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多发性硬化症脑白质中血管密度增加和内皮细胞增殖。

Increased blood vessel density and endothelial cell proliferation in multiple sclerosis cerebral white matter.

机构信息

Peninsula Medical School, University of Exeter, St Luke's Campus, Magdalen Road, Exeter, EX1 2LU, United Kingdom.

出版信息

Neurosci Lett. 2010 Feb 5;470(1):65-70. doi: 10.1016/j.neulet.2009.12.059. Epub 2009 Dec 29.

DOI:10.1016/j.neulet.2009.12.059
PMID:20036712
Abstract

Multiple sclerosis (MS) is primarily considered an inflammatory demyelinating disease, however the role of vasculature in MS pathogenesis is now receiving much interest. MS lesions often develop along blood vessels and alterations in blood brain barrier structure and function, with associated changes in the basement membrane, are pathological features. Nevertheless, the possibility of angiogenesis occurring in MS has received little attention. In this study we used triple label enzyme immunohistochemistry to investigate blood vessel density and endothelial cell proliferation in MS samples (n=39) compared with control tissue to explore evidence of angiogenesis in MS. The results showed that in all MS samples examined blood vessel density increased compared with controls. The greatest increase was found in subacute lesions where numbers of positively stained vessels increased from 43.9+/-8.5% in controls to 84.2+/-13.3% (P=0.001). Furthermore, using an antibody against endoglin (CD105), a specific marker of proliferating endothelial cells, which are characteristic of angiogenesis, we have shown that vessels containing proliferating endothelial cells were more pronounced in all MS tissue examined (normal-appearing white matter, acute, subacute and chronic lesions, P>or=0.027) compared with control and this was greatest in the MS normal-appearing white matter (68.8+/-19.8% versus 10.58+/-6.4%, P=0.003). These findings suggest that angiogenesis may play a role in lesion progression, failure of repair and scar formation.

摘要

多发性硬化症(MS)主要被认为是一种炎症性脱髓鞘疾病,然而血管在 MS 发病机制中的作用现在受到了广泛关注。MS 病变通常沿着血管发展,血脑屏障结构和功能的改变,以及相关的基膜变化,是病理特征。然而,MS 中发生血管生成的可能性尚未得到充分关注。在这项研究中,我们使用三重标记酶免疫组织化学方法,比较了 MS 样本(n=39)与对照组织中的血管密度和内皮细胞增殖,以探讨 MS 中血管生成的证据。结果表明,在所有检查的 MS 样本中,与对照相比,血管密度增加。在亚急性病变中增加最为明显,阳性染色血管的数量从对照组的 43.9+/-8.5%增加到 84.2+/-13.3%(P=0.001)。此外,使用针对内皮细胞(endoglin, CD105)的抗体,该抗体是增殖内皮细胞的特异性标志物,也是血管生成的特征,我们已经表明,在所有检查的 MS 组织中,含有增殖内皮细胞的血管更为明显(正常表现白质、急性、亚急性和慢性病变,P>or=0.027),与对照相比,MS 正常表现白质中更为明显(68.8+/-19.8%比 10.58+/-6.4%,P=0.003)。这些发现表明,血管生成可能在病变进展、修复失败和瘢痕形成中发挥作用。

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