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中枢神经系统中NG2阳性细胞的功能以及抗NG2抗体在脱髓鞘疾病中的病理作用。

NG2-positive cells in CNS function and the pathological role of antibodies against NG2 in demyelinating diseases.

作者信息

Trotter Jacqueline

机构信息

Unit of Molecular Cell Biology, Institute of Zoology, Department of Biology, Johannes Gutenberg University of Mainz, Bentzelweg 3, 55128 Mainz, Germany.

出版信息

J Neurol Sci. 2005 Jun 15;233(1-2):37-42. doi: 10.1016/j.jns.2005.03.024. Epub 2005 Apr 20.

Abstract

NG2 is expressed by a variety of immature glia in the CNS including oligodendrocyte progenitor cells, paranodal astrocytes and perisynaptic glia. The protein has a large extracellular domain with two LNS/Lam G domains at the N-terminus and a short intracellular tail with a PDZ-recognition domain at the C-terminus. Experiments suggest that the protein plays a role in migration. The PDZ protein GRIP was identified as an intracellular binding partner of NG2 in immature glial cells. A complex is formed between GRIP, NG2 and the AMPA class of glutamate receptors: this may position these glial receptors towards sites of neuronal glutamate release at synapses and during myelination. Identification of neuronal receptors and links to the cytoskeleton of NG2 is of critical importance. Some Multiple Sclerosis patients have autoantibodies to NG2 in the cerebral spinal fluid: such antibodies could interfere with remyelination by lysing oligodendrocyte progenitor cells or blocking their migration but may also cause pathology by disrupting glial-neuronal signalling at synapses and paranodes.

摘要

NG2 在中枢神经系统中由多种未成熟神经胶质细胞表达,包括少突胶质前体细胞、结旁星形胶质细胞和突触周围神经胶质细胞。该蛋白具有一个大的细胞外结构域,在 N 端有两个 LNS/Lam G 结构域,以及一个短的细胞内尾巴,在 C 端有一个 PDZ 识别结构域。实验表明该蛋白在迁移中起作用。PDZ 蛋白 GRIP 被鉴定为未成熟神经胶质细胞中 NG2 的细胞内结合伴侣。GRIP、NG2 和 AMPA 类谷氨酸受体之间形成复合物:这可能使这些神经胶质受体定位到突触处和髓鞘形成过程中神经元谷氨酸释放的部位。鉴定 NG2 的神经元受体及其与细胞骨架的联系至关重要。一些多发性硬化症患者的脑脊液中存在针对 NG2 的自身抗体:此类抗体可能通过裂解少突胶质前体细胞或阻断其迁移来干扰髓鞘再生,但也可能通过破坏突触和结旁的神经胶质-神经元信号传导而导致病理变化。

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