Yu Chye Yun, Ng Gandi, Liao Ping
Calcium Signaling Laboratory, National Neuroscience Institute, 11 Jalan Tan Tock Seng, Singapore, 308433 Singapore.
Transl Stroke Res. 2013 Oct;4(5):477-83. doi: 10.1007/s12975-013-0281-2. Epub 2013 Aug 16.
Immunotherapy represents an active area of biomedical research to treat cancer, autoimmune diseases, and neurodegenerative disorders. In stroke, recanalization therapy is effective in reducing brain tissue damage after acute ischemic stroke. However, the narrow time window restricts its application for the majority of stroke patients. There is an urgent need to develop adjuvant therapies such as immunotherapy, stem cell replacement, and neuroprotective drugs. A number of molecules have been targeted for immunotherapy in stroke management, including myelin-associated proteins and their receptors, N-methyl-d-aspartic acid receptors, cytokines, and cell adhesion molecules. Both active vaccination and passive antibodies were tested in animal models of acute ischemic stroke. However, the mechanisms underlying the efficacy of immunotherapy are different for each target protein. Blocking myelin-associated proteins may enhance neuroplasticity, whereas blocking adhesion molecules may yield neuroprotection by suppressing the immune response after stroke. Although results from animal studies are encouraging, clinical trials using therapeutic antibodies failed to improve stroke outcome due to severe side effects. It remains a challenge to generate specific therapeutic antibodies with minimal side effects on other organs and systems.
免疫疗法是生物医学研究中治疗癌症、自身免疫性疾病和神经退行性疾病的一个活跃领域。在中风治疗中,再通疗法对减少急性缺血性中风后的脑组织损伤有效。然而,狭窄的时间窗限制了其在大多数中风患者中的应用。迫切需要开发免疫疗法、干细胞替代疗法和神经保护药物等辅助疗法。在中风治疗中,许多分子已成为免疫疗法的靶点,包括髓鞘相关蛋白及其受体、N-甲基-D-天冬氨酸受体、细胞因子和细胞黏附分子。主动疫苗接种和被动抗体均在急性缺血性中风动物模型中进行了测试。然而,每种靶蛋白的免疫疗法疗效背后的机制各不相同。阻断髓鞘相关蛋白可能增强神经可塑性,而阻断黏附分子可能通过抑制中风后的免疫反应产生神经保护作用。尽管动物研究结果令人鼓舞,但由于严重的副作用,使用治疗性抗体的临床试验未能改善中风预后。生成对其他器官和系统副作用最小的特异性治疗性抗体仍然是一项挑战。
