Neuron-specific SALM5 limits inflammation in the CNS via its interaction with HVEM | Zendy

Yuwen Zhu | Zendy; Sheng Yao | Zendy; Mathew M. Augustine | Zendy; Haiying Xu | Zendy; Jun Wang | Zendy; Jingwei Sun | Zendy; Megan Broadwater | Zendy; William Ruff | Zendy; Liqun Luo | Zendy; Gefeng Zhu | Zendy; Koji Tamada | Zendy; Lieping Chen | Zendy

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Neuron-specific SALM5 limits inflammation in the CNS via its interaction with HVEM

Author(s) -

Yuwen Zhu,

Sheng Yao,

Mathew M. Augustine,

Haiying Xu,

Jun Wang,

Jingwei Sun,

Megan Broadwater,

William Ruff,

Liqun Luo,

Gefeng Zhu,

Koji Tamada,

Lieping Chen

Publication year - 2016

Publication title -

science advances

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 5.928

H-Index - 146

ISSN - 2375-2548

DOI - 10.1126/sciadv.1500637

Subject(s) - inflammation , immune system , immune privilege , neuroscience , neuron , biology , immunology

The central nervous system (CNS) is an immune-privileged organ with the capacity to prevent excessive inflammation. Aside from the blood-brain barrier, active immunosuppressive mechanisms remain largely unknown. We report that a neuron-specific molecule, synaptic adhesion-like molecule 5 (SALM5), is a crucial contributor to CNS immune privilege. We found that SALM5 suppressed lipopolysaccharide-induced inflammatory responses in the CNS and that a SALM-specific monoclonal antibody promoted inflammation in the CNS, and thereby aggravated clinical symptoms of mouse experimental autoimmune encephalomyelitis. In addition, we identified herpes virus entry mediator as a functional receptor that mediates SALM5's suppressive function. Our findings reveal a molecular link between the neuronal system and the immune system, and provide potential therapeutic targets for the control of CNS diseases.

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