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微球栓塞诱导大鼠脑内神经生长因子水平升高及活化T淋巴细胞中神经生长因子免疫反应性的出现。

Microsphere embolism-induced elevation of nerve growth factor level and appearance of nerve growth factor immunoreactivity in activated T-lymphocytes in the rat brain.

作者信息

Mizuma H, Takagi K, Miyake K, Takagi N, Ishida K, Takeo S, Nitta A, Nomoto H, Furukawa Y, Furukawa S

机构信息

Department of Pharmacology, Tokyo University of Pharmacy & Life Science, Hachioji, Japan.

出版信息

J Neurosci Res. 1999 Mar 15;55(6):749-61. doi: 10.1002/(SICI)1097-4547(19990315)55:6<749::AID-JNR9>3.0.CO;2-N.

Abstract

Changes in nerve growth factor (NGF) level and type of cells producing NGF were investigated in the rat brain after sustained cerebral embolism. The NGF level was determined by a two-site enzyme immunoassay specific for NGF. The cerebral cortex, striatum, and hippocampus of the embolized hemisphere maximally contained 2.4-, 2.4-, and 1.7-times higher NGF levels than the corresponding regions of the nonembolized hemisphere. A significant increase was transiently observed for 1 week in the cerebral cortex and striatum, whereas the increase was longer lasting, at least of 4 weeks' duration, in the hippocampus. To examine the localization of NGF-like immunoreactivity (NGF-LI), we used a newly developed anti-NGF peptide antiserum that specifically recognized a 30-kDa molecule(s) in the hippocampal extracts or in NGF cDNA-transfected cells, suggesting that the antibody predominantly reacted with the putative NGF precursor protein(s). NGF-LI, which was localized in neurons of the normal or non-embolized hemisphere, was reduced, and on the embolized side new signals emerged in small non-neuronal cells having a round shape. These included cells with common leukocyte antigen CD45 and T-lymphocyte antigen CD3, which did not appear in the normal or non-embolized hemisphere. NGF-LI and CD3 were colocalized in a substantial number of the cells, suggesting that some activated T-lymphocytes produce NGF for neuronal regeneration after sustained cerebral embolism.

摘要

在大鼠持续性脑栓塞后,研究了神经生长因子(NGF)水平及产生NGF的细胞类型的变化。通过对NGF特异的双位点酶免疫测定法来测定NGF水平。栓塞侧半球的大脑皮质、纹状体和海马中的NGF水平分别比未栓塞侧半球相应区域高2.4倍、2.4倍和1.7倍。在大脑皮质和纹状体中,在1周内短暂观察到显著增加,而在海马中增加持续时间更长,至少持续4周。为了检测NGF样免疫反应性(NGF-LI)的定位,我们使用了一种新开发的抗NGF肽抗血清,该抗血清能在海马提取物或NGF cDNA转染细胞中特异性识别一个30 kDa的分子,这表明该抗体主要与假定的NGF前体蛋白发生反应。NGF-LI定位于正常或未栓塞侧半球的神经元中,其含量减少,而在栓塞侧,圆形的小非神经元细胞中出现了新的信号。这些细胞包括具有共同白细胞抗原CD45和T淋巴细胞抗原CD3的细胞,它们在正常或未栓塞侧半球中未出现。大量细胞中NGF-LI和CD3共定位,这表明在持续性脑栓塞后,一些活化的T淋巴细胞产生NGF用于神经元再生。

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