首页> 外文期刊>The journal of histochemistry and cytochemistry >Protease-Activated Receptor–1 Expression in Rat Microglia after Trimethyltin Treatment
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Protease-Activated Receptor–1 Expression in Rat Microglia after Trimethyltin Treatment

机译:三甲基锡治疗后大鼠微胶质蛋白酶活化受体-1表达

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In the nervous system, protease-activated receptors , which are activated by thrombin and other extracellular proteases, are expressed widely at both neuronal and glial levels and have been shown to be involved in several brain pathologies. As far as the glial receptors are concerned, previous experiments performed in rat hippocampus showed that expression of PAR-1, the prototypic member of the PAR family, increased in astrocytes both in vivo and in vitro following treatment with trimethyltin . TMT is an organotin compound that induces severe hippocampal neurodegeneration associated with astrocyte and microglia activation. In the present experiments, the authors extended their investigation to microglial cells. In particular, by 7 days following TMT intoxication in vivo, confocal immunofluorescence revealed an evident PAR-1-related specific immunoreactivity in OX-42-positive microglial cells of the CA3 and hilus hippocampal regions. In line with the in vivo results, when primary rat microglial cells were treated in vitro with TMT, a strong upregulation of PAR-1 was observed by immunocytochemistry and Western blot analysis. These data provide further evidence that PAR-1 may be involved in microglial response to brain damage.
机译:在神经系统中,由凝血酶和其他细胞外蛋白酶激活的蛋白酶活化受体在神经元和神经胶质水平上广泛表达,并且已被证明参与了几种脑病变。就胶质受体而言,在大鼠海马中进行的先前实验表明,PAR-1的表达,PAR系列的原型成员,在用三甲基锡治疗后的体内和体外的星形胶质细胞中增加。 TMT是一种有机锡化合物,诱导与星形胶质细胞和微胶质细胞活化相关的严重的海马神经变性。在目前的实验中,作者将其对小细胞细胞进行了调查。特别地,在体内TMT中毒后7天,共聚焦免疫荧光揭示了CA3和Hilus海马区的OX-42阳性微胶质细胞中明显的PAR-1相关的特异性免疫反应性。根据体内结果,当用TMT体外处理原代大鼠小胶质细胞时,通过免疫细胞化学和免疫印迹分析观察到PAR-1的强烈上调。这些数据提供了进一步的证据,即PAR-1可以参与对脑损伤的微胶质响应。

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