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Specific localized expression of cGMP PDEs in Purkinje neurons and macrophages.

机译:cGMP PDEs在浦肯野神经元和巨噬细胞中的特定局部表达。

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摘要

As cGMP hydrolyzing cyclic nucleotide phosphodiesterases (PDEs) have diverse regulatory and catalytic properties, the specific cGMP PDEs a cell expresses will determine the duration and intensity of a cGMP signal. This, in turn, results in different cellular responses between cell types and tissues. Therefore, identifying which cGMP PDEs are expressed in different tissues and cell types could increase our understanding of physiological and pathological processes. The brain is one area where large numbers of diverse cGMP PDEs are expressed in specific regions and cell types. A case in point is differential expression of cGMP PDEs in neuronal cells. For example, we have recently found that PDE5 is expressed in all Purkinje neurons while PDE1B is expressed in only a subset of these neurons. The expression of PDE2 has also been found to be selective for discrete populations of neurons. Another example of selective cGMP PDE expression is seen with cytokine-induced differentiation of monocytes to macrophages. We have recently discovered that monocyte differentiation with the cytokine macrophage colony-stimulating factor (M-CSF) causes an upregulation of PDE2 and a small increase in PDE1B while granulocyte-macrophage colony-stimulating factor (GM-CSF) causes a large increase in PDE1B but a decrease in PDE2. These same cytokines can influence the phenotype of microglial cells and are likely to affect their expression of cGMP PDEs. In this report, we present recent results from our laboratory and review earlier findings illustrating the concept of highly specific expression of cGMP PDEs and discuss how this may be important for understanding brain function and dysfunction.
机译:由于cGMP水解环状核苷酸磷酸二酯酶(PDE)具有多种调节和催化特性,细胞表达的特定cGMP PDE将决定cGMP信号的持续时间和强度。反过来,这导致细胞类型与组织之间的细胞反应不同。因此,鉴定哪些cGMP PDEs在不同的组织和细胞类型中表达可以增进我们对生理和病理过程的了解。大脑是在特定区域和细胞类型中表达大量不同cGMP PDE的区域。一个典型的例子是神经元细胞中cGMP PDE的差异表达。例如,我们最近发现PDE5在所有浦肯野神经元中表达,而PDE1B仅在这些神经元的一个子集中表达。还发现PDE2的表达对离散的神经元群体具有选择性。选择性cGMP PDE表达的另一个例子是细胞因子诱导的单核细胞向巨噬细胞分化。我们最近发现,单核细胞分化与细胞因子巨噬细胞集落刺激因子(M-CSF)导致PDE2上调和PDE1B的少量增加,而粒细胞巨噬细胞集落刺激因子(GM-CSF)导致PDE1B的大量增加但PDE2降低。这些相同的细胞因子可影响小胶质细胞的表型,并可能影响其cGMP PDEs的表达。在本报告中,我们介绍了实验室的最新结果,并回顾了先前的发现,这些结果阐明了cGMP PDEs高度特异性表达的概念,并讨论了这对于理解脑功能和功能障碍的重要性。

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