| Literature DB >> 35921817 |
Xu Wang1, Mingyue Liu1, Jifeng Zhang2, Nicholas K Brown3, Peng Zhang4, Yan Zhang5, Heng Liu1, Xuexiang Du6, Wei Wu7, Martin Devenport8, Weng Tao8, Yang Mao-Draayer9, Guo-Yun Chen10, Y Eugene Chen2, Pan Zheng11, Yang Liu12.
Abstract
The molecular interactions that regulate chronic inflammation underlying metabolic disease remain largely unknown. Since the CD24-Siglec interaction regulates inflammatory response to danger-associated molecular patterns (DAMPs), we have generated multiple mouse strains with single or combined mutations of Cd24 or Siglec genes to explore the role of the CD24-Siglec interaction in metaflammation and metabolic disorder. Here, we report that the CD24-Siglec-E axis, but not other Siglecs, is a key suppressor of obesity-related metabolic dysfunction. Inactivation of the CD24-Siglec-E pathway exacerbates, while CD24Fc treatment alleviates, diet-induced metabolic disorders, including obesity, dyslipidemia, insulin resistance, and nonalcoholic steatohepatitis (NASH). Mechanistically, sialylation-dependent recognition of CD24 by Siglec-E induces SHP-1 recruitment and represses metaflammation to protect against metabolic syndrome. A first-in-human study of CD24Fc (NCT02650895) supports the significance of this pathway in human lipid metabolism and inflammation. These findings identify the CD24-Siglec-E axis as an innate immune checkpoint against metaflammation and metabolic disorder and suggest a promising therapeutic target for metabolic disease.Entities:
Keywords: CD24; NASH; Siglec-E; Siglecs; insulin resistance; metabolic syndrome; metaflammation; obesity; sialic acid-binding immunoglobulin-like lectins; sialylation
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Year: 2022 PMID: 35921817 PMCID: PMC9393047 DOI: 10.1016/j.cmet.2022.07.005
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 31.373