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大鼠实验性脑动脉瘤形成及增殖修复过程中纤连蛋白的免疫组化改变

Immunohistochemical alterations of fibronectin during the formation and proliferative repair of experimental cerebral aneurysms in rats.

作者信息

Futami K, Yamashita J, Tachibana O, Higashi S, Ikeda K, Yamashima T

机构信息

Department of Neurosurgery, Kanazawa University School of Medicine, Japan.

出版信息

Stroke. 1995 Sep;26(9):1659-64. doi: 10.1161/01.str.26.9.1659.

Abstract

BACKGROUND AND PURPOSE

To determine whether distributional changes of fibronectin, a factor promoting wound healing, occur during the formation and repair of cerebral saccular aneurysms, we performed immunohistochemical analyses in experimental aneurysms.

METHODS

Cerebral aneurysms were induced in rats by both the ligation of the unilateral common carotid artery and induced hypertension. Intimal proliferation in aneurysmal walls was induced by the ligation of the preserved common carotid artery 3 months after the first operation. The distribution of fibronectin was examined by immunohistochemistry in anterior cerebral artery-olfactory artery bifurcations under the following three conditions: normal bifurcations in control rats, early aneurysmal lesions during the aneurysm induction, and aneurysmal lesions with intimal proliferation. Furthermore, the immunohistochemical distributions of type I and IV collagens were examined to evaluate the specificity of fibronectin immunoreactivity.

RESULTS

In the normal bifurcations, fibronectin was positive in the subintimal space, the surrounding area of the medial smooth muscle cells, and the adventitial fibrous tissue. In early aneurysmal lesions, linear staining of fibronectin and type I and IV collagens in the subendothelial space disappeared with the loss of the internal elastic lamina. In the intimal proliferation of early aneurysmal lesions, fibronectin was strongly immunostained in the subendothelial space and diffusely immunostained in the widened extracellular space surrounding proliferated cells. In contrast, the stainings of type I and IV collagens were sparse or negative.

CONCLUSIONS

Although the present findings regarding dynamic changes of fibronectin distribution do not prove any causality in the process of aneurysm formation and repair, these immunohistochemical changes may constitute the crucial sequela of intimal endothelial damage and its subsequent recovery in cerebral aneurysms.

摘要

背景与目的

为了确定促进伤口愈合的因子纤连蛋白在脑囊状动脉瘤形成和修复过程中是否发生分布变化,我们对实验性动脉瘤进行了免疫组织化学分析。

方法

通过结扎单侧颈总动脉并诱导高血压在大鼠中诱发脑动脉瘤。首次手术后3个月,通过结扎保留的颈总动脉诱导动脉瘤壁内膜增生。在以下三种情况下,通过免疫组织化学检查大脑前动脉 - 嗅动脉分叉处纤连蛋白的分布:对照大鼠的正常分叉处、动脉瘤诱导期间的早期动脉瘤病变以及伴有内膜增生的动脉瘤病变。此外,检查I型和IV型胶原的免疫组织化学分布以评估纤连蛋白免疫反应性的特异性。

结果

在正常分叉处,纤连蛋白在内膜下间隙、内侧平滑肌细胞周围区域和外膜纤维组织中呈阳性。在早期动脉瘤病变中,随着内弹性膜的丧失,内皮下间隙中纤连蛋白以及I型和IV型胶原的线性染色消失。在早期动脉瘤病变的内膜增生中,纤连蛋白在内皮下间隙中呈强免疫染色,在增殖细胞周围增宽的细胞外间隙中呈弥漫性免疫染色。相比之下,I型和IV型胶原的染色稀疏或呈阴性。

结论

尽管目前关于纤连蛋白分布动态变化的研究结果并未证明在动脉瘤形成和修复过程中有任何因果关系,但这些免疫组织化学变化可能构成脑动脉瘤内膜内皮损伤及其后续恢复的关键后遗症。

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