氮杂环丁烷-2-羧酸诱导的少突胶质病变：与多发性硬化症发病机制的相关性。

Azetidine-2-Carboxylic Acid-Induced Oligodendrogliopathy: Relevance to the Pathogenesis of Multiple Sclerosis.

机构信息

From the Laboratory Service, Veterans Affairs Health Care System, Palo Alto, California, USA.

Department of Pathology, Stanford University School of Medicine, Stanford, California, USA.

出版信息

J Neuropathol Exp Neurol. 2022 May 20;81(6):414-433. doi: 10.1093/jnen/nlac028.

DOI:10.1093/jnen/nlac028

PMID:35521963

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9123080/

Abstract

The naturally occurring imino acid azetidine-2-carboxylic acid (Aze) is consumed by humans and can be misincorporated in place of proline in myelin basic protein (MBP) in vitro. To determine Aze effects on the mammalian CNS in vivo, adult CD1 mice were given Aze orally or intraperitoneally. Clinical signs reminiscent of MBP-mutant mice occurred with 600 mg/kg Aze exposure. Aze induced oligodendrocyte (OL) nucleomegaly and nucleoplasm clearing, dilated endoplasmic reticulum, cytoplasmic vacuolation, abnormal mitochondria, and Aze dose-dependent apoptosis. Immunohistochemistry demonstrated myelin blistering and nuclear translocation of unfolded protein response (UPR)/proinflammatory molecules (ATF3, ATF4, ATF6, eIF2α, GADD153, NFκB, PERK, XBP1), MHC I expression, and MBP cytoplasmic aggregation in OL. There were scattered microglial nodules in CNS white matter (WM); other CNS cells appeared unaffected. Mice given Aze in utero and postnatally showed more marked effects than their dams. These OL, myelin, and microglial alterations are found in normal-appearing WM (NAWM) in multiple sclerosis (MS) patients. Thus, Aze induces a distinct oligodendrogliopathy in mice that recapitulates MS NAWM pathology without leukocyte infiltration. Because myelin proteins are relatively stable throughout life, we hypothesize that Aze misincorporation in myelin proteins during myelinogenesis in humans results in a progressive UPR that may be a primary process in MS pathogenesis.

摘要

天然存在的亚氨基羧酸氮杂环丁烷-2-羧酸（Aze）被人类消耗，并可在体外替代髓鞘碱性蛋白（MBP）中的脯氨酸发生错误掺入。为了确定 Aze 在体内对哺乳动物中枢神经系统的影响，成年 CD1 小鼠经口或腹膜内给予 Aze。600mg/kg Aze 暴露后出现类似于 MBP 突变小鼠的临床症状。Aze 诱导少突胶质细胞（OL）核肥大和核质清除、内质网扩张、细胞质空泡化、线粒体异常以及与 Aze 剂量呈依赖性的细胞凋亡。免疫组织化学显示髓鞘起泡和未折叠蛋白反应（UPR）/炎症分子（ATF3、ATF4、ATF6、eIF2α、GADD153、NFκB、PERK、XBP1）、MHC I 表达以及 OL 中 MBP 细胞质聚集的核易位。中枢神经系统白质（WM）中有散在的小胶质细胞结节；其他中枢神经系统细胞似乎未受影响。在子宫内和产后给予 Aze 的小鼠比其母体表现出更明显的效果。这些 OL、髓鞘和小胶质细胞的改变在多发性硬化症（MS）患者的正常外观 WM（NAWM）中均有发现。因此，Aze 在小鼠中诱导了一种独特的少突胶质细胞病，其重现了 MS NAWM 病理学而没有白细胞浸润。由于髓鞘蛋白在整个生命过程中相对稳定，我们假设 Aze 在人类髓鞘发生过程中错误掺入髓鞘蛋白会导致未折叠蛋白反应（UPR）的进行，这可能是 MS 发病机制中的一个主要过程。