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正常小鼠和切-东(米色)小鼠肾脏β-葡萄糖醛酸酶的周转率

Turnover of kidney beta-glucuronidase in normal and Chédiak-Higashi (beige) mice.

作者信息

Swank R T, Brandt E J

出版信息

Am J Pathol. 1978 Sep;92(3):755-72.

Abstract

Kidney beta-glucuronidase turnover has been examined by specific antibody methods in normal C57BL/6J mice and in coisogenic C57BL/6J beige mice, an animal model for the human Chédiak-Higashi syndrome. No effect of the beige gene on the rate of glucuronidase synthesis was detected in either untreated or testosterone-treated mice. Moreover, glucuronidase of beige mice decayed relatively slowly in pulse labeling and in hormone withdrawal experiments. Direct measurements of secretion confirmed that both in the presence of testosterone and following its withdrawal, there was a threefold lower rate of secretion of kidney glucuronidase in beige mice. Following hormone withdrawal, the loss of glucuronidase activity in beige mice was biphasic, with the second more slowly turning over component apparently lost by a nonsecretory mechanism. This persistent nonsecreted glucuronidase activity was specifically associated with giant lysosomes in kidney proximal tubule cells near the corticomedullary border. Thus, there are two major populations of lysosomes in proximal tubule cells of beige mice. Cells of the outer cortex contain mainly morphologically normal lysosomes, and their lysosomal enzymes are secreted at near normal rates. However, lysosomal enzymes derived from the giant lysosomes of cells near the corticomedullary border are secreted either very slowly or not at all. The altered secretion of lysosomal enzymes from specific kidney cells of beige mice may serve as a model system for study of defective fusion of lysosomes with phagocytosed bacteria in cells of Chédiak-Higashi patients.

摘要

已通过特异性抗体方法在正常C57BL/6J小鼠和同基因C57BL/6J米色小鼠(人类切-东综合征的动物模型)中检测了肾脏β-葡萄糖醛酸酶的更新情况。在未处理或经睾酮处理的小鼠中,均未检测到米色基因对葡萄糖醛酸酶合成速率的影响。此外,在脉冲标记和激素撤除实验中,米色小鼠的葡萄糖醛酸酶降解相对较慢。分泌的直接测量结果证实,无论在睾酮存在时还是撤除后,米色小鼠肾脏葡萄糖醛酸酶的分泌速率均降低了三倍。激素撤除后,米色小鼠中葡萄糖醛酸酶活性的丧失呈双相性,第二个周转较慢的组分显然是通过非分泌机制丢失的。这种持续的非分泌性葡萄糖醛酸酶活性与皮质髓质交界处附近肾近端小管细胞中的巨大溶酶体特异性相关。因此,米色小鼠近端小管细胞中有两种主要的溶酶体群体。外皮质的细胞主要含有形态正常的溶酶体,其溶酶体酶以接近正常的速率分泌。然而,源自皮质髓质交界处附近细胞的巨大溶酶体的溶酶体酶分泌非常缓慢或根本不分泌。米色小鼠特定肾细胞中溶酶体酶分泌的改变可能作为一个模型系统,用于研究切-东患者细胞中溶酶体与吞噬细菌的融合缺陷。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a443/2018270/eea7b79ec23f/amjpathol00737-0201-a.jpg

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