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通过共聚焦激光扫描显微镜观察糖尿病和半乳糖血症大鼠晶状体皮质组织的液化情况。

Liquefaction of cortical tissue in diabetic and galactosemic rat lenses defined by confocal laser scanning microscopy.

作者信息

Bond J, Green C, Donaldson P, Kistler J

机构信息

School of Biological Sciences, University of Auckland, New Zealand.

出版信息

Invest Ophthalmol Vis Sci. 1996 Jul;37(8):1557-65.

PMID:8675398
Abstract

PURPOSE

To investigate whether a histologic link exists between osmotic fiber cell swelling and cortical tissue liquefaction in experimentally induced diabetic and galactosemic cataractogenesis of the rat lens.

METHODS

Confocal laser scanning microscopy, in conjunction with specific membrane labels and correlative transmission electron microscopy, was used to image large cortical areas with precise definition of the individual cells.

RESULTS

In both cataract models, tissue liquefaction--defined as the disintegration of tissue and the appearance of large fluid-filled spaces--typically was limited to a discrete zone in the lens cortex. The borders of the liquefaction zone were characterized by transitions between normal-appearing cells and swollen cells, which gained in size as plasma membranes ruptured and cytoplasmic contents fused and ultimately burst, thereby contributing to the formation of large fluid-filled spaces. During cataractogenesis, before tissue liquefaction became evident, selected fiber cells appeared swollen and accumulated specifically in the zone destined for tissue liquefaction. With increasing duration of diabetes or galactosemia, swollen fiber cells in this zone became more frequent and enlarged, resulting first in tissue disorder and then in tissue disintegration and the formation of large fluid-filled spaces.

CONCLUSIONS

New imaging protocols strongly support a direct involvement of lens fiber cell swelling in the liquefaction of cortical tissue. The appearance of swollen fiber cells in the lens cortex, therefore, can be used as an early indicator of the histopathology of sugar cataractogenesis.

摘要

目的

研究在实验诱导的大鼠晶状体糖尿病性和半乳糖性白内障形成过程中,渗透性纤维细胞肿胀与皮质组织液化之间是否存在组织学联系。

方法

共聚焦激光扫描显微镜结合特定的膜标记物以及相关的透射电子显微镜,用于对大的皮质区域进行成像,精确界定单个细胞。

结果

在两种白内障模型中,组织液化(定义为组织解体和出现大的充满液体的空间)通常局限于晶状体皮质中的一个离散区域。液化区的边界特征是正常细胞与肿胀细胞之间的过渡,随着质膜破裂、细胞质内容物融合并最终破裂,细胞体积增大,从而导致形成大的充满液体的空间。在白内障形成过程中,在组织液化明显之前,选定的纤维细胞出现肿胀,并特别聚集在注定要发生组织液化的区域。随着糖尿病或半乳糖血症持续时间的增加,该区域肿胀的纤维细胞变得更加频繁且体积增大,首先导致组织紊乱,然后导致组织解体并形成大的充满液体的空间。

结论

新的成像方案有力地支持晶状体纤维细胞肿胀直接参与皮质组织的液化。因此,晶状体皮质中肿胀纤维细胞的出现可作为糖性白内障形成组织病理学的早期指标。

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