首页> 外文期刊>Journal of Lipid Research >Altered renal lipid metabolism and renal lipid accumulation in human diabetic nephropathy.
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Altered renal lipid metabolism and renal lipid accumulation in human diabetic nephropathy.

机译:改变肾脏脂质代谢和人糖尿病肾病中的肾脂积累。

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摘要

Animal models link ectopic lipid accumulation to renal dysfunction, but whether this process occurs in the human kidney is uncertain. To this end, we investigated whether altered renal TG and cholesterol metabolism results in lipid accumulation in human diabetic nephropathy (DN). Lipid staining and the expression of lipid metabolism genes were studied in kidney biopsies of patients with diagnosed DN (n = 34), and compared with normal kidneys (n = 12). We observed heavy lipid deposition and increased intracellular lipid droplets. Lipid deposition was associated with dysregulation of lipid metabolism genes. Fatty acid β-oxidation pathways including PPAR-α, carnitine palmitoyltransferase 1, acyl-CoA oxidase, and L-FABP were downregulated. Downregulation of renal lipoprotein lipase, which hydrolyzes circulating TGs, was associated with increased expression of angiopoietin-like protein 4. Cholesterol uptake receptor expression, including LDL receptors, oxidized LDL receptors, and acetylated LDL receptors, was significantly increased, while there was downregulation of genes effecting cholesterol efflux, including ABCA1, ABCG1, and apoE. There was a highly significant correlation between glomerular filtration rate, inflammation, and lipid metabolism genes, supporting a possible role of abnormal lipid metabolism in the pathogenesis of DN. These data suggest that renal lipid metabolism may serve as a target for specific therapies aimed at slowing the progression of glomerulosclerosis.
机译:动物模型将异位脂质积累与肾功能不全,但在人肾是否发生这种过程是不确定的。为此,我们研究了是否改变了肾TG和胆固醇代谢的改变导致人类糖尿病肾病(DN)中的脂质积累。脂质染色和脂质代谢基因的表达在诊断为DN(n = 34)的患者的肾脏活组织检查中,与正常肾(n = 12)进行比较。我们观察到重脂沉积和细胞内脂滴增加。脂质沉积与脂质代谢基因的失衡有关。下调包括PPAR-α,肉氨基氨酰氨酰转移酶1,酰基-CoA氧化酶和L-FABP的脂肪酸β-氧化途径。水解循环Tgs的肾脂蛋白脂肪酶的下调与血管发成素样蛋白的表达增加有关。胆固醇吸收受体表达,包括LDL受体,氧化的LDL受体和乙酰化的LDL受体,显着增加,而下调基因效应胆固醇流出,包括ABCA1,ABCG1和Apoe。肾小球过滤速率,炎症和脂质代谢基因之间存在非常显着的相关性,支持异常脂质代谢在DN的发病机制中的可能作用。这些数据表明肾脂质代谢可以作为旨在减缓肾小球粥样硬化进展的特定疗法的靶标。

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