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2
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本文引用的文献

1
Structure and stability of internodal myelin in mouse models of hereditary neuropathy.遗传性神经病变小鼠模型中节间髓鞘的结构与稳定性
J Neuropathol Exp Neurol. 2005 Nov;64(11):976-90. doi: 10.1097/01.jnen.0000186925.95957.dc.
2
Endoplasmic reticulum stress modulates the response of myelinating oligodendrocytes to the immune cytokine interferon-gamma.内质网应激调节有髓少突胶质细胞对免疫细胞因子γ干扰素的反应。
J Cell Biol. 2005 May 23;169(4):603-12. doi: 10.1083/jcb.200502086.
3
Impaired proteasome activity and accumulation of ubiquitinated substrates in a hereditary neuropathy model.遗传性神经病变模型中蛋白酶体活性受损及泛素化底物的积累
J Neurochem. 2005 Mar;92(6):1531-41. doi: 10.1111/j.1471-4159.2004.02987.x.
4
Disruption of Mtmr2 produces CMT4B1-like neuropathy with myelin outfolding and impaired spermatogenesis.Mtmr2的破坏会产生类似CMT4B1的神经病变,伴有髓鞘折叠和精子发生受损。
J Cell Biol. 2004 Nov 22;167(4):711-21. doi: 10.1083/jcb.200407010.
5
Expression analysis of the N-Myc downstream-regulated gene 1 indicates that myelinating Schwann cells are the primary disease target in hereditary motor and sensory neuropathy-Lom.N-Myc下游调控基因1的表达分析表明,髓鞘形成雪旺细胞是遗传性运动和感觉神经病-Lom的主要疾病靶点。
Neurobiol Dis. 2004 Nov;17(2):290-9. doi: 10.1016/j.nbd.2004.07.014.
6
XBP1: a link between the unfolded protein response, lipid biosynthesis, and biogenesis of the endoplasmic reticulum.XBP1:未折叠蛋白反应、脂质生物合成与内质网生物发生之间的联系。
J Cell Biol. 2004 Oct 11;167(1):35-41. doi: 10.1083/jcb.200406136. Epub 2004 Oct 4.
7
Pathology of a mouse mutation in peripheral myelin protein P0 is characteristic of a severe and early onset form of human Charcot-Marie-Tooth type 1B disorder.外周髓磷脂蛋白P0的小鼠突变病理学特征为人类1B型夏科-马里-图斯病的严重早发型。
J Cell Biol. 2004 May 24;165(4):565-73. doi: 10.1083/jcb.200402087. Epub 2004 May 17.
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A trip to the ER: coping with stress.急诊室之行:应对压力
Trends Cell Biol. 2004 Jan;14(1):20-8. doi: 10.1016/j.tcb.2003.11.001.
9
Phenotypic clustering in MPZ mutations.MPZ 突变中的表型聚类
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Disease mechanisms in inherited neuropathies.遗传性神经病的发病机制。
Nat Rev Neurosci. 2003 Sep;4(9):714-26. doi: 10.1038/nrn1196.

不同的细胞内致病机制在转基因小鼠中产生了多种髓鞘蛋白零神经病变。

Different intracellular pathomechanisms produce diverse Myelin Protein Zero neuropathies in transgenic mice.

作者信息

Wrabetz Lawrence, D'Antonio Maurizio, Pennuto Maria, Dati Gabriele, Tinelli Elisa, Fratta Pietro, Previtali Stefano, Imperiale Daniele, Zielasek Jurgen, Toyka Klaus, Avila Robin L, Kirschner Daniel A, Messing Albee, Feltri M Laura, Quattrini Angelo

机构信息

DIBIT, San Raffaele Scientific Institute, 20132 Milan, Italy.

出版信息

J Neurosci. 2006 Feb 22;26(8):2358-68. doi: 10.1523/JNEUROSCI.3819-05.2006.

DOI:10.1523/JNEUROSCI.3819-05.2006
PMID:16495463
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6674823/
Abstract

Missense mutations in 22 genes account for one-quarter of Charcot-Marie-Tooth (CMT) hereditary neuropathies. Myelin Protein Zero (MPZ, P0) mutations produce phenotypes ranging from adult demyelinating (CMT1B) to early onset [Déjérine-Sottas syndrome (DSS) or congenital hypomyelination] to predominantly axonal neuropathy, suggesting gain of function mechanisms. To test this directly, we produced mice in which either the MpzS63C (DSS) or MpzS63del (CMT1B) transgene was inserted randomly, so that the endogenous Mpz alleles could compensate for any loss of mutant P0 function. We show that either mutant allele produces demyelinating neuropathy that mimics the corresponding human disease. However, P0S63C creates a packing defect in the myelin sheath, whereas P0S63del does not arrive to the myelin sheath and is instead retained in the endoplasmic reticulum, where it elicits an unfolded protein response (UPR). This is the first evidence for UPR in association with neuropathy and provides a model to determine whether and how mutant proteins can provoke demyelination from outside of myelin.

摘要

22个基因中的错义突变占夏科-马里-图斯(CMT)遗传性神经病的四分之一。髓磷脂蛋白零(MPZ,P0)突变产生的表型范围从成人脱髓鞘型(CMT1B)到早发型[德热里纳-索塔斯综合征(DSS)或先天性髓鞘形成不足]再到主要为轴索性神经病,提示存在功能获得机制。为了直接验证这一点,我们培育了随机插入MpzS63C(DSS)或MpzS63del(CMT1B)转基因的小鼠,这样内源性Mpz等位基因可以补偿突变型P0功能的任何缺失。我们发现,任一突变等位基因都会产生模仿相应人类疾病的脱髓鞘性神经病。然而,P0S63C在髓鞘中造成了堆积缺陷,而P0S63del没有到达髓鞘,而是保留在内质网中,在那里引发未折叠蛋白反应(UPR)。这是与神经病相关的未折叠蛋白反应的首个证据,并提供了一个模型来确定突变蛋白是否以及如何能从髓鞘外部引发脱髓鞘。