NLRP3 inflammasome inhibition protects against intracranial aneurysm rupture and alters the phenotype of infiltrating macrophages

W. Dodd, Devan Patel, K. Motwani, B. Lucke-Wold, K. Hosaka, B. Hoh
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Abstract

Aneurysmal subarachnoid hemorrhage is a devastating cerebrovascular disease associated with high morbidity and mortality. Macrophage-mediated mural inflammation is a key pathogenic component contributing to aneurysm rupture.To investigate the effect of pharmacological inhibition of the NLRP3 inflammasome on aneurysm rupture.Cerebral aneurysms were induced in C57BL/6 mice with a combination of hypertension and an intracranial dose of elastase. Mice were treated with either 40 mg/kg of MCC950 or saline via intraperitoneal injections. Vascular tissue at the circle of Willis was harvested for analysis via immunofluorescent microscopy or qPCR.NLRP3+ cells are more common in the aneurysm tissue compared to the normal cerebral vasculature. The mRNA expression of the downstream NLRP3 pathway components caspase-1, IL-1β, and GSDMD is also increased in the aneurysm tissue compared to healthy vessels. There was no difference in the aneurysm formation rate between MCC950- and vehicle-treated mice; however, MCC950 treatment significantly reduced aneurysm rupture rate. There was no difference in systemic blood pressure between both groups. MCC950 treatment also extended the symptom-free survival of mice after aneurysm induction. Mechanistically, NLRP3 inhibition decreased the phenotype polarization of infiltrating macrophages without affecting the total number of macrophages in the vessel wall.Our results indicate that the NLRP3 inflammasome contributes to aneurysm rupture and macrophage polarization within the vessel wall. The NLRP3 pathway is a promising therapeutic target for the development of therapeutics to prevent aneurysmal hemorrhagic stroke.
NLRP3炎性小体抑制可防止颅内动脉瘤破裂并改变浸润性巨噬细胞的表型
动脉瘤性蛛网膜下腔出血是一种高发病率和死亡率的破坏性脑血管疾病。巨噬细胞介导的壁面炎症是导致动脉瘤破裂的关键致病因素。探讨药物抑制NLRP3炎性体对动脉瘤破裂的影响。C57BL/6小鼠在高压和大剂量弹性蛋白酶联合作用下诱发脑动脉瘤。小鼠分别腹腔注射40 mg/kg的MCC950或生理盐水。收集威利斯环的维管组织,通过免疫荧光显微镜或qPCR进行分析。与正常的脑血管系统相比,NLRP3+细胞在动脉瘤组织中更为常见。与健康血管相比,动脉瘤组织中下游NLRP3通路成分caspase-1、IL-1β和GSDMD的mRNA表达也增加。MCC950与载药处理小鼠的动脉瘤形成率无差异;MCC950治疗可显著降低动脉瘤破裂率。两组之间的全身血压没有差异。MCC950治疗也延长了动脉瘤诱导后小鼠的无症状生存期。在机制上,NLRP3抑制降低了浸润性巨噬细胞的表型极化,但不影响血管壁巨噬细胞总数。我们的研究结果表明,NLRP3炎性体有助于动脉瘤破裂和血管壁内巨噬细胞极化。NLRP3通路是开发预防动脉瘤性出血性卒中治疗方法的一个有希望的治疗靶点。
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