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在多发性硬化症的灰质病变中,内质网应激和缺氧相关分子的表达增加。

Increased expression of ER stress- and hypoxia-associated molecules in grey matter lesions in multiple sclerosis.

机构信息

MS and Stroke Research Group, NCBES, National University of Ireland, Ireland.

出版信息

Mult Scler. 2012 Oct;18(10):1437-47. doi: 10.1177/1352458512438455. Epub 2012 Feb 21.

Abstract

BACKGROUND

The endoplasmic reticulum (ER) stress pathway may play a role in the pathogenesis multiple sclerosis (MS), and while ER stress-associated molecules have been demonstrated in white matter (WM) lesions, these have not been analysed in grey matter (GM) demyelination.

OBJECTIVE

The objective was to characterise the type and frequency of GM lesions and establish expression profiles of ER stress- and hypoxia-associated markers.

METHODS

Sections from 16 MS cases and 12 non-MS controls were stained for ER stress molecules (BiP and CHOP) and hypoxia-associated D110 antigen.

RESULTS

Of the GM lesions analysed, 24% were type 1 (continuous between GM and WM), 22% were type 2 (entirely within GM) and the majority (54%) were type 3 (extending from pia mater). Comparison of GM lesions, MS normal-appearing grey matter (NAGM) and non-MS control tissue showed that NAGM, type 1 and type 3 lesions all had significantly increased levels of CHOP compared to controls. According to morphological and dual-labelling criteria, the majority of CHOP-positive cells were microglia. Approximately 50% of GM lesions contained D110-positive cells.

CONCLUSION

These data suggest that ER stress plays an important role in GM lesion development and may be critical in activation of microglia in pre-lesional NAGM. The high number of lesions containing D110-positive cells suggests a role for hypoxic-like insult in GM lesion development.

摘要

背景

内质网(ER)应激途径可能在多发性硬化症(MS)的发病机制中发挥作用,尽管已经在白质(WM)病变中证明了与 ER 应激相关的分子,但尚未在灰质(GM)脱髓鞘中对其进行分析。

目的

本研究旨在描述 GM 病变的类型和频率,并建立 ER 应激和缺氧相关标志物的表达谱。

方法

对 16 例 MS 病例和 12 例非 MS 对照的组织切片进行 ER 应激分子(BiP 和 CHOP)和缺氧相关 D110 抗原染色。

结果

在所分析的 GM 病变中,24%为 1 型(连续存在于 GM 和 WM 之间),22%为 2 型(完全位于 GM 内),大多数(54%)为 3 型(从软脑膜延伸)。比较 GM 病变、MS 正常外观灰质(NAGM)和非 MS 对照组织发现,与对照组相比,NAGM、1 型和 3 型病变的 CHOP 水平均显著升高。根据形态学和双重标记标准,大多数 CHOP 阳性细胞为小胶质细胞。约 50%的 GM 病变含有 D110 阳性细胞。

结论

这些数据表明 ER 应激在 GM 病变发展中起重要作用,并且可能对 NAGM 中病变前小胶质细胞的激活至关重要。大量含有 D110 阳性细胞的病变表明缺氧样损伤在 GM 病变发展中起作用。

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