Transcriptomics

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Semaphorin 3E as a novel therapeutic target for neuropathic pain


ABSTRACT: We aimed to identify neuropathic pain (NP)-related immune semaphorins (SEMAs) and assess the efficacy of SEMA targeted therapy for NP. We quantified serum SEMA3A, 3E, 4A, 4D, and 7A in 45 patients with NP and 17 age- and sex-matched healthy controls (HCs) by enzyme-linked immunosorbent assay (ELISA). SEMA expression in DRG and peripheral nerve (PN) tissues of autopsied/biopsied patients with NP and controls as well as NP mouse model with partial sciatic nerve ligation (PSNL) was assessed by immunohistochemistry. Moreover, we intraperitoneally injected SEMA-blocking IgG or control IgG into PSNL-operated mice for 5 consecutive days immediately and 14 days after PSNL, and assessed mechanical hypersensitivity using von Frey filament on day 4 and 18 after PSNL. In vitro, we evaluated neurite outgrowth and the gene expression by RNA microarray analysis of mouse DRG neurons treated with or without SEMA3E. ELISA showed a significant increase of the SEMA3E in NP patients compared to HCs. Immunohistochemistry revealed enhanced SEMA3E expression in DRG and PN tissues of both NP patients and mouse model, especially in pro-inflammatory macrophages. SEMA3E-blocking IgG injection not only abolished the pro-inflammatory macrophage accumulation in PNs but also resolved hypersensitivity in PSNL-operated mice on both days 4 and 18. In vitro, SEMA3E treatment inhibited neurite outgrowth of DRG neurons accompanied with the upregulation of S100A9 which promotes neuroinflammation and downregulation of Dync1h1 that promote neurite outgrowth compared to non-treated DRG neurons. SEMA3E inhibition is a potential therapeutic strategy for NP via regulating neuroinflammation.

ORGANISM(S): Mus musculus

PROVIDER: GSE290407 | GEO | 2025/02/28

REPOSITORIES: GEO

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