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首页> 外文期刊>Journal of Endocrinological Investigation: Official Journal of the Italian Society of Endocrinology >Kidney abnormalities in low density lipoprotein receptor associated protein knockout mice.
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Kidney abnormalities in low density lipoprotein receptor associated protein knockout mice.

机译:低密度脂蛋白受体相关蛋白敲除小鼠的肾脏异常。

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Mice lacking the LDL receptor associated protein (RAP) have a severe defect of thyroglobulin secretion into the colloid, associated with moderately increased serum TSH levels and histological features of early goiter. RAP is expressed also in renal proximal tubule cells, where it functions as a molecular chaperone for the endocytic receptor megalin, which is responsible for reabsorption of low molecular weight proteins from the glomerular filtrate. Here we investigated whether the thyroid phenotype in RAP knockout (KO) mice is associated with kidney alterations. By immunohistochemistry, we found that in RAP KO mice megalin expression on the apical membrane of renal proximal tubule cells was markedly reduced, with intracellular retention of the receptor. The reduced expression of megalin was associated with its impaired function. Thus, urinary protein concentrations and urinary protein excretion in 24 h were higher in RAP KO than in wild-type mice. Coomassie staining of urine samples revealed an increased intensity of low molecular mass bands in the urine of RAP KO mice, indicating that they had low molecular weight proteinuria. Therefore, we concluded that disruption of the RAP gene determines not only thyroid abnormalities, but also a severe defect of megalin expression and function in the kidney.
机译:缺乏LDL受体相关蛋白(RAP)的小鼠甲状腺球蛋白分泌到胶体中存在严重缺陷,与血清TSH水平和早期甲状腺肿的组织学特征适度增加有关。 RAP在肾近端肾小管细胞中也表达,在其中它作为内吞受体巨蛋白的分子伴侣,负责从肾小球滤出物中重吸收低分子量蛋白质。在这里,我们调查了RAP基因敲除(KO)小鼠中的甲状腺表型是否与肾脏改变有关。通过免疫组织化学,我们发现在RAP KO小鼠中,肾小管近端细胞顶膜上的巨蛋白表达显着降低,并在细胞内保留了受体。巨蛋白的表达减少与其功能受损有关。因此,RAP KO中24 h的尿蛋白浓度和尿蛋白排泄高于野生型小鼠。尿液样品的考马斯染色显示RAP KO小鼠尿液中低分子量带的强度增加,表明它们具有低分子量蛋白尿。因此,我们得出的结论是,RAP基因的破坏不仅决定甲状腺异常,而且决定肾脏中巨蛋白表达和功能的严重缺陷。

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