Analysis of LAP+ and GARP+ Treg subsets in peripheral blood of patients with neuromyelitis optica spectrum disorders

Introduction Neuromyelitis optica spectrum disorder (NMOSD) is a group of antibody-mediated inflammatory demyelinating central nervous system diseases. T lymphocytes participate in NMOSD pathogenesis, with regulatory T cells (Treg) being the core in maintaining immune homeostasis. Studies have revea...

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Bibliographic Details
Published in:Neurological sciences 2023-05, Vol.44 (5), p.1739-1747
Main Authors: Cai, Haobing, Liu, Yu, Dong, Xiaohua, Jiang, Fei, Li, Hongliang, Ouyang, Song, Yin, Weifan, He, Ting, Zeng, Qiuming, Yang, Huan
Format: Article
Language:English
Subjects:
Autoimmune diseases
CD4 antigen
Central nervous system
Central nervous system diseases
Demyelination
Flow cytometry
Foxp3 protein
Glucocorticoids
Glucocorticoids - metabolism
Homeostasis
Humans
Immunoregulation
Inflammation
Interleukin 10
Lymphocytes T
Medicine
Medicine & Public Health
Neurology
Neuromyelitis
Neuromyelitis Optica
Neuroradiology
Neurosciences
Neurosurgery
Original Article
Peripheral blood
Psychiatry
T-Lymphocytes, Regulatory
Transforming Growth Factor beta1
Transforming growth factor-b1
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Summary:Introduction Neuromyelitis optica spectrum disorder (NMOSD) is a group of antibody-mediated inflammatory demyelinating central nervous system diseases. T lymphocytes participate in NMOSD pathogenesis, with regulatory T cells (Treg) being the core in maintaining immune homeostasis. Studies have revealed that different Treg subsets play different roles in autoimmune diseases. The distribution of LAP + or GARP + Treg subsets in NMOSD may help us deeply understand their immune mechanism. Methods This study reviewed 22 NMOSD patients and 20 normal controls. Flow cytometric analysis was utilized to detect subsets of Treg cells expressing Foxp3, Helios, LAP, or GARP in peripheral blood. ELISA was used to detect plasma TGF-β1 and IL-10. In addition, changes in the proportion of Treg cell subsets before and after glucocorticoid treatment in 10 patients were analyzed. Results Compared with healthy controls, LAP and GARP expressions were significantly downregulated in the peripheral blood of NMOSD patients. TGF-β1 expression in NMOSD patients was lower and was positively correlated with the ratio of CD4 + GARP + Treg cells. After treatment with glucocorticoid, LAP and GARP expressions in the peripheral blood of NMOSD patients were upregulated. Conclusions The proportion of Treg cells expressing LAP and GARP is downregulated, implying that Treg cells with the best inhibitory function are insufficient to maintain autoimmune homeostasis in NMOSD patients. Upregulation of Treg cells expressing LAP and GARP in NMOSD patients may be one of the mechanisms of glucocorticoid treatment.
ISSN:1590-1874
1590-3478
DOI:10.1007/s10072-023-06629-8