Podocyte loss and albuminuria of KK-Ay mouse: A spontaneous animal model for human type 2 diabetic nephropathy

Podocyte loss was well known in type 2 diabetic nephropathy patients. The objective of the present study was to determine the number of podocytes and the degree of albuminuria in diabetic KK-Ay/Ta (KK-Ay) mice which had been reported as diabetic nephropathy model. Diabetic KK-Ay mice, diabetic KK/Ta mice and non-diabetic BALB/cA Jcl (BALB/cA) mice were studied. We analyzed glomerular lesions in all mice by morphometric analysis and immunofluorescence to determine the number of podocytes. Level of urinary albumin was also measured. Glomerular enlargement and mesangial expansion were observed in KK-Ay mice. Mean number of podocytes per glomerulus (NG pod) in diabetic KK-Ay mice was significantly lower than that in non-diabetic BALB/cA mice. Mean NG pod/glomerular area (GA) per glomerulus was also significantly decreased in diabetic KK-Ay mice. The level of urinary albumin/creatinine ratio (ACR) in diabetic KK-Ay mice was significantly higher than that in non-diabetic BALB/cA mice. These data suggest that podocyte loss might induce albuminuria in KK-Ay mice. This finding confirmed our previous report that KK-Ay mice, especially in terms of histological findings, are a suitable animal model for glomerular injury in type 2 diabetic nephropathy.

Influence of the period between onset of IgA nephropathy and medical intervention on renal prognosis

Background. The clinical course of IgA nephropathy (IgAN) is highly variable. In order to verify the necessity of early medical intervention in IgAN patients, the present study investigated the clinical impact of the duration between disease onset and first medical intervention on renal prognosis. Methods. We enrolled 57 patients diagnosed with IgAN on the basis of biopsy performed at our hospital. The medical records of these patients were traceable to the last 10 years, during which they had not undergone dialysis or treatment at any other hospital. On the basis of histological assessment of prognosis, these patients were classified according to the Japanese guidelines into the following groups: groups I, good prognosis;group II, relatively good prognosis;group III, relatively poor prognosis;and group IV, poor prognosis. We investigated the correlation between the duration of disease onset and the first consultation with a nephrologist and the rate of increase in serum creatinine over a 10 year period. In addition to the abovementioned patients, 6 patients with IgAN who underwent dialysis within the 10 years were separately evaluated. These patients came under the poor prognosis category;i.e., they belonged to group IV. Results. The duration between disease onset and medical consultation was significantly longer in younger patients or in those with asymptomatic proteinuria at onset when compared to that in older patients or in those with other urinary abnormalities. There was a significant correla tion between this duration and renal prognosis, particularly in group III patients. Although the duration between onset and consultation was not correlated to the serum creatinine level at the time of first medical intervention, urinary protein level among group IV patients at the time of first consultation was significantly higher in patients with dialysis than that in those without dialysis. Conclusions. Early medical intervention may lead to a better renal prognosis, particularly in group III patients, who form a major portion of the IgAN population. It therefore appears that early diagnostic screening and subsequent intervention are important for a good prognosis in IgAN patients.

Dimethylarginine Dimethylaminohydrolase 2 Gene Polymorphism and Its Association with Asymmetrical Dimethyl Arginine in Hemodialyzed Patients

Introduction:Patients with CKD have elevated plasma levels of Asymmetrical Dimethyl Arginine (ADMA), impaired EDRF/NO responses in isolated resistance vessels, and a marked increase in the frequency of cardiovascular events that are predicated by plasma levels of ADMA. ADMA is considered as a risk factor for endothelial dysfunction, progression of chronic kidney disease and a marked increase in the frequency of cardiovascular events that are predicated by plasma levels of ADMA. Elevated ADMA in CKD have been related to a combination of a reduced renal ADMA excretion and a reduced catabolism of ADMA by dimethylarginine dimethylaminohydrolase (DDAH). The current study was undertaken to determine whether there is a correlation between ADMA and SNPs at -449 DDAH 2.Subjects and Methods :It was a cross sectional analytic study, 56 hemodialysis patients and 30 healthy individuals were enrolled. Based on its etiology, HD patients group was further divided in to hypertension (HT) subgroup and non-HT subgroup. Genotyping of the polymorphisms was performed using PCR-based SNP detection methods based on 5’-exonuclease activity assays for rs805305.Results :Heterozygotes were observed as the most abundant genotypes in both groups, followed by GG genotype in the HD patients (30%) and CC (27%) healthy individuals. Among the HT subgroup, the mean plasma levels of ADMA were sequentially higher from genotypes CC, G/C and GG (p = 0.037). Further multiple comparisons between groups using post hoc test showed results that genotype GG and CC were different at 0.05 level of significance. These findings were not found among non HT subgroup.Conclusion: Genetic variation in the DDAH 2 genes is significantly associated with serum ADMA levels in hypertensive HD patients. We observed that carriage of a G at position -449 in the promoter region of the DDAH 2 gene is associated with higher ADMA levels.

晚期糖基化产物受体信号传导在羧甲赖氨酸诱导足细胞表达单核细胞趋化因子中的作用

目的了解足细胞上晚期糖基化产物受体(RAGE)激活后的细胞内信号的传导途径。方法激光共聚焦显微镜观察细胞内反应性氧自由基(ROS)的产生。Western印迹方法检测足细胞内丝裂原激活的蛋白激酶(MAPK)家族磷酸化,RT-PCR方法检测单核细胞趋化因子-1(MCP-1)的mRNA表达。结果足细胞细胞核内存在基础性的ROS,AGE和羧甲赖氨酸(carboxymethyllysine, CML)分别诱导细胞浆内ROS增加2.2和2.6倍。N-乙酰-L-半胱氨酸(NAC)抑制基础性和诱导性ROS形成,RAGE中和抗体则完全抑制诱导性的ROS产生。NAC也可直接抑制CML以及外源性H_2O_2诱导的MCP-1的表达。使用CML刺激足细胞10 min后,磷酸化细胞外信号调节激酶(ERK)增加3.8倍。而CML刺激足细胞120 min仍没有发现磷酸化的p38MAPK和应激活化蛋白激酶(SAPK)/氨基末端激酶(JNK)表达或上词。使用NAC,7氨4三氟甲基香豆素(AFC)可以完全防止ERK磷酸化并抑制MCP-1的mRNA表达。PD98059阻断了ERK磷酸化却并不能完全抑制MCP-1的mRNA的表达。结论足细胞上RAGE激活后,通过ROS-p21Ras-ERK信号途径诱导足细胞表达MCP-1。

糖基化终产物通过其受体诱导小鼠足细胞表达单核细胞趋化因子1

目的了解糖基化终产物(AGE)能否在体外诱导小鼠足细胞表达单核细胞趋化蛋白1(MCP-1)以及其受体RAGE在其中的作用。方法以RT-PCR和ELISA的方法检测AGE、羰甲基化白蛋白(CML)、S100蛋白和RAGE中和抗体对小鼠足细胞的MCP-1的基因和蛋白质表达的影响。结果(1)未分化和已分化的足细胞都能表达RAGE。(2)AGE和CML以剂量依赖的方式诱导足细胞表达MCP-1mRNA。AGE和CML孵育8h诱导足细胞产生MCP-1蛋白[分别为(7.44±1.01,8.06±0.96)ng/L],明显高于牛血清白蛋白(BSA)孵育的足细胞[(3.77±0.39)ng/L,均P<0.05],而孵育24hMCP-1的浓度分别为(87.78±9.32,85.35±9.83和17.95±0.76)ng/L(均P<0.01)。(3)RAGE的另外一个配体,S100蛋白,也能以剂量依赖的方式诱导足细胞表达MCP-1mRNA。RAGE中和抗体完全阻断了AGE、CML和S100的作用。结论AGE和CML通过RAGE使诱导分化的足细胞表达MCP-1。

普伐他汀抑制羧甲赖氨酸修饰白蛋白诱导足细胞表达单核细胞趋化蛋白1

目的研究普伐他汀对羧甲基赖氨酸修饰白蛋白（CML-BSA）诱导的小鼠足细胞单核细胞趋化蛋白1（MCP-1）表达的干预作用。方法使用RT-PCR和ELISA方法检测MCP-1的表达水平及细胞上清液MCP-1含量。共聚焦显微镜测量对二氯荧光黄敏感的细胞内活性氧（ROS）的产量。Western印迹法和免疫组化技术检测活化的细胞外信号调节蛋白激酶（ERK）、核因子κB（NF-κB）和转录因子Sp1的表达。结果CML-BSA呈时间和浓度依赖的方式诱导MCP-1的表达。0.1或1.0 mmol/L普伐他汀可抑制CML-BSA诱导的MCP-1 mRNA和蛋白的表达。CML-BSA可迅速诱导足细胞内ROS的生成。普伐他汀不影响细胞ROS生成。CML-BSA诱导足细胞磷酸化ERK（p-ERK）表达升高,而普伐他汀可以浓度依赖方式对此加以阻断。Western印迹法和免疫组化实验结果均提示普伐他汀预处理足细胞可以阻断CML-BSA诱导的NF-κB和Sp1的易位。结论普伐他汀能够通过调节足细胞内ERK、NF-κB和Sp1信号途径,阻断CML-BSA诱导MCP-1的表达。

转录因子Sp1和核因子κB调节小鼠足细胞单核细胞趋化蛋白1基因的转录

以往的研究发现羰甲基赖氨酸（CML）修饰的白蛋白可以通过足细胞上晚期糖麟化产物受体（RAGE）激活足细胞。阻断足细胞中活性氧（ROS）及p21Ras和抑制ERK1／2，对CML诱导足细胞表达单核细胞趋化蛋向（MCP）1基因的作用不同，提示可能有不同的信号途径诱导MCP-1基因表达。