Orexin B Reduces Cerebral Aneurysms by Inhibiting SP-1 via OX2R Activation
Background
Cerebral aneurysms (CAs) are dangerous dilations of intracranial arteries with a high rupture risk, leading to devastating outcomes. Current treatments often involve invasive procedures, and the underlying molecular mechanisms driving CA formation remain poorly understood, limiting pharmacological prevention strategies. The Orexin B/OX2R system, primarily known for its roles in arousal and metabolism, has recently been implicated in vascular pathology, presenting a novel avenue for investigation into CA pathogenesis and potential therapeutic targets.
Study Design
Researchers measured serum Orexin A and B levels in 38 CA patients and 43 healthy controls. A murine CA model was established using elastase-induced aneurysms in wild-type (WT) and OX2R knockout (OX2R-/-) mice. WT mice received Orexin B 30 μg/kg/day for 7 weeks, with controls receiving vehicle. Aneurysm size, inflammatory markers (IL-6, MMP-9, MCP-1, E-selectin), macrophage infiltration (CD68), and SP-1 expression were assessed. In vitro studies used human brain microvascular endothelial cells (HBMVECs) to examine Ang II-induced OX2R suppression, monocyte adhesion, and SP-1-mediated signaling.
Results
CA patients exhibited significantly reduced serum Orexin B levels (3.21 ± 0.52 pg/mL) compared to healthy controls (8.56 ± 1.23 pg/mL, p < 0.01), with no change in Orexin A. OX2R expression was downregulated in the circle of Willis of CA mice. Orexin B administration attenuated aneurysm formation in WT mice, reducing aneurysm size from 3.72 ± 0.469 mm to 1.93 ± 0.252 mm (p < 0.01). This protective effect was entirely absent in OX2R-/- mice. Orexin B suppressed the expression of inflammatory mediators (IL-6, MMP-9, MCP-1, E-selectin), reduced CD68+ macrophage infiltration, and decreased SP-1 levels in WT but not OX2R-/- mice. In HBMVECs, Ang II dose-dependently reduced OX2R expression.
Orexin B inhibited Ang II-induced monocyte adhesion and
SP-1-mediated pro-inflammatory signaling, effects that were abolished byOX2R siRNAorSP-1overexpression, confirming theOX2R/SP-1axis.
Key Findings
- CA patients showed significantly lower serum Orexin B levels (3.21 ± 0.52 pg/mL) compared to controls (8.56 ± 1.23 pg/mL, p < 0.01).
- Orexin B treatment (30 μg/kg/day) reduced aneurysm size in WT mice from 3.72 ± 0.469 mm to 1.93 ± 0.252 mm (p < 0.01).
- The protective effects of Orexin B were abolished in
OX2R-/-mice, confirmingOX2Rdependency. - Orexin B suppressed inflammatory mediators (
IL-6,MMP-9,MCP-1,E-selectin) andCD68+macrophage infiltration. - Orexin B inhibited
SP-1expression andSP-1-mediated pro-inflammatory signaling in endothelial cells.
Why It Matters
This study identifies Orexin B as a promising therapeutic candidate for cerebral aneurysm prevention or treatment, offering a novel anti-inflammatory mechanism via the OX2R/SP-1 pathway. The finding that Orexin B levels are reduced in CA patients suggests a potential biomarker for risk or disease progression. While preclinical, this research provides a strong rationale for exploring Orexin B or OX2R agonists in clinical settings, potentially as an adjunct to existing therapies or for individuals at high risk. Future protocols for CA management might consider Orexin B-based interventions to modulate inflammation and prevent aneurysm growth.
orexin-b
cerebral-aneurysm
inflammation
ox2r
sp-1
preclinical-animal