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低水平接触赭曲霉毒素A会导致帕金森症吗?

Can low level exposure to ochratoxin-A cause parkinsonism?

作者信息

Sava V, Reunova O, Velasquez A, Sanchez-Ramos J

机构信息

University of South Florida, Tampa, FL 33612, USA.

出版信息

J Neurol Sci. 2006 Nov 1;249(1):68-75. doi: 10.1016/j.jns.2006.06.006. Epub 2006 Jul 14.

DOI:10.1016/j.jns.2006.06.006
PMID:16844142
Abstract

Mycotoxins are fungal metabolites with pharmacological activities that have been utilized in the production of antibiotics, growth promoters, and other classes of drugs. Some mycotoxins have been developed as biological and chemical warfare agents. Bombs and ballistic missiles loaded with aflatoxin were stockpiled and may have been deployed by Iraq during the first Gulf War. In light of the excess incidence of amyotrophic lateral sclerosis (ALS) in veterans from Operation Desert Storm, the potential for delayed neurotoxic effects of low doses of mycotoxins should not be overlooked. Ochratoxin-A (OTA) is a common mycotoxin with complex mechanisms of action, similar to that of the aflatoxins. Acute administration of OTA at non-lethal doses (10% of the LD(50)) have been shown to increase oxidative DNA damage in brain up to 72 h, with peak effects noted at 24 h in midbrain (MB), caudate/putamen (CP) and hippocampus (HP). Levels of dopamine (DA) and its metabolites in the striatum (e.g., CP) were shown to be decreased in a dose-dependent manner. The present study focused on the effects of chronic low dose OTA exposure on regional brain oxidative stress and striatal DA metabolism. Continuous administration of low doses of OTA with implanted subcutaneous Alzet minipumps caused a small but significant decrease in striatal DA levels and an upregulation of anti-oxidative systems and DNA repair. It is possible that low dose exposure to OTA will result in an earlier onset of parkinsonism when normal age-dependent decline in striatal DA levels are superimposed on the mycotoxin-induced lesion.

摘要

霉菌毒素是具有药理活性的真菌代谢产物,已被用于生产抗生素、生长促进剂和其他各类药物。一些霉菌毒素已被开发为生物和化学战剂。装有黄曲霉毒素的炸弹和弹道导弹曾被储存,伊拉克在第一次海湾战争期间可能已部署过。鉴于参与“沙漠风暴行动”的退伍军人中肌萎缩侧索硬化症(ALS)发病率过高,低剂量霉菌毒素产生延迟神经毒性作用的可能性不容忽视。赭曲霉毒素A(OTA)是一种常见的霉菌毒素,其作用机制复杂,与黄曲霉毒素类似。非致死剂量(LD50的10%)的OTA急性给药已显示,在长达72小时内可增加大脑中的氧化性DNA损伤,中脑(MB)、尾状核/壳核(CP)和海马体(HP)在24小时时出现峰值效应。纹状体(如CP)中的多巴胺(DA)及其代谢产物水平呈剂量依赖性降低。本研究聚焦于慢性低剂量OTA暴露对局部脑氧化应激和纹状体DA代谢的影响。通过植入皮下的Alzet微型泵持续给予低剂量OTA,导致纹状体DA水平出现轻微但显著的下降,并使抗氧化系统和DNA修复上调。当纹状体DA水平随年龄正常下降叠加在霉菌毒素诱导的损伤上时,低剂量暴露于OTA可能会导致帕金森症更早发作。

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