首页> 外文期刊>Journal of neuroimmune pharmacology: the official journal of the Society on NeuroImmune Pharmacology >Expression of dopaminergic receptors on human CD4+ T lymphocytes: Flow cytometric analysis of naive and memory subsets and relevance for the neuroimmunology of neurodegenerative disease
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Expression of dopaminergic receptors on human CD4+ T lymphocytes: Flow cytometric analysis of naive and memory subsets and relevance for the neuroimmunology of neurodegenerative disease

机译:多巴胺能受体在人CD4 + T淋巴细胞上的表达:幼稚和记忆子集的流式细胞术分析及其与神经退行性疾病的神经免疫学的相关性

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Dopamine (DA) is a crucial transmitter in the neuroimmune network, where it contributes to the nervous system-immune system interplay as well as in the communication among immune cells. DA acts through five different dopaminergic receptors (DR) grouped into two families: the D1-like (D1 and D5) and the D2-like (D2, D3 and D4). By use of 5-color flow cytometric analysis, we examined the expression of DR on human CD4+ naive T lymphocytes (CD3+CD4+CD45RA+CCR7+), central memory (TCM, CD3+CD4+CD45RA-CCR7+) and effector memory T cells (TEM, CD3+CD4+CD45RA-CCR7-). In addition, in cultured CD4+ T cells we investigated the changes in DR expression induced by stimulation with antiCD3/antiCD28 antibodies. Results showed that CD4+ T cells always expressed all the five DR: D1-like DR were identified on average on 11.6-13.1 % and D2-like DR on 3.1-8.1 % of the cells. DR on CD4+ naive T cells, TCM, and TEM had distinct expression patterns: naive T cells expressed more D1-like than D2-like DR, which on the contrary were increased in TCM and TEM cells. In cultured CD4+ T cells stimulation with anti-CD3/anti-CD28 antibodies increased the expression of D1-like DR by 71-84 % and of D2-like DR by 55-97 %. The frequency of DR was higher in apoptotic cells in comparison to viable cells, however stimulation increased all DR on viable cells, without affecting their expression on apoptotic cells. The present results contribute to unravel the complexity of dopaminergic pathways in human CD4+ T lymphocytes, suggesting their involvement in memory functions as well as in apoptotic processes. In view of the role of CD4+ memory T cells in neuroinflammation and neurodegeneration during Parkinson's disease, the relevance of these findings must be assessed in the clinical setting.
机译:多巴胺(DA)是神经免疫网络中的重要递质,在其中它促进神经系统与免疫系统的相互作用以及免疫细胞之间的通讯。 DA通过五个不同的多巴胺能受体(DR)起作用,该受体分为两个家族:D1类(D1和D5)和D2类(D2,D3和D4)。通过使用5色流式细胞术分析,我们检查了DR在人CD4 +幼稚T淋巴细胞(CD3 + CD4 + CD45RA + CCR7 +),中枢记忆(TCM,CD3 + CD4 + CD45RA-CCR7 +)和效应记忆T细胞上的表达(TEM,CD3 + CD4 + CD45RA-CCR7-)。此外,在培养的CD4 + T细胞中,我们研究了抗CD3 / antiCD28抗体刺激诱导的DR表达的变化。结果表明,CD4 + T细胞始终表达全部五个DR:平均鉴定出D1类DR占11.6-13.1%,D2类DR占3.1-8.1%。 CD4 +原始T细胞,TCM和TEM上的DR具有不同的表达模式:原始T细胞比D2相似的DR表达更多的D1样,而在TCM和TEM细胞中则增加。在培养的CD4 + T细胞中,用抗CD3 /抗CD28抗体刺激可使D1样DR的表达增加71-84%,使D2样DR的表达增加55-97%。与活细胞相比,凋亡细胞中DR的频率更高,但是刺激增加了活细胞上所有DR的表达,而不影响它们在凋亡细胞上的表达。目前的结果有助于揭示人类CD4 + T淋巴细胞中多巴胺能途径的复杂性,表明它们参与了记忆功能以及凋亡过程。考虑到CD4 +记忆T细胞在帕金森氏病期间神经炎症和神经退行性变中的作用,必须在临床环境中评估这些发现的相关性。

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