Department of Pharmacology, University of Florence, Italy.
J Neuroinflammation. 2011 Apr 12;8:31. doi: 10.1186/1742-2094-8-31.
Permanent functional deficits following spinal cord injury (SCI) arise both from mechanical injury and from secondary tissue reactions involving inflammation. Enhanced release of adenosine and glutamate soon after SCI represents a component in the sequelae that may be responsible for resulting functional deficits. The role of adenosine A2A receptor in central ischemia/trauma is still to be elucidated. In our previous studies we have demonstrated that the adenosine A2A receptor-selective agonist CGS21680, systemically administered after SCI, protects from tissue damage, locomotor dysfunction and different inflammatory readouts. In this work we studied the effect of the adenosine A2A receptor antagonist SCH58261, systemically administered after SCI, on the same parameters. We investigated the hypothesis that the main action mechanism of agonists and antagonists is at peripheral or central sites.
Spinal trauma was induced by extradural compression of SC exposed via a four-level T5-T8 laminectomy in mouse. Three drug-dosing protocols were utilized: a short-term systemic administration by intraperitoneal injection, a chronic administration via osmotic minipump, and direct injection into the spinal cord.
SCH58261, systemically administered (0.01 mg/kg intraperitoneal. 1, 6 and 10 hours after SCI), reduced demyelination and levels of TNF-α, Fas-L, PAR, Bax expression and activation of JNK mitogen-activated protein kinase (MAPK) 24 hours after SCI. Chronic SCH58261 administration, by mini-osmotic pump delivery for 10 days, improved the neurological deficit up to 10 days after SCI. Adenosine A2A receptors are physiologically expressed in the spinal cord by astrocytes, microglia and oligodendrocytes. Soon after SCI (24 hours), these receptors showed enhanced expression in neurons. Both the A2A agonist and antagonist, administered intraperitoneally, reduced expression of the A2A receptor, ruling out the possibility that the neuroprotective effects of the A2A agonist are due to A2A receptor desensitization. When the A2A antagonist and agonist were centrally injected into injured SC, only SCH58261 appeared neuroprotective, while CGS21680 was ineffective.
Our results indicate that the A2A antagonist protects against SCI by acting on centrally located A2A receptors. It is likely that blockade of A2A receptors reduces excitotoxicity. In contrast, neuroprotection afforded by the A2A agonist may be primarily due to peripheral effects.
脊髓损伤(SCI)后的永久性功能缺陷既来自机械损伤,也来自涉及炎症的继发性组织反应。SCI 后不久,腺苷和谷氨酸的大量释放是可能导致功能缺陷的后续事件的一个组成部分。腺苷 A2A 受体在中枢缺血/创伤中的作用仍有待阐明。在我们之前的研究中,我们已经证明,在 SCI 后系统给予的腺苷 A2A 受体选择性激动剂 CGS21680 可防止组织损伤、运动功能障碍和不同的炎症反应。在这项工作中,我们研究了在 SCI 后系统给予腺苷 A2A 受体拮抗剂 SCH58261 对相同参数的影响。我们假设激动剂和拮抗剂的主要作用机制是在周围或中枢部位。
通过在 T5-T8 椎管水平进行的 4 级椎板切除术暴露的 SCI ,通过硬膜外压迫诱导脊髓创伤。利用了三种药物给药方案:腹腔内注射的短期全身给药、通过渗透微型泵的慢性给药和直接脊髓内注射。
SCH58261(0.01mg/kg 腹腔内注射,SCI 后 1、6 和 10 小时)可减少 SCI 后 24 小时的脱髓鞘和 TNF-α、Fas-L、PAR、Bax 表达水平,并激活 JNK 丝裂原活化蛋白激酶(MAPK)。通过微型渗透泵输送 10 天的慢性 SCH58261 给药可改善 SCI 后 10 天的神经功能缺损。SCI 后不久(24 小时),这些受体在神经元中表现出增强的表达。腹腔内给予腺苷 A2A 激动剂和拮抗剂均可降低 A2A 受体的表达,排除了 A2A 激动剂的神经保护作用是由于 A2A 受体脱敏的可能性。当 A2A 拮抗剂和激动剂被注入受伤的脊髓时,只有 SCH58261 表现出神经保护作用,而 CGS21680 则无效。
我们的结果表明,A2A 拮抗剂通过作用于中枢 A2A 受体来保护 SCI。阻断 A2A 受体可能会减少兴奋性毒性。相比之下,A2A 激动剂提供的神经保护作用可能主要归因于外周效应。
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