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Cooling and immunomodulation for treating hypoxic-ischemic brain injury

机译:治疗缺氧缺血性脑损伤的冷却和免疫调节

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摘要

Therapeutic hypothermia is now well established to partially reduce disability in term and near-term infants with moderate-severe hypoxic-ischemic encephalopathy. Preclinical and clinical studies have confirmed that current protocols for therapeutic hypothermia are near optimal. The challenge is now to identify complementary therapies that can further improve outcomes, in combination with therapeutic hypothermia. Overall, anti-excitatory and anti-apoptotic agents have shown variable or even no benefit in combination with hypothermia, suggesting overlapping mechanisms of neuroprotection. Inflammation appears to play a critical role in the pathogenesis of injury in the neonatal brain, and thus, there is potential for drugs with immunomodulatory properties that target inflammation to be used as a therapy in neonates. In this review, we examine the evidence for neuroprotection with immunomodulation after hypoxia-ischemia. For example, stem cell therapy can reduce inflammation, increase cell survival, and promote cell maturation and repair. There are also encouraging preclinical data from small animals suggesting that stem cell therapy can augment hypothermic neuroprotection. However, there is conflicting evidence, and rigorous testing in translational animal models is now needed.
机译:治疗性低温现已被广泛用于部分降低中重度缺氧缺血性脑病足月儿和近足月儿的残疾。临床前和临床研究已经证实,目前治疗性低温的方案接近最佳。目前面临的挑战是,结合治疗性低温,找出能够进一步改善预后的补充疗法。总的来说,抗兴奋性和抗凋亡药物在与低温结合时表现出不同甚至没有益处,这表明神经保护机制重叠。炎症似乎在新生儿脑损伤的发病机制中起着关键作用,因此,针对炎症的具有免疫调节特性的药物有可能用于新生儿的治疗。在这篇综述中,我们研究了缺氧缺血后通过免疫调节进行神经保护的证据。例如,干细胞疗法可以减少炎症,提高细胞存活率,促进细胞成熟和修复。还有来自小动物的令人鼓舞的临床前数据表明,干细胞疗法可以增强低温神经保护。然而,有相互矛盾的证据,现在需要在翻译动物模型中进行严格的测试。

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