首页> 外文期刊>American Journal of Kidney Diseases: The official journal of the National Kidney Foundation >Glycoxidation-modified macrophages and lipid peroxidation products are associated with the progression of human diabetic nephropathy.
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Glycoxidation-modified macrophages and lipid peroxidation products are associated with the progression of human diabetic nephropathy.

机译:糖氧化修饰的巨噬细胞和脂质过氧化产物与人类糖尿病性肾病的进展有关。

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摘要

The aim of this study is to investigate the role of glomerular macrophages activated by glycoxidation and lipid peroxidation products in the progression of glomerular lesions in diabetic nephropathy. Renal biopsy samples from 43 patients with diabetes (age, 54 +/- 14 years) and 10 control cases were immunohistochemically examined for the expression of carboxymethyllysine (CML), a representative glycoxidative product; oxidized phosphatidylcholine (Ox-PC), a representative lipid peroxidation product; leukocyte common antigen (LCA); CD68; and macrophage scavenger receptor (MSR) class A. The severity of the diffuse lesions in each glomerulus was histologically graded from 0 to IV. When grade II and III lesions had Kimmelstiel-Wilson (KW) nodules, they were placed in a new category called grade III with KW nodules. The number of cells positive for CML, Ox-PC, LCA, CD68, and MSR was compared in different grades. The number of macrophages per glomerulus increased with the glomerular lesion grade and was highest in grade III with KW nodules. Conversely, the number of lymphocytes did not parallel the grade of glomerular lesions. Almost 50% of macrophages contained CML, and more than 40% of those were observed in exudative lesions, tuft adhesions, and at the periphery of KW nodules. Ox-PC accumulated in 50% of CML-positive macrophages, which coexpress MSR. Macrophages positive for CML and Ox-PC increased with the grade. Glomerular macrophages may be activated by glycoxidative and lipid peroxidation products through MSR and may have a role in the development of human diabetic glomerulosclerosis.
机译:这项研究的目的是研究糖化氧化和脂质过氧化产物激活的肾小球巨噬细胞在糖尿病肾病肾小球病变进展中的作用。对43例糖尿病患者(54 +/- 14岁)和10例对照患者的肾脏活检样本进行了免疫组织化学检查,以检测羧甲基赖氨酸(CML)(一种典型的糖氧化产物)的表达;氧化磷脂酰胆碱(Ox-PC),一种典型的脂质过氧化产物;白细胞共同抗原(LCA); CD68;在组织学上,每个肾小球弥漫性病变的严重程度在组织学上分级为0到IV。当II级和III级病变具有Kimmelstiel-Wilson(KW)结节时,它们被归为具有KW结节的新类别III级。比较了不同等级的CML,Ox-PC,LCA,CD68和MSR阳性的细胞数量。每个肾小球的巨噬细胞数目随着肾小球病变等级的增加而增加,在KW结节的Ⅲ级中最高。相反,淋巴细胞的数量与肾小球病变的程度不符。几乎50%的巨噬细胞含有CML,其中40%以上的巨噬细胞出现在渗出性病变,簇状粘连和KW结节周围。 Ox-PC在50%的CML阳性巨噬细胞中积累,它们共同表达MSR。 CML和Ox-PC阳性的巨噬细胞随等级增加。肾小球巨噬细胞可能通过MSR被糖氧化和脂质过氧化产物激活,并可能在人类糖尿病性肾小球硬化的发展中发挥作用。

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