Ageing Unit, IRCCS MultiMedica, Via G. Fantoli 16/15, 20138 Milan, Italy.
Department of Medicine, Surgery and Dentistry, "Scuola Medica Salernitana" University of Salerno, Via S. Allende, 84081 Baronissi (SA), Italy.
Eur Heart J. 2020 Jul 7;41(26):2487-2497. doi: 10.1093/eurheartj/ehz459.
Here, we aimed to determine the therapeutic effect of longevity-associated variant (LAV)-BPIFB4 gene therapy on atherosclerosis.
ApoE knockout mice (ApoE-/-) fed a high-fat diet were randomly allocated to receive LAV-BPIFB4, wild-type (WT)-BPIFB4, or empty vector via adeno-associated viral vector injection. The primary endpoints of the study were to assess (i) vascular reactivity and (ii) atherosclerotic disease severity, by Echo-Doppler imaging, histology and ultrastructural analysis. Moreover, we assessed the capacity of the LAV-BPIFB4 protein to shift monocyte-derived macrophages of atherosclerotic mice and patients towards an anti-inflammatory phenotype. LAV-BPIFB4 gene therapy rescued endothelial function of mesenteric and femoral arteries from ApoE-/- mice; this effect was blunted by AMD3100, a CXC chemokine receptor type 4 (CXCR4) inhibitor. LAV-BPIFB4-treated mice showed a CXCR4-mediated shift in the balance between Ly6Chigh/Ly6Clow monocytes and M2/M1 macrophages, along with decreased T cell proliferation and elevated circulating levels of interleukins IL-23 and IL-27. In vitro conditioning with LAV-BPIFB4 protein of macrophages from atherosclerotic patients resulted in a CXCR4-dependent M2 polarization phenotype. Furthermore, LAV-BPIFB4 treatment of arteries explanted from atherosclerotic patients increased the release of atheroprotective IL-33, while inhibiting the release of pro-inflammatory IL-1β, inducing endothelial nitric oxide synthase phosphorylation and restoring endothelial function. Finally, significantly lower plasma BPIFB4 was detected in patients with pathological carotid stenosis (>25%) and intima media thickness >2 mm.
Transfer of the LAV of BPIFB4 reduces the atherogenic process and skews macrophages towards an M2-resolving phenotype through modulation of CXCR4, thus opening up novel therapeutic possibilities in cardiovascular disease.
本研究旨在确定与长寿相关的变异体(LAV)-BPIFB4 基因治疗对动脉粥样硬化的治疗效果。
载脂蛋白 E 基因敲除(ApoE-/-)小鼠喂食高脂肪饮食,通过腺相关病毒载体注射随机分为接受 LAV-BPIFB4、野生型(WT)-BPIFB4 或空载体治疗组。研究的主要终点是通过回声多普勒成像、组织学和超微结构分析评估(i)血管反应性和(ii)动脉粥样硬化疾病严重程度。此外,我们评估了 LAV-BPIFB4 蛋白将动脉粥样硬化小鼠和患者来源的单核细胞衍生的巨噬细胞向抗炎表型转变的能力。LAV-BPIFB4 基因治疗可挽救 ApoE-/- 小鼠肠系膜和股动脉的内皮功能;这种作用被 CXCR4 抑制剂 AMD3100 减弱。LAV-BPIFB4 治疗的小鼠表现出 Ly6Chigh/Ly6Clow 单核细胞和 M2/M1 巨噬细胞之间平衡的 CXCR4 介导的转移,以及 T 细胞增殖减少和循环白细胞介素 IL-23 和 IL-27 水平升高。用 LAV-BPIFB4 蛋白对动脉粥样硬化患者的巨噬细胞进行体外条件处理,导致 CXCR4 依赖性 M2 极化表型。此外,LAV-BPIFB4 处理从动脉粥样硬化患者中提取的动脉增加了保护性 IL-33 的释放,同时抑制了促炎 IL-1β 的释放,诱导内皮型一氧化氮合酶磷酸化并恢复内皮功能。最后,在病理性颈动脉狭窄(>25%)和内膜中层厚度>2mm 的患者中检测到 BPIFB4 血浆水平明显降低。
BPIFB4 的 LAV 转移通过调节 CXCR4 减少动脉粥样硬化过程,并使巨噬细胞向 M2 缓解表型倾斜,从而为心血管疾病开辟新的治疗可能性。
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