Additive aluminum as a cause of induced immunoexcitoxicity resulting in neurodevelopmental and neurodegenerative disorders: A biochemical, pathophysiological, and pharmacological analysis

R. L. Blaylock
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Abstract

Much has been learned about the neurotoxicity of aluminum over the past several decades in terms of its ability to disrupt cellular function, result in slow accumulation, and the difficulty of its removal from cells. Newer evidence suggests a central pathophysiological mechanism may be responsible for much of the toxicity of aluminum and aluminofluoride compounds on the brain and spinal cord. This mechanism involves activation of the brain’s innate immune system, primarily the microglia, astrocytes, and macrophages, with a release of neurotoxic concentrations of excitotoxins and proinflammatory cytokines, chemokines, and immune mediators. Many studies suggest that excitotoxicity plays a significant role in the neurotoxic action of several metals, including aluminum. Recently, researchers have found that while most of the chronic pathology involved in the observed neurodegenerative effects of these metals are secondary to prolonged inflammation, it is the enhancement of excitotoxicity by the immune mediators that are responsible for most of the metal’s toxicity. This enhancement occurs through a crosstalk between cytokines and glutamate-related mechanisms. The author coined the name immunoexcitotoxicity to describe this process. This paper reviews the evidence linking immunoexcitotoxicity to aluminum’s neurotoxic effects and that a slow accumulation of aluminum may be the cause of neurodevelopmental defects as well as neurodegeneration in the adult.
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铝添加剂是导致神经发育和神经退行性疾病的免疫毒性诱因:生化、病理生理学和药理学分析
在过去的几十年中,人们对铝的神经毒性已经有了很多了解,包括铝扰乱细胞功能的能力、缓慢累积的结果以及从细胞中清除铝的难度。新的证据表明,铝和氟化铝化合物对大脑和脊髓的毒性可能是由一种核心病理生理机制造成的。这一机制涉及激活大脑的先天性免疫系统,主要是小胶质细胞、星形胶质细胞和巨噬细胞,释放出神经毒性浓度的兴奋性毒素和促炎细胞因子、趋化因子和免疫介质。许多研究表明,兴奋性毒性在包括铝在内的几种金属的神经毒性作用中起着重要作用。最近,研究人员发现,虽然在这些金属的神经退行性效应中观察到的大多数慢性病变都是继发于长期炎症,但免疫介质对兴奋毒性的增强才是金属毒性的主要原因。这种增强是通过细胞因子和谷氨酸相关机制之间的串联作用实现的。作者创造了免疫兴奋毒性这一名称来描述这一过程。本文回顾了将免疫兴奋毒性与铝的神经毒性效应联系起来的证据,以及铝的缓慢积累可能是神经发育缺陷和成人神经变性的原因。
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CiteScore
1.30
自引率
0.00%
发文量
623
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