Bazzi Claudio, Petrini Concetta, Rizza Virginia, Arrigo Girolamo, Napodano Pietro, Paparella Maria, D'Amico Giuseppe
Division of Nephrology and Dialysis and. Biochemical Laboratory, San Carlo Borromeo Hospital, Milan, Italy.
Nephrol Dial Transplant. 2002 Nov;17(11):1890-6. doi: 10.1093/ndt/17.11.1890.
The urinary excretion of N-acetyl-beta-glucosamynidase (NAG) is increased in subjects exposed to substances toxic for renal tubular cells. In experimental and human glomerular diseases, its increased excretion is probably due to the dysfunction of tubular epithelial cells induced by increased traffic of proteins in the tubular lumen. The first aim of this study was to evaluate whether NAG excretion is correlated not only with the amount of proteinuria but also with some proteinuric components which reflect both glomerular capillary wall damage (IgG) and an impairment of tubular reabsorption of microproteins (alpha(1) microglobulin). The second aim was to assess whether NAG excretion has a predictive value on functional outcome and response to therapy.
In 136 patients with primary glomerulonephritis [74 with idiopathic membranous nephropathy (IMN), 44 with primary focal segmental glomerulosclerosis (FSGS) and 18 with minimal change disease (MCD)] urinary NAG excretion was measured by a colorimetric method and expressed in units per gram of urinary creatinine.
Using univariate linear regression analysis NAG excretion in all 136 patients was significantly dependent on IgG excretion, 24-h proteinuria, fractional excretion of alpha(1) microglobulin (FE alpha(1)m) and diagnosis. Using multiple linear regression analysis, NAG excretion was significantly dependent only on IgG excretion and 24-h proteinuria. Limiting the analysis to 67 patients with nephrotic syndrome (NS) and baseline normal renal function, by multiple linear regression, NAG excretion was significantly dependent on IgG excretion (P=0.0004), 24-h proteinuria (P=0.0067) and FE alpha(1)-m (P=0.0032) (R(2)=0.63). In 66 patients with NS and normal baseline renal function (MCD 10 patients; FSGS 20 patients; IMN 36 patients), according to values below or above defined cut-offs (IMN, </= or >18 U/g urinary Cr; FSGS and MCD, </= or >24 U/g urinary Cr), NAG excretion predicted remission in 86 vs 27% of IMN patients (P=0.0002) and 77 vs 14% of FSGS patients (P=0.005). Progression to chronic renal failure (CRF) was 0 vs 47% in IMN patients (P=0.001) and 8 vs 57% in FSGS patients (P=0.03). Using Cox model, in IMN patients only NAG excretion (P=0.01, RR 5.8), but not 24-h proteinuria, predicted progression to CRF. All MCD patients had NAG excretion values below the chosen cut-off, and 90% of them developed remission. Response to immunosuppressive therapy was significantly different in patients with NAG excretion values below or above the cut-offs.
Urinary NAG excretion can be considered as a reliable marker of the tubulo-toxicity of proteinuria in the early stage of IMN, FSGS and MCD; the excretion values show a significant relationship with 24-h proteinuria, IgG excretion and FE alpha(1)m. Its determination may be a non-invasive, useful test for the early identification of patients who will subsequently develop CRF or clinical remission and responsiveness to therapy.
接触对肾小管细胞有毒性的物质的受试者,其N - 乙酰 - β - 氨基葡萄糖苷酶(NAG)的尿排泄量会增加。在实验性和人类肾小球疾病中,其排泄增加可能是由于肾小管腔内蛋白质流量增加导致肾小管上皮细胞功能障碍。本研究的首要目的是评估NAG排泄是否不仅与蛋白尿的量相关,还与一些反映肾小球毛细血管壁损伤(IgG)和微蛋白肾小管重吸收受损(α₁微球蛋白)的蛋白尿成分相关。第二个目的是评估NAG排泄对功能转归和治疗反应是否具有预测价值。
对136例原发性肾小球肾炎患者[74例特发性膜性肾病(IMN)、44例原发性局灶节段性肾小球硬化(FSGS)和18例微小病变病(MCD)],采用比色法测定尿NAG排泄量,并以每克尿肌酐的单位数表示。
采用单变量线性回归分析,所有136例患者的NAG排泄量显著依赖于IgG排泄量、24小时蛋白尿、α₁微球蛋白排泄分数(FEα₁m)和诊断。采用多变量线性回归分析,NAG排泄量仅显著依赖于IgG排泄量和24小时蛋白尿。将分析限于67例肾病综合征(NS)且基线肾功能正常的患者,通过多变量线性回归分析,NAG排泄量显著依赖于IgG排泄量(P = 0.0004)、24小时蛋白尿(P = 0.0067)和FEα₁ - m(P = 0.0032)(R² = 0.63)。在66例NS且基线肾功能正常的患者中(MCD 10例;FSGS 20例;IMN 36例),根据低于或高于定义的临界值(IMN,≤或>18 U/g尿肌酐;FSGS和MCD,≤或>24 U/g尿肌酐),NAG排泄量在86%的IMN患者中预测缓解,而在27%的患者中未缓解(P = 0.0002),在77%的FSGS患者中预测缓解,而在14%的患者中未缓解(P = 0.005)。IMN患者进展为慢性肾衰竭(CRF)的比例为0%,而在FSGS患者中为47%(P = 0.001),FSGS患者中为8%,而在57%的患者中进展(P = 0.03)。使用Cox模型,在IMN患者中,仅NAG排泄量(P = 0.01,RR 5.8),而非24小时蛋白尿,预测进展为CRF。所有MCD患者的NAG排泄量值均低于选定的临界值,其中90%患者病情缓解。NAG排泄量值低于或高于临界值的患者对免疫抑制治疗的反应有显著差异。
尿NAG排泄量可被视为IMN、FSGS和MCD早期蛋白尿肾小管毒性的可靠标志物;排泄量值与24小时蛋白尿、IgG排泄量和FEα₁m有显著关系。其测定可能是一种用于早期识别随后将发展为CRF或临床缓解以及对治疗有反应的患者的非侵入性有用检测方法。
