Department of Internal Medicine, Washington University School of Medicine, 660 S, Euclid Ave, St. Louis, MO 63110, USA.
J Neuroinflammation. 2011 Dec 6;8:170. doi: 10.1186/1742-2094-8-170.
Multiple Sclerosis (MS) is characterized by the pathological trafficking of leukocytes into the central nervous system (CNS). Using the murine MS model, experimental autoimmune encephalomyelitis (EAE), we previously demonstrated that antagonism of the chemokine receptor CXCR7 blocks endothelial cell sequestration of CXCL12, thereby enhancing the abluminal localization of CXCR4-expressing leukocytes. CXCR7 antagonism led to decreased parenchymal entry of leukocytes and amelioration of ongoing disease during EAE. Of note, animals that received high doses of CXCR7 antagonist recovered to baseline function, as assessed by standard clinical scoring. Because functional recovery reflects axonal integrity, we utilized diffusion tensor imaging (DTI) to evaluate axonal injury in CXCR7 antagonist- versus vehicle-treated mice after recovery from EAE.
C57BL6/J mice underwent adoptive transfer of MOG-reactive Th1 cells and were treated daily with either CXCR7 antagonist or vehicle for 28 days; and then evaluated by DTI to assess for axonal injury. After imaging, spinal cords underwent histological analysis of myelin and oligodendrocytes via staining with luxol fast blue (LFB), and immunofluorescence for myelin basic protein (MBP) and glutathione S-transferase-π (GST-π). Detection of non-phosphorylated neurofilament H (NH-F) was also performed to detect injured axons. Statistical analysis for EAE scores, DTI parameters and non-phosphorylated NH-F immunofluorescence were done by ANOVA followed by Bonferroni post-hoc test. For all statistical analysis a p < 0.05 was considered significant.
In vivo DTI maps of spinal cord ventrolateral white matter (VLWM) axial diffusivities of naïve and CXCR7 antagonist-treated mice were indistinguishable, while vehicle-treated animals exhibited decreased axial diffusivities. Quantitative differences in injured axons, as assessed via detection of non-phosphorylated NH-F, were consistent with axial diffusivity measurements. Overall, qualitative myelin content and presence of oligodendrocytes were similar in all treatment groups, as expected by their radial diffusivity values. Quantitative assessment of persistent inflammatory infiltrates revealed significant decreases within the parenchyma of CXCR7 antagonist-treated mice versus controls.
These data suggest that CXCR7 antagonism not only prevents persistent inflammation but also preserves axonal integrity. Thus, targeting CXCR7 modifies both disease severity and recovery during EAE, suggesting a role for this molecule in both phases of disease.
多发性硬化症(MS)的特征是白细胞病理性地进入中枢神经系统(CNS)。我们之前使用实验性自身免疫性脑脊髓炎(EAE)的小鼠 MS 模型证明,趋化因子受体 CXCR7 的拮抗作用阻止了 CXCL12 在内皮细胞中的隔离,从而增强了表达 CXCR4 的白细胞的管腔下定位。CXCR7 拮抗作用导致白细胞实质内进入减少,并在 EAE 期间改善进行性疾病。值得注意的是,接受高剂量 CXCR7 拮抗剂的动物恢复到基线功能,如通过标准临床评分评估。由于功能恢复反映轴突完整性,我们利用弥散张量成像(DTI)评估 EAE 恢复后 CXCR7 拮抗剂与载体处理的小鼠中的轴突损伤。
C57BL6/J 小鼠接受 MOG 反应性 Th1 细胞的过继转移,并每天接受 CXCR7 拮抗剂或载体治疗 28 天;然后通过 DTI 评估以评估轴突损伤。成像后,通过用卢索快速蓝(LFB)染色对髓鞘和少突胶质细胞进行脊髓的组织学分析,以及对髓鞘碱性蛋白(MBP)和谷胱甘肽 S-转移酶-π(GST-π)进行免疫荧光染色。还检测了非磷酸化神经丝 H(NH-F)的存在以检测受损的轴突。通过方差分析(ANOVA)后进行 Bonferroni 事后检验,对 EAE 评分、DTI 参数和非磷酸化 NH-F 免疫荧光的统计分析。对于所有统计分析,p <0.05 被认为具有统计学意义。
在体内 DTI 图中,幼稚和 CXCR7 拮抗剂处理的小鼠的脊髓腹外侧白质(VLWM)轴向扩散率没有区别,而载体处理的动物则表现出轴向扩散率降低。通过检测非磷酸化 NH-F 评估的受损轴突的定量差异与轴向扩散率测量结果一致。总的来说,所有治疗组的髓鞘含量和少突胶质细胞的存在都相似,这与它们的径向扩散率值一致。定量评估持续的炎症浸润显示 CXCR7 拮抗剂处理的小鼠与对照组相比,实质内的浸润明显减少。
这些数据表明,CXCR7 拮抗作用不仅可以防止持续的炎症,还可以保持轴突完整性。因此,靶向 CXCR7 不仅改变了 EAE 期间的疾病严重程度和恢复,而且还提示该分子在疾病的两个阶段都有作用。
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