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有机磷诱导的迟发性神经病(OPIDN)中神经蛋白抗体及其改善情况。

Antibodies to neural proteins in organophosphorus-induced delayed neuropathy (OPIDN) and its amelioration.

作者信息

El-Fawal Hassan A N, McCain Wilfred C

机构信息

Neurotoxicology Laboratory, Division of Health Professions and Natural Sciences, Mercy College, Dobbs Ferry, NY 10522, USA.

出版信息

Neurotoxicol Teratol. 2008 May-Jun;30(3):161-6. doi: 10.1016/j.ntt.2008.01.005. Epub 2008 Feb 7.

Abstract

The development of OPIDN and the efficacy of experimental intervention using the calcium-channel blocker verapamil were used as a model to test the serial time-measurements of serum autoantibodies against neuronal cytoskeletal proteins [e.g., neurofilament triplet (NF)] and glial proteins [myelin-basic protein (MBP) and glial fibrillary-acidic protein (GFAP)] as biomarkers of neurotoxicity and its amelioration. Ten White Leghorn hens (>7 months, 1.2-1.8 kg) were administered phenyl-saligenin phosphate (PSP; 2.5 mg/kg; im), a dose reported to induce a 70% decrease in neurotoxic esterase (NTE) activity. Five of the hens were administered verapamil (7 mg/kg; im) for 4 days starting one day before PSP administration. Serum was isolated from blood collected by serial brachial venepuncture before PSP (day 0) administration and on days 3, 7 and 21 after PSP administration, each hen acting as its own control. Serum antibodies (IgG) to NF-L, NF-M, NF-H, MBP, and GFAP were assayed using an ELISA. There were no detectable levels of antibodies on days 0 and 3. IgG against all neural proteins were detected on days 7 and 21, with titer levels being significantly (p< or =0.05) higher in sera of hens receiving PSP only. Anti-NF-L titers were highest compared to those against NF-M, NF-H or MBP at 21 days. Titers of anti-NF-L and anti-MBP significantly (p< or =0.01) correlated with clinical scores at days 7 and 21. Detection of anti-NF and anti-MBP antibodies confirms the neuroaxonal degeneration accompanied by myelin loss reported in this model of OPIDN and the amelioration of neuropathy using verapamil. The detection of anti-GFAP antibodies suggests CNS involvement in OPIDN, since astrocytes are only found therein. This study demonstrates that detection of neuroantibodies can be used as biomarkers of neuropathy development and to monitor the amelioration resulting from therapeutic intervention. Together with biomarkers of exposure neuroantibodies can be used to monitor neuropathogenesis due to environmental or occupational exposures.

摘要

以有机磷酸酯诱导的迟发性神经病(OPIDN)的发展以及使用钙通道阻滞剂维拉帕米进行实验干预的效果为模型,来测试针对神经元细胞骨架蛋白[如神经丝三联体(NF)]和神经胶质蛋白[髓鞘碱性蛋白(MBP)和胶质纤维酸性蛋白(GFAP)]的血清自身抗体的连续时间测量,以此作为神经毒性及其改善情况的生物标志物。选用10只白来航鸡(>7个月,1.2 - 1.8千克),给予苯基水杨苷磷酸酯(PSP;2.5毫克/千克;肌肉注射),据报道该剂量可使神经毒性酯酶(NTE)活性降低70%。其中5只母鸡在给予PSP前一天开始,连续4天给予维拉帕米(7毫克/千克;肌肉注射)。在给予PSP前(第0天)以及给予PSP后的第3、7和21天,通过连续肱静脉穿刺采集血液,分离血清,每只母鸡自身作为对照。使用酶联免疫吸附测定法(ELISA)检测血清中针对NF-L、NF-M、NF-H、MBP和GFAP的抗体(IgG)。在第0天和第3天未检测到可检测水平的抗体。在第7天和第21天检测到针对所有神经蛋白的IgG,仅接受PSP的母鸡血清中的滴度水平显著更高(p≤0.05)。在第21天时,抗NF-L滴度相较于抗NF-M、NF-H或MBP的滴度最高。在第7天和第21天,抗NF-L和抗MBP的滴度与临床评分显著相关(p≤0.01)。抗NF和抗MBP抗体的检测证实了在该OPIDN模型中报道的伴有髓鞘丢失的神经轴突退变以及使用维拉帕米对神经病变的改善。抗GFAP抗体的检测表明中枢神经系统参与了OPIDN,因为星形胶质细胞仅存在于中枢神经系统中。本研究表明,神经抗体的检测可作为神经病变发展的生物标志物,并用于监测治疗干预所带来的改善情况。与接触生物标志物一起,神经抗体可用于监测由于环境或职业接触导致的神经病变发生过程。

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