  barrier; secretory; skin epidermis; sphingolipid metabolism; stem cells; transcription factors

Year:  2022        PMID: 36008138      PMCID: PMC9480852          DOI: 10.1101/gad.349662.122

Source DB:  PubMed          Journal:  Genes Dev        ISSN: 0890-9369            Impact factor:   12.890


  145 in total

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Authors:  Matteo Vietri Rudan; Ajay Mishra; Christian Klose; Ulrike S Eggert; Fiona M Watt
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