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X射线诱发的白内障先于晶状体上皮细胞(LEC)丢失,并与皮质DNA和活性氧(ROS)的积累同时发生;这与年龄相关性白内障相似。

X-ray induced cataract is preceded by LEC loss, and coincident with accumulation of cortical DNA, and ROS; similarities with age-related cataracts.

作者信息

Pendergrass William, Zitnik Galynn, Tsai Ryan, Wolf Norman

机构信息

Department of Pathology, University of Washington School of Medicine, Seattle, WA 98195, USA.

出版信息

Mol Vis. 2010 Aug 6;16:1496-513.

Abstract

PURPOSE

To compare age-related cataractous (ARC) changes in unirradiated mice lenses to those induced by head-only X-irradiation of 3 month-old mice.

METHODS

lens epithelial cells (LECs) as well as partially degraded cortical DNA were visualized in fixed sections using 4',6-diamidino-2-phenylindole (DAPI) staining, and in fresh lenses using the vital stain Hoechst 33342. reactive oxygen species (ROS) activity was also visualized directly in fresh lenses using the vital dye Dihydrorhodamine (DHR). In fixed lenses an antibody specific for 8-OH Guanosine (8-OH-G) lesions was used to visualize DNA oxidative adducts from ROS damage. Alpha smooth muscle actin was visualized using specific antibodies to determine if myofibroblasts were present. Fluorescence was quantified using Laser Scanning Confocal Microscopy (LSCM). The degree of lens opacity and cataract formation was determined by slit lamp, or from digitalized images of light reflections taken with a low magnification light microscope.

RESULTS

Using DNA- and ROS-specific vital fluorescent dyes, and laser scanning confocal microscopy we have previously described 4 changes in the aging rodent lenses: 1) a significantly decreased density of surface LECs in lenses from old compared to younger mice and rats; 2) a very large increase in retained cortical nuclei and DNA fragments in the secondary lens fibers of old rodent lenses; 3) increased cortical ROS in old rodent lenses; 4) increased cataract concomitantly with the cortical DNA and ROS increases. In the current study we report that these same 4 changes also occur in an accelerated fashion in mice given head-only X-irradiation at 3 months of age. In addition to vital staining of fresh lenses, we also examined sections from fixed eyes stained with DAPI or hematoxylin and eosin (H&E) and found the same loss of surface LECs and accumulation of undigested nuclei and debris in secondary lens fibers occur with age or following X-irradiation. In addition sections from fixed-eyes were examined for ROS damage to DNA with antibodies specific for 8-OH-G lesions. The frequency of 8-OH-G lesions increased dramatically in lenses from old unirradiated mice over 24 months of age, and similarly in X-irradiated lenses by 9-11 months post irradiation. The accumulation of cortical nuclei was not the result of conversion or invasion by myofibroblasts as tested by antibodies to a marker for such cells, alpha smooth muscle actin.

CONCLUSIONS

X-irradiation damage induces a large decrease in surface LECs over a period of 3-11 months post X-irradiation of young mice. These changes are similar in extent to those seen in 24-29 months-old control mouse lenses with age-related cataracts. In 24+ month-old unirradiated mice the secondary lens fibers are not able to degrade nuclei or nuclear DNA efficiently and accumulate large numbers of cortical nuclei and nuclear fragments as well as ROS and 8-OHG lesions. X-irradiated lenses develop the same abnormalities in a more accelerated fashion. The extensive loss of LECS and accumulation of undegraded nuclei, ROS, and ROS damage may play a causal role in cataract generation in both unirradiated old mice and in previously irradiated young adult mice.

摘要

目的

比较未受辐射的小鼠晶状体中与年龄相关的白内障(ARC)变化和3月龄小鼠头部X射线照射诱导的变化。

方法

使用4′,6-二脒基-2-苯基吲哚(DAPI)染色在固定切片中观察晶状体上皮细胞(LEC)以及部分降解的皮质DNA,使用活性染料Hoechst 33342在新鲜晶状体中观察。还使用活性染料二氢罗丹明(DHR)在新鲜晶状体中直接观察活性氧(ROS)活性。在固定的晶状体中,使用针对8-羟基鸟苷(8-OH-G)损伤的特异性抗体观察ROS损伤导致的DNA氧化加合物。使用特异性抗体观察α平滑肌肌动蛋白,以确定是否存在肌成纤维细胞。使用激光扫描共聚焦显微镜(LSCM)对荧光进行定量。通过裂隙灯或用低倍光学显微镜拍摄的光反射数字化图像确定晶状体混浊程度和白内障形成情况。

结果

使用DNA和ROS特异性活性荧光染料以及激光扫描共聚焦显微镜,我们之前描述了衰老啮齿动物晶状体中的4种变化:1)与年轻小鼠和大鼠相比,老年小鼠和大鼠晶状体中表面LEC的密度显著降低;2)老年啮齿动物晶状体次级晶状体纤维中保留的皮质细胞核和DNA片段大幅增加;3)老年啮齿动物晶状体中皮质ROS增加;4)白内障随着皮质DNA和ROS的增加而增加。在当前研究中,我们报告在3月龄接受头部X射线照射的小鼠中,同样的4种变化也以加速的方式出现。除了对新鲜晶状体进行活性染色外,我们还检查了用DAPI或苏木精和伊红(H&E)染色的固定眼睛切片,发现随着年龄增长或X射线照射后,表面LEC同样会丢失,次级晶状体纤维中未消化的细胞核和碎片会积累。此外,用针对8-OH-G损伤的特异性抗体检查固定眼睛的切片,以检测ROS对DNA的损伤。在24个月以上未受辐射的老年小鼠晶状体中,8-OH-G损伤的频率显著增加,在照射后9 - 11个月的X射线照射晶状体中也是如此。通过针对此类细胞标志物α平滑肌肌动蛋白的抗体检测,皮质细胞核的积累不是肌成纤维细胞转化或侵入的结果。

结论

X射线照射损伤在幼年小鼠接受X射线照射后的3 - 11个月内导致表面LEC大幅减少。这些变化的程度与24 - 29月龄患有年龄相关性白内障的对照小鼠晶状体中观察到的变化相似。在24个月以上未受辐射的小鼠中,次级晶状体纤维不能有效地降解细胞核或核DNA,积累了大量皮质细胞核和核碎片以及ROS和8-OHG损伤。X射线照射的晶状体以更加速的方式出现相同的异常。LEC的广泛丢失以及未降解细胞核、ROS和ROS损伤的积累可能在未受辐射的老年小鼠和先前接受照射的年轻成年小鼠的白内障形成中起因果作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c8b0/2925908/835b9aa61c47/mv-v16-1496-f1.jpg

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