经前舒颗粒对PMS肝气郁证模型大鼠下丘脑MAOA和MAOB表达水平的影响

目的通过研究PMS肝气郁证模型大鼠下丘脑MAOA和MAOB基因的表达,探讨PMS肝气郁证的微观发病机制及中药经前舒颗粒的作用靶点。方法束缚法制备PMS肝气郁证模型大鼠,用经前舒颗粒干预治疗,运用半定量RT-PCR和Western Blotting方法检测正常组、模型组、给药组大鼠下丘脑区MAOA、MAOB mRNA及其蛋白表达水平;通过单因素方差分析及LSD法统计数据。结果与正常组相比,PMS肝气郁证模型组大鼠MAOA mRNA在下丘脑表达显著升高(P<0.05),蛋白表达极显著升高(P<0.01);MAOB mRNA及蛋白在下丘脑表达均无统计学差异(P>0.05);给药组与模型组相比,MAOA mRNA在下丘脑表达降低(P<0.05),蛋白表达显著降低(P<0.01);MAOB mRNA及蛋白在下丘脑表达均无统计学差异(P>0.05);给药组与正常组相比,MAOA、MAOB mRNA及蛋白在大鼠下丘脑中表达均无统计学差异(P>0.05)。结论模型组大鼠与正常组大鼠相比,下丘脑MAOA基因表达升高,通过经前舒颗粒干预后,恢复正常。说明MAOA基因与PMS肝气郁证相关,并且可能是经前舒颗粒治疗该证的作用机制之一。

利用RNA干扰技术抑制单胺氧化酶B基因的表达

目的确定并筛选用于特异静默单胺氧化酶B(Monoamine Oxidase B,MAOB)基因的干扰小RNA(siRNA)片段,建立RNA干扰技术平台。方法构建含单胺氧化酶B基因siRNA片段的pSilencer 1.0-U6 siRNA表达质粒,转染Hela细胞,用RT-PCR和定量PCR方法检测单氨氧化酶B mRNA的水平。结果所设计的两段siRNA片段均有干扰MAOB mRNA水平的作用,片段2的作用优于片段1,两个片段之间有一定的协同作用。结论选择的siRNA片段可以抑制Hela细胞单胺氧化酶B的表达。

Protein profiling identified mitochondrial dysfunction and synaptic abnormalities after dexamethasone intervention in rats with traumatic brain injury

Dexamethasone has been widely used after various neurosurgical procedures due to its anti-inflammatory property and the abilities to restore vascular permeability,inhibit free radicals,and reduce cerebrospinal fluid production.According to the latest guidelines for the treatment of traumatic brain injury in the United States,high-dose glucocorticoids cause neurological damage.To investigate the reason why high-dose glucocorticoids after traumatic brain injury exhibit harmful effect,rat controlled cortical impact models of traumatic brain injury were established.At 1 hour and 2 days after surgery,rat models were intraperitoneally administered dexamethasone 10 mg/kg.The results revealed that 31 proteins were significantly upregulated and 12 proteins were significantly downregulated in rat models of traumatic brain injury after dexamethasone treatment.The Ingenuity Pathway Analysis results showed that differentially expressed proteins were enriched in the mitochondrial dysfunction pathway and synaptogenesis signaling pathway.Western blot analysis and immunohistochemistry results showed that Ndufv2,Maob and Gria3 expression and positive cell count in the dexamethasone-treated group were significantly greater than those in the model group.These findings suggest that dexamethasone may promote a compensatory increase in complex I subunits(Ndufs2 and Ndufv2),increase the expression of mitochondrial enzyme Maob,and upregulate synaptic-transmission-related protein Gria3.These changes may be caused by nerve injury after traumatic brain injury treatment by dexamethasone.The study was approved by Institutional Ethics Committee of Beijing Neurosurgical Institute(approval No.201802001)on June 6,2018.

单胺氧化酶B单核苷酸多态性与幼犬工作行为性状的关联分析

测定了204条德国牧羊犬、拉布拉多犬、史宾格犬二月龄幼犬对人依恋性和服从性、衔取、争夺游戏和胆量等行为性状,同时用PCR-RFLP方法检测各犬单胺氧化酶B(MAOB)基因型。用2χ检验MAOB基因多态性的基因型和基因频率在品种间的分布,发现基因型和基因频率在犬品种之间差异极显著(P<0.01)。构建一般线性模型分析MAOB基因型与行为性状的关系,发现MAOB基因型对幼犬的衔取行为有显著影响(P<0.05)。TC基因型犬的衔取得分值均高于TT型(P<0.01)。这些结果表明,MAOB基因可能是影响犬衔取行为的主效基因或与主效基因紧密连锁的标记基因,可用于建立选择犬衔取性状的基因标记辅助选择方法。

Alzheimer病与单胺氧化酶B基因的关联分析

目的：论证Alzheimer病(AD)与单胺氧化酶B基因（MAOB）的两个微卫星DNA标记（MAOBI2和MAOBTG）是否存在关联．方法：应用微卫星DNA多态性的方法，计算73例AD患者和81名正常对照者等位基因频率，并对AD与MAOBI2及MAOBTG的各等位基因进行关联分析．结果：得出了正常人和AD病人MAOBI2和MAOBTG的筹位基因频率．关联分析表明，AD与MAOBI2的等位基因176bp存在接近显著的正相关，相对危险率为4.21，x2=2.98，与MAOBTG的等位基因201bp和207bp分别存在接近显著的正相关和负相关，相对危险率分别为4．76和0．14，x2分别为3．73和3.30．结论：Alzheimer病与单胺氧化酶B基因的两个微卫星DNA标记（MAOBI2和MAOBTG）可能不存在显著性关联．

拟除虫菊酯对大鼠脑组织及肝脏生物转化酶的影响

目的 实验研究溴氰菊酯 (DM)和氯菊酯 (PM)对大鼠脑组织及肝脏某些生物转化酶的影响。方法 应用荧光分光光度法、二硝基苯肼比色法和Habig法检测 7 乙氧基试卤灵 O 脱乙基酶(EROD)、B型单胺氧化酶 (MAOB)和谷胱甘肽S 转移酶 (GST)活力。结果 整体实验中 ,DM染毒动物肝脏EROD、MAOB活力分别下降了 47.94%和 2 2 .76 % ;脑组织和肝脏GST活力分别增加了 2 2 .2 0 %和39.5 5 % ;多氯联苯 (PCB)的诱导EROD效应被明显抑制。PM染毒动物肝脏MAOB活力下降了36 .11% ;脑组织和肝脏GST活力分别增加了 36 .76 %和 39.2 5 %。体外实验中 ,DM在 1× 10 -4 ～1× 10 -3 mol/L、PM在 1× 10 -5～ 1× 10 -3 mol/L的浓度时 ,肝微粒体EROD活力均受抑制 ,并有剂量 -效应关系 (r =- 0 .90、r =- 0 .84,P <0 .0 1) ;DM在 1× 10 -6～ 1× 10 -5mol/L的浓度时 ,脑线粒体MAOB活力均受抑制 (r=- 0 .88) ;PM在 1× 10 -4 ～ 1× 10 -3 mol/L、DM在 1× 10 -5～ 1× 10 -3 mol/L的浓度时 ,脑组织胞浆GST活力均增强 ,与对照组的差异均有显著性 (r=0 .86、r =0 .83,P <0 .0 5 ,P <0 .0 1)。