Axon-glial interaction in the CNS: what we have learned from mouse models of Pelizaeus-Merzbacher disease.

Gruenenfelder FI; Thomson G; Penderis J; Edgar JM

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Axon-glial interaction in the CNS: what we have learned from mouse models of Pelizaeus-Merzbacher disease.

机译：中枢神经系统中的轴突-胶质相互作用：我们从佩利扎伊斯-梅尔茨巴赫病小鼠模型中学到的东西。

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In the central nervous system (CNS) the majority of axons are surrounded by a myelin sheath, which is produced by oligodendrocytes. Myelin is a lipid-rich insulating material that facilitates the rapid conduction of electrical impulses along the myelinated nerve fibre. Proteolipid protein and its isoform DM20 constitute the most abundant protein component of CNS myelin. Mutations in the PLP1 gene encoding these myelin proteins cause Pelizaeus-Merzbacher disease and the related allelic disorder, spastic paraplegia type 2. Animal models of these diseases, particularly models lacking or overexpressing Plp1, have shed light on the interplay between axons and oligodendrocytes, and how one component influences the other.

机译：在中枢神经系统（CNS）中，大多数轴突被少突胶质细胞产生的髓鞘包围。髓磷脂是一种富含脂质的绝缘材料，可促进电脉冲沿有髓神经纤维的快速传导。蛋白脂蛋白及其同工型DM20构成中枢神经系统髓磷脂最丰富的蛋白成分。编码这些髓磷脂蛋白的PLP1基因中的突变会导致Pelizaeus-Merzbacher病和相关的等位基因失调，即痉挛性截瘫2型。这些疾病的动物模型，尤其是缺乏或过表达Plp1的模型，为轴突与少突胶质细胞之间的相互作用提供了线索。一个组件如何影响另一个。

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《Journal of Anatomy》 |2011年第1期|共11页
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Gruenenfelder FI; Thomson G; Penderis J; Edgar JM;
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1. Axon-glial interaction in the CNS: what we have learned from mouse models of Pelizaeus-Merzbacher disease. [J] . Gruenenfelder FI, Thomson G, Penderis J, Journal of Anatomy . 2011,第1期

机译：中枢神经系统中的轴突-胶质相互作用：我们从佩利扎伊斯-梅尔茨巴赫病小鼠模型中学到的东西。
2. Alteration of the CNS pathway to the hippocampus in a mouse model of Niemann-Pick, type C disease. [J] . Byun K, Kim JM, Kim N, Journal of chemical neuroanatomy . 2011,第1期

机译：在C型Niemann-Pick小鼠模型中，CNS通路向海马的改变。
3. Intracerebroventricular infusion of acid sphingomyelinase corrects CNS manifestations in a mouse model of Niemann-Pick A disease. [J] . Dodge JC, Clarke J, Treleaven CM Experimental Neurology . 2009,第2期

机译：脑室内注入酸性鞘磷脂酶可纠正Niemann-Pick A病小鼠模型中的CNS表现。
4. Scn2a-Null Heterozygosity Improves Survival and Modifies Neurocardiac Interaction in the Kcna1-Null Mouse Model of SUDEP [C] . Vikas Mishra, Nicky Gautier, Bharat K. Karumuri, Southern Biomedical Engineering Conference . 2016

机译：Scn2a-空杂合性提高生存率，并修改SUDEP的Kcna1-空小鼠模型中的神经心相互作用。
5. Application of magnetic resonance imaging to understanding the pathogenesis of the X-linked leukodystrophy Pelizaeus-Merzbacher disease. [D] . Laukka, Jeremy Jerome. 2010

机译：磁共振成像的应用，以了解X链接的白细胞营养不良Pelizaeus-Merzbacher病的发病机理。
6. Axon–glial interaction in the CNS: what we have learned from mouse models of Pelizaeus–Merzbacher disease [O] . Fredrik I Gruenenfelder, Gemma Thomson, Jacques Penderis, 2011

机译：中枢神经系统中的轴突-胶质相互作用：我们从比利牛斯-梅尔茨巴赫病小鼠模型中学到的东西
7. Dysfunction of the CNS-heart axis in mouse models of Huntington's disease. [O] . Michal Mielcarek, Linda Inuabasi, Marie K Bondulich, 2014

机译：亨廷顿病小鼠模型中CNs-心轴的功能障碍。

Axon-glial interaction in the CNS: what we have learned from mouse models of Pelizaeus-Merzbacher disease.

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