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首页> 外文期刊>Experimental Neurology >Microglia, astrocytes, and macrophages react differentially to central and peripheral lesions in the developing and mature rat whisker-to-barrel pathway: a study using immunohistochemistry for lipocortin1, phosphotyrosine, s100 beta, and mannose rece
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Microglia, astrocytes, and macrophages react differentially to central and peripheral lesions in the developing and mature rat whisker-to-barrel pathway: a study using immunohistochemistry for lipocortin1, phosphotyrosine, s100 beta, and mannose rece

机译:小胶质细胞,星形胶质细胞和巨噬细胞对发育中的和成熟的大鼠晶须-桶通路中的中央和周围病变的反应不同:使用免疫组化技术对lipocortin1,磷酸酪氨酸,s100 beta和甘露糖残渣进行免疫组化的研究

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Adult and neonatal rats were subjected to transection of the left infraorbital nerve or ablation of the left parietal cortex. The ensuing glial reaction in the whisker-to-barrel pathway was studied with immunohistochemistry for Lipocortin1- (LC1+), phosphotyrosine- (PY+), S100 beta- (S100 beta+), and mannose receptor- (MR+) immunoreactive microglia, astrocytes, and macrophages. Four days after infraorbital nerve transection in adult rats, LC1+ and PY+ microglia were prominently increased in the trigeminal sensory brain-stem nuclei on the deafferented side compared with the intact side. Changes were negligible at the second synapse of the pathway, i.e., the thalamic ventroposterior medial nucleus. Cortical ablation in adults led to an increase in microglia in the ipsilateral ventroposterior medial nucleus that reciprocally connects with the ablated cortex. Moreover, microglial reactions occurred in the contralateral trigeminal sensory brain-stem nuclei in which corticofugal projections from the ablated cortex terminate. S100 beta+ astrocytes, in contrast, appeared unaltered after both types of lesion in adults. In neonates, LC1+, PY+, and S100 beta+ cells did not have the adult morphology of microglia or astrocytes. Four days after nerve transection, LC1+ and PY+ cells were sparse and remained unchanged. In contrast, S100 beta+ cells substantially increased in the deafferented trigeminal brain-stem nuclei. Four days after cortical ablation in neonates, LC1+, PY+, and S100 beta+ cells had accumulated in the deprived thalamus. In contrast to adults, many of these cells were MR+ macrophages. In the deprived brain-stem, only S100 beta+ cells increased and none were macrophages. Therefore, macrophages do not appear to stem from microglia, and neonatal LC1+, PY+, and S100 beta+ cells may possess functions different from those in adults. Copyright 2001 Academic Press.
机译:成年和新生大鼠均接受左眶下神经横断或左顶叶皮质消融。用免疫组化方法研究了脂晶素1-(LC1 +),磷酸酪氨酸-(PY +),S100β-(S100β+)和甘露糖受体-(MR +)免疫反应性小胶质细胞,星形胶质细胞和巨噬细胞。成年大鼠眶下神经横断四天后,与完整侧相比,脱除腹膜的一侧的三叉神经感觉脑干核中LC1 +和PY +小胶质细胞显着增加。在该途径的第二个突触,即丘脑腹膜后内侧内侧核的变化可以忽略不计。成人的皮质消融导致与消融皮质相互连接的同侧腹后内侧核中的小胶质细胞增加。此外,小胶质细胞反应发生在对侧的三叉神经感觉脑干核中,来自消融皮层的皮质阴道突突终止。相比之下,在成年人的两种类型的病变之后,S100 beta +星形胶质细胞均未改变。在新生儿中,LC1 +,PY +和S100 beta +细胞没有小胶质细胞或星形胶质细胞的成年形态。神经横断后四天,LC1 +和PY +细胞稀疏并保持不变。相反,S100 beta +细胞在脱除三叉神经的三叉神经干核中显着增加。新生儿皮层消融后四天,剥夺的丘脑中已积累了LC1 +,PY +和S100 beta +细胞。与成人相反,这些细胞中有许多是MR +巨噬细胞。在被剥夺的脑干中,只有S100 beta +细胞增加,而没有一个是巨噬细胞。因此,巨噬细胞似乎并非源于小胶质细胞,新生儿LC1 +,PY +和S100 beta +细胞的功能可能与成年人不同。版权所有2001,学术出版社。

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