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Protective Effect of CXCR4 Antagonist CX807 in a Rat Model of Hemorrhagic Stroke

机译:CXCR4拮抗剂CX807在出血性卒中大鼠模型中的保护作用

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摘要

Intracerebral hemorrhage (ICH) is a major cause of stroke, with high mortality and morbidity. There is no effective pharmacological therapy for ICH. Previous studies have indicated that CXCR4 antagonists reduced microglia activation, attenuated infiltration of T cells, and improved functional recovery in ischemic stroke animals. The interaction of CXCR4 antagonists and ICH has not been characterized. The purpose of this study is to examine the neuroprotective action of a novel CXCR4 antagonist CX807 against ICH. In primary cortical neuronal and BV2 microglia co-culture, CX807 reduced glutamate-mediated neuronal loss and microglia activation. Adult rats were locally administered with collagenase VII to induce ICH. CX807 was given systemically after the ICH. Early post-treatment with CX807 improved locomotor activity in ICH rats. Brain tissues were collected for qRTPCR and histological staining. ICH upregulated the expression of CXCR4, CD8, TNFα, IL6, and TLR4. The immunoreactivity of IBA1 and CD8, as well as TUNEL labeling, were enhanced in the perilesioned area. CX807 significantly mitigated these responses. In conclusion, our data suggest that CX807 is neuroprotective and anti-inflammatory against ICH. CX807 may have clinical implications for the treatment of hemorrhagic stroke.
机译:脑出血(ICH)是中风的主要原因,死亡率和发病率高。对ICH没有有效的药理学疗法。以前的研究表明,CXCR4拮抗剂降低了微血花症活化,减弱T细胞的渗透,并改善了缺血性卒中动物的功能性回收。尚未表征CXCR4拮抗剂和ICH的相互作用。本研究的目的是检查新型CXCR4拮抗剂CX807对ICH的神经保护作用。在原发性皮质神经元和BV2微胶质植物共培养中,CX807降低了谷氨酸介导的神经元损失和微胶质增生活化。将成年大鼠用胶原酶VII局部施用,诱导ICH。 CX807在ICH后系统性地提供。用CX807提前治疗后治疗改善了ICH大鼠的运动活性。收集脑组织的QRTPCR和组织学染色。 ich上调CXCR4,CD8,TNFα,IL6和TLR4的表达。 IBA1和CD8的免疫反应性以及TUNEL标记在佩林区域的增强。 CX807显着减轻了这些反应。总之,我们的数据表明CX807是针对ICH的神经保护和抗炎。 CX807可能对治疗出血性卒中的临床意义。

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