Objective To investigate the role of myelin protein zero (P 0) in 2,5-hexanedione (2,5-HD)-induced peripheral nerve injury,and the protective effect of Ginkgo biloba extract (Egb761) on 2,5-HD-induced toxic peri...Objective To investigate the role of myelin protein zero (P 0) in 2,5-hexanedione (2,5-HD)-induced peripheral nerve injury,and the protective effect of Ginkgo biloba extract (Egb761) on 2,5-HD-induced toxic peripheral neuropathy.Methods After 4 weeks of treatment with 2,5-HD at different doses (50,100,200,400 mg/kg) in rats,changes in the levels of P 0 in rat sciatic nerves was investigated,and the effect of Egb761 on 2,5-HD-induced toxic peripheral neuropathy was studied.Results The blood-nerve barrier (BNB) permeability of the sciatic nerve increased,and the expression of P 0 mRNA and P 0 protein decreased in a dose-dependent manner after treatment with 2,5-HD for 4 weeks.Pretreatment with Egb761 protected against BNB interruption,and inhibited P 0 mRNA and protein reduction during 2,5-HD treatment.Pretreatment with Egb761 significantly reduced loss of body weight (P0.01) and mitigated gait abnormalities (2.85±0.22) induced by 400 mg/kg 2,5-HD (P0.01).It also reduced the signs of neurotoxicity induced by 2,5-HD.Conclusion 2,5-HD inhibited the expression of P 0 in a dose-dependent manner,and this may be an important mechanism by which toxic peripheral neuropathy is induced by 2,5-HD.Egb761 has a protective effect against 2,5-HD-induced peripheral neurotoxicity in rats.展开更多
目的建立气相色谱-质谱法(gas chromatography mass spectrometry,GC-MS)测定食品中合成香料3-乙酰基-2,5-二甲基呋喃的方法。方法样品用正己烷涡旋提取后过滤,含油脂样品采用冷冻过滤技术去除油脂和其他杂质,选用TG-5MS毛细管色谱柱(30...目的建立气相色谱-质谱法(gas chromatography mass spectrometry,GC-MS)测定食品中合成香料3-乙酰基-2,5-二甲基呋喃的方法。方法样品用正己烷涡旋提取后过滤,含油脂样品采用冷冻过滤技术去除油脂和其他杂质,选用TG-5MS毛细管色谱柱(30 m×0.25 mm,0.25μm),载气流速1 mL/min进行分离后进质谱分析。结果3-乙酰基-2,5-二甲基呋喃在0.005~10.000μg/L质量浓度范围内曲线线性良好,相关系数为0.9997;在不同基质及不同加标浓度下,加标回收率为80.16%~103.76%,相对标准偏差为1.83%~7.87%(n=6);3-乙酰基-2,5-二甲基呋喃在不同基质中的检出限均可达到1μg/kg,定量限均可达到3μg/kg。结论该方法简单、准确度高、灵敏度好,可以用于食品中3-乙酰基-2,5-二甲基呋喃含量的快速检测,为合成香料的安全使用和监管提供技术手段。展开更多
基金supported by the National Nature Science Foundation of China (No.30700674 and No.30625031)the Project for Technologies of Occupational Health Surveillance and Detection (200902006)the Youth Fund of Chinese Center of Disease Control (2010A204)
文摘Objective To investigate the role of myelin protein zero (P 0) in 2,5-hexanedione (2,5-HD)-induced peripheral nerve injury,and the protective effect of Ginkgo biloba extract (Egb761) on 2,5-HD-induced toxic peripheral neuropathy.Methods After 4 weeks of treatment with 2,5-HD at different doses (50,100,200,400 mg/kg) in rats,changes in the levels of P 0 in rat sciatic nerves was investigated,and the effect of Egb761 on 2,5-HD-induced toxic peripheral neuropathy was studied.Results The blood-nerve barrier (BNB) permeability of the sciatic nerve increased,and the expression of P 0 mRNA and P 0 protein decreased in a dose-dependent manner after treatment with 2,5-HD for 4 weeks.Pretreatment with Egb761 protected against BNB interruption,and inhibited P 0 mRNA and protein reduction during 2,5-HD treatment.Pretreatment with Egb761 significantly reduced loss of body weight (P0.01) and mitigated gait abnormalities (2.85±0.22) induced by 400 mg/kg 2,5-HD (P0.01).It also reduced the signs of neurotoxicity induced by 2,5-HD.Conclusion 2,5-HD inhibited the expression of P 0 in a dose-dependent manner,and this may be an important mechanism by which toxic peripheral neuropathy is induced by 2,5-HD.Egb761 has a protective effect against 2,5-HD-induced peripheral neurotoxicity in rats.