Neuraminidase 1 regulates the cellular state of microglia by modulating the sialylation of Trem2

神经氨酸酶1通过调节Trem2的唾液酸化来调控小胶质细胞的细胞状态。

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作者:Fremuth,Leigh Ellen,Hu,Huimin,van de Vlekkert,Diantha,Annunziata,Ida,Weesner,Jason Andrew,Gomero,Elida,d'Azzo,Alessandra
期刊:影响因子:
时间:2024起止号:2024 May 20
doi:10.1101/2024.05.20.595036研究方向: 信号转导细胞生物学
细胞类型: 胶质细胞

Abstract

Neuraminidase 1 (Neu1) cleaves terminal sialic acids from sialoglycoproteins in endolysosomes and at the plasma membrane. As such, Neu1 regulates immune cells, primarily those of the monocytic lineage. Here we examined how Neu1 influences microglia by modulating the sialylation of full-length Trem2 (Trem2-FL), a multifunctional receptor that regulates microglial survival, phagocytosis, and cytokine production. When Neu1 was deficient/downregulated, Trem2-FL remained sialylated, accumulated intracellularly, and was excessively cleaved into a C-terminal fragment (Trem2-CTF) and an extracellular soluble domain (sTrem2), enhancing their signaling capacities. Sialylated Trem2-FL (Sia-Trem2-FL) did not hinder Trem2-FL-DAP12-Syk complex assembly but impaired signal transduction through Syk, ultimately abolishing Trem2-dependent phagocytosis. Concurrently, Trem2-CTF-DAP12 complexes dampened NFκB signaling, while sTrem2 propagated Akt-dependent cell survival and NFAT1-mediated production of TNFα and CCL3. Because Neu1 and Trem2 are implicated in neurodegenerative/neuroinflammatory diseases, including Alzheimer disease (AD) and sialidosis, modulating Neu1 activity represents a therapeutic approach to broadly regulate microglia-mediated neuroinflammation.

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