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铜负荷大鼠中毒和耐受的细胞机制。III. 肾脏的超微结构变化及铜的定位

Cellular mechanisms of toxicity and tolerance in the copper-loaded rat. III. Ultrastructural changes and copper localization in the kidney.

作者信息

Fuentealba I C, Haywood S, Foster J

机构信息

Department of Veterinary Pathology, University of Liverpool, UK.

出版信息

Br J Exp Pathol. 1989 Oct;70(5):543-56.

Abstract

The distribution of copper and related changes have been studied in copper-loaded rat kidneys at the ultrastructural level by X-ray electron probe microanalysis, in order to clarify the pathogenesis of copper-induced damage and subsequent recovery in this organ. Male rats fed a high copper diet (1500 ppm) for 16 weeks were killed at intervals; their kidneys were removed and portions of kidney cortex fixed in 4% paraformaldehyde and 2% glutaraldehyde for electron microscopy: other samples were analysed for copper by AA spectrophotometry. Increasing copper accumulation was associated with progressive PCT cell disarray and characterized by irreversible nuclear damage coincident with the intranuclear accumulation of Cu, S, P, and Ca. Copper was also identified within structurally intact lysosomes associated with Zn and Fe (Type I lysosomes) or P and S (Type II lysosomes, putative Cu-MT). Subsequent copper decline and tubular recovery was associated with the facilitated lysosomal sequestration of copper and excretion of copper-containing cell products into the tubule lumina, Cu-MT and alpha-2 urinary protein-copper. The cytotoxicity of copper in the kidney, as well as the liver, is associated primarily with irreversible nuclear damage, whereas lysosomal copper sequestration protects the cell from injury.

摘要

为了阐明铜诱导的肾脏损伤及其后续恢复的发病机制,通过X射线电子探针显微分析在超微结构水平上研究了铜负荷大鼠肾脏中铜的分布及相关变化。给雄性大鼠喂食高铜饮食(1500 ppm)16周,定期处死;取出它们的肾脏,将部分肾皮质固定在4%多聚甲醛和2%戊二醛中用于电子显微镜检查:其他样本通过原子吸收分光光度法分析铜含量。铜积累的增加与近端小管细胞逐渐紊乱有关,其特征是与核内铜、硫、磷和钙的积累同时出现不可逆的核损伤。在与锌和铁相关的结构完整的溶酶体(I型溶酶体)或与磷和硫相关的溶酶体(II型溶酶体,推测为铜-金属硫蛋白)中也发现了铜。随后铜含量下降和肾小管恢复与溶酶体对铜的隔离促进以及含铜细胞产物排泄到肾小管腔、铜-金属硫蛋白和α-2尿蛋白-铜有关。铜在肾脏以及肝脏中的细胞毒性主要与不可逆的核损伤有关,而溶酶体对铜的隔离可保护细胞免受损伤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/37ed/2040601/789123f0dfe9/brjexppathol00149-0052-a.jpg

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