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CD24-Siglec axis is an innate immune checkpoint against metaflammation and metabolic disorder

Xu Wang, Mingyue Liu, Jifeng Zhang, Nicholas K. Brown, Peng Zhang, Yan Zhang, Heng Liu, Xuexiang Du, Wei Wu, Martin Devenport, W Tao, Yang Mao‐Draayer, Guo‐Yun Chen, Y. Eugene Chen, Pan Zheng, Yang Liu

2022Cell Metabolism66 citationsDOIOpen Access PDF

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.

Topics & Concepts

Innate immune systemSIGLECImmune checkpointBiologyImmunologyImmune systemCell biologyImmunotherapyAdvanced Glycation End Products researchAtherosclerosis and Cardiovascular DiseasesBiomarkers in Disease Mechanisms
CD24-Siglec axis is an innate immune checkpoint against metaflammation and metabolic disorder | Litcius