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肾病综合征中蛋白尿选择性和肾小管间质损伤的现代研究方法

A modern approach to selectivity of proteinuria and tubulointerstitial damage in nephrotic syndrome.

作者信息

Bazzi C, Petrini C, Rizza V, Arrigo G, D'Amico G

机构信息

Division of Nephrology and Dialysis, Biochemical Laboratory, San Carlo Borromeo Hospital, Milan, Italy.

出版信息

Kidney Int. 2000 Oct;58(4):1732-41. doi: 10.1046/j.1523-1755.2000.00334.x.

Abstract

BACKGROUND

The selectivity of proteinuria, introduced in clinical nephrology in 1960 and useful in predicting steroid responsiveness in nephrotic syndrome, found little place in clinical practice in subsequent decades, since its assessment did not appear to help predict histologic diagnosis or determine prognosis. The amount of proteinuria and the degree of tubulointerstitial damage appeared to be better predictors of functional outcome. A correlation between them has been found, referred to some toxicity of proteinuria on tubular cells, but so far no single feature or component of proteinuria has been identified as being responsible for this toxicity.

METHODS

We evaluated 89 patients with nephrotic syndrome [9 with minimal change disease (MCD), 29 with primary focal segmental glomerulosclerosis (FSGS), and 51 with idiopathic membranous glomerulonephritis (MGN)] to determine if the selectivity of proteinuria was associated with tubulointerstitial damage. A semiquantitative grading of histologic lesions and qualitative evaluation of the "tubular" component of proteinuria expressed as a pattern of sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE) and as fractional excretion of the low molecular weight (LMW) protein alpha1-microglobulin (FE alpha1m) were used. A second aim of the study was to assess the predictive value on functional outcome [remission or progression to chronic renal failure (CRF)] and response to therapy of the selectivity of proteinuria, considered alone and in combination with FE alpha1m.

RESULTS

Proteinuria was classified as highly selective [selectivity index (SI) < or = 0.10, N = 15], moderately selective (SI > or = 0.11 < or = 0.20, N = 34), or nonselective (SI > or = 0.21, N = 40). A significant relationship was found between the SI and the histologic degree of tubulointerstitial damage (score 0 to 1 vs. score > or =2, P = 0.000), severity of the tubular component of proteinuria (mixed SDS-PAGE pattern with LMW proteins not lower than 23 kD vs. mixed pattern with LMW proteins up to 20 to 10 kD, P = 0.000), and FE alpha1m (values below vs. above a defined cut-off, P = 0.000). The functional outcome was evaluated in 60 patients with baseline normal renal function (serum creatinine 0.97 +/- 0.19 mg/dL). The patients with high, moderate, or nonselective proteinuria had 100, 50, and 29% of complete or partial remission (P = 0.0001) and 0, 25, and 35% of progression to CRF, respectively (P = 0.050). In 45 patients with moderately selective (N = 28) and nonselective (N = 17) proteinuria, according to some arbitrary cutoffs for FE alpha1m (MGN, < or = vs. > 0. 240% of creatinine clearance; FSGS and MCD, < or = vs. > 0.350%), the remission rate was 62 versus 6% in patients with FE alpha1m below or above the cutoffs (P = 0.0001), and progression to CRF was 7 and 69%, respectively (P = 0.0001). The response to therapy (complete or partial remission at the last observation), evaluated retrospectively in 40 patients, was 100, 67, and 33% in high, moderate, and nonselective proteinuria (P = 0.0002); in 30 patients with moderate and nonselective proteinuria, according to an FE alpha1m value that was < or = or > the cutoffs, the response rate was 75 versus 10% (P = 0.001).

CONCLUSIONS

There is a significant relationship between selectivity of proteinuria and tubulointerstitial damage. Moreover, the selectivity of proteinuria has a predictive value on functional outcome. When proteinuria is highly selective, the tubulointerstitial damage is rather infrequent, and 100% of patients develop clinical remission. When proteinuria is moderately selective or nonselective, increasing numbers of patients develop tubulointerstitial damage; in these patients, the functional outcome and response to therapy is partly dependent on tubulointerstitial involvement, and the best predictor of functional outcome is the combination of SI and FE alpha1m.

摘要

背景

蛋白尿选择性于1960年引入临床肾脏病学,对预测肾病综合征的类固醇反应性有用,但在随后几十年的临床实践中却很少应用,因为其评估似乎无助于预测组织学诊断或判断预后。蛋白尿的量和肾小管间质损伤程度似乎是功能转归的更好预测指标。已发现二者之间存在相关性,这与蛋白尿对肾小管细胞的某些毒性有关,但迄今为止,尚未确定蛋白尿的单一特征或成分是造成这种毒性的原因。

方法

我们评估了89例肾病综合征患者[9例微小病变病(MCD)、29例原发性局灶节段性肾小球硬化(FSGS)和51例特发性膜性肾小球肾炎(MGN)],以确定蛋白尿选择性是否与肾小管间质损伤相关。采用组织学病变的半定量分级以及以十二烷基硫酸钠 - 聚丙烯酰胺凝胶电泳(SDS - PAGE)图谱和低分子量(LMW)蛋白α1 - 微球蛋白的分数排泄(FEα1m)表示的蛋白尿“肾小管”成分的定性评估。该研究的第二个目的是评估蛋白尿选择性单独及与FEα1m联合对功能转归[缓解或进展至慢性肾衰竭(CRF)]及治疗反应的预测价值。

结果

蛋白尿分为高度选择性[选择性指数(SI)≤0.10,n = 15]、中度选择性(SI≥0.11≤​0.20,n = 34)或非选择性(SI≥0.21,n = 40)。发现SI与肾小管间质损伤的组织学程度(评分0至1 vs.评分≥2,P = 0.000)、蛋白尿肾小管成分的严重程度(LMW蛋白不低于23 kD的混合SDS - PAGE图谱与LMW蛋白高达20至10 kD的混合图谱,P = 0.000)以及FEα1m(低于或高于定义的临界值,P = 0.000)之间存在显著关系。对60例基线肾功能正常(血清肌酐0.97±0.19 mg/dL)的患者评估了功能转归。高度、中度或非选择性蛋白尿患者的完全或部分缓解率分别为100%、50%和29%(P = 0.0001),进展至CRF的比例分别为0%、25%和35%(P = 0.050)。在45例中度选择性(n = 28)和非选择性(n = 17)蛋白尿患者中,根据FEα1m的一些任意临界值(MGN,肌酐清除率≤​或> 0.240%;FSGS和MCD,≤​或> 0.350%),FEα1m低于或高于临界值的患者缓解率分别为62%和6%(P = 0.0001),进展至CRF的比例分别为7%和69%(P = 0.0001)。对40例患者进行回顾性评估的治疗反应(最后一次观察时的完全或部分缓解),高度、中度和非选择性蛋白尿患者分别为100%、67%和33%(P = 0.0002);在30例中度和非选择性蛋白尿患者中,根据FEα1m值≤​或>临界值,反应率分别为75%和10%(P = 0.001)。

结论

蛋白尿选择性与肾小管间质损伤之间存在显著关系。此外,蛋白尿选择性对功能转归具有预测价值。当蛋白尿高度选择性时,肾小管间质损伤相当少见,100%的患者出现临床缓解。当蛋白尿为中度选择性或非选择性时,发生肾小管间质损伤的患者数量增加;在这些患者中,功能转归和治疗反应部分取决于肾小管间质受累情况,功能转归的最佳预测指标是SI和FEα1m的联合。

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