摘要
阿尔茨海默病是一种慢性神经退化性疾病,该疾病主要与β-淀粉样蛋白聚集,tau蛋白及神经炎症相关。人静脉输注免疫球蛋白(IVIG)是从成千上万的健康捐赠者中提取和聚集的多克隆抗体IgG 混合剂。作为治疗AD病的潜在药物,IVIG测试的科学原理包括其天然抗Aβ抗体活性、良好的安全性及其固有的抗炎或免疫调节特性。过去十年,一些临床与临床前实验结果增加了我们与AD 病治疗相关的IVIG生物治疗特性方面的知识。IVIG的抗淀粉体抗体显示了比Aβ单体明显高的淀粉样聚合物和纤维的结合亲和力。AD双转基因小鼠模型中,脑内注射IVIG 可以抑制Aβ纤维的病理形成,然而长期的外周IVIG治疗会引起全脑Aβ表达水平增加,对Aβ沉积物有着不可估量的影响,或者该治疗有脑内微出血的趋势。此外,长期的IVIG治疗会抑制神经炎症,培育成年性海马神经发生。在AD 病人的临床研究中,IVIG显示了可接受的安全性;还没有报道显示IVIG可以增加淀粉样成像相关异常的发生率。在对少数病人的初步研究中有报道其对轻度或者中度AD病人的临床效果。然而,随后的双盲,安慰剂对照研究并没能重复初步的实验结果。然而有趣的是,APOE4携带者和中度亚组病人被报道有阳性认知信号。不过,关于小鼠的临床和实验研究均显示IVIG的抗体可以聚集在中枢神经系统,它的生物活性包括Aβ低聚物的中合作用、神经炎症的抑制及其免疫调节。IVIG在细胞分子水平的识别介质效应得到认可。鉴于IVIG很好的安全性和前面提到的生物活性,它仍然是众多潜在的AD病治疗剂的实验研究候选者。
关键词: 阿尔茨海默病,β淀粉体,抗体,人体静脉输注免疫球蛋白,免疫球蛋白G唾液酸,免疫调节,小神经胶质,神经再生,神经炎症,低聚物
Current Alzheimer Research
Title:Intravenous Immunoglobulins for Alzheimer's Disease
Volume: 11 Issue: 7
Author(s): Lakshman Puli, Heikki Tanila and Norman Relkin
Affiliation:
关键词: 阿尔茨海默病,β淀粉体,抗体,人体静脉输注免疫球蛋白,免疫球蛋白G唾液酸,免疫调节,小神经胶质,神经再生,神经炎症,低聚物
摘要: Alzheimer’s disease (AD) is a chronic neurodegenerative disease associated with intracerebral accumulation of aggregated amyloid-beta (Aβ) and tau proteins, as well as neuroinflammation. Human intravenous immunoglobulin (IVIG) is a mixture of polyclonal IgG antibodies isolated and pooled from thousands of healthy human donors. The scientific rationale for testing IVIG as a potential AD treatment include its natural anti-Aβ antibody activity, its favorable safety profile and inherent anti-inflammatory/immunomodulatory properties. Over the past decade, several clinical and pre-clinical experimental findings, advanced our knowledge about biological and therapeutic properties of IVIG that are relevant to AD therapy. Anti-amyloid antibodies in IVIG show significantly higher binding avidity for amyloid oligomers and fibrils than for Aβ monomers. In a double transgenic murine model of AD, intracerebral injection of IVIG causes suppression of Aβ fibril pathology whereas long term peripheral IVIG treatments causes elevation of total brain Aβ levels with no measurable impact on Aβ deposits or tendency for inducing cerebral microhemmorhage. Furthermore, chronic IVIG treatment suppressed neuroinflammation and fostered adult hippocampal neurogenesis. In clinical studies with AD patients, IVIG showed an acceptable safety profile and has not been reported to increase the incidence of amyloid related imaging abnormalities. Preliminary studies on small number of patients reported clinical benefits in mild to moderate stage AD patients. However, double blind, placebo controlled studies later did not replicate those initial findings. Interestingly though, in APOE4 carriers and in moderate disease stage subgroups, positive cognitive signals were reported. Nevertheless, both clinical and experimental (mouse) studies show that antibodies in IVIG can accumulate in CNS and its biological activities include neutralization of Aβ oligomers, suppression of neuroinflammation and immunomodulation. Identifying mediators of IVIG’s effects at the cellular and molecular level is warranted. In light of its favourable safety profile and aforementioned biological properties, IVIG is still an enigmatic experimental candidate with enormous potential for being an AD therapeutic.
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Cite this article as:
Puli Lakshman, Tanila Heikki and Relkin Norman, Intravenous Immunoglobulins for Alzheimer's Disease, Current Alzheimer Research 2014; 11 (7) . https://dx.doi.org/10.2174/1567205011666140812113415
DOI https://dx.doi.org/10.2174/1567205011666140812113415 |
Print ISSN 1567-2050 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-5828 |
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