Bazzi Claudio, Rizza Virginia, Paparella Maria, Casellato Daniela, Napodano Pietro, Olivieri Giulia, D'Amico Giuseppe
Fondazione D'Amico per la Ricerca sulle Malattie Renali, Milan - Italy.
J Nephrol. 2009 May-Jun;22(3):387-96.
Several aspects of renoprotection by angiotensin-converting enzyme inhibitors (ACEi) in IgA nephropathy (IgAN) are poorly defined: factors affecting responsiveness, role of proteinuria components and histological lesions, and criteria to identify patients who may benefit from ACEi.
In an observational study of 140 IgAN patients (follow up 62 +/- 36 months), 73 untreated and 67 ACEitreated for 53 +/- 28 months, 9 baseline risk factors (RFs) (blood pressure, serum creatinine, proteinuria/day, fractional excretion of IgG [FEIgG] and alpha1-microglobulin, global and segmental [SS] glomerular sclerosis, tubulointerstitial damage and arteriolar hyalinosis [AH] score), each divided into 2 subgroups according to a cutoff with the highest sensitivity and specificity for progression, were evaluated for ability to predict renoprotection. Primary end point: end-stage renal disease (ESRD) and doubling of serum creatinine (sCr); secondary end point: increase >or=25% of sCr with last sCr >or=1.58 mg/dL; total progression: sum of end points.
Patients with RFs below cutoffs did not benefit from ACEi. All clinical and proteinuric and 2 histological RFs (SS, AH score) with values above cutoffs showed significant reduction of progression in ACEitreated vs. untreated patients; FEIgG showed the highest prediction of renoprotection: ESRD/sCrx2: 20% vs. 62% (p=0.0004); total progression: 40% vs. 85% (p=0.0003). By multivariate analysis, independent predictors of progression were FEIgG, sCr and no ACEi treatment. Proteinuria reduction from -100% to -30%, spontaneous or after ACEi treatment, did not affect progression in treated vs. untreated patients (19% vs. 13%, p=0.85). Patients with proteinuria increased or reduced <30% showed a reduction of total progression if ACEi-treated (15% vs. 77%, p=0.0002). Presence of 1 clinical or proteinuric RF above the cutoff may be a criterion to identify patients who may benefit from ACEi.
Renoprotection by ACEi is a multifactorial phenomenon: the best predictor of renoprotection is FEIgG, a marker of disruption of glomerular barrier to proteins; renoprotection depends not only on ability to reduce proteinuria, but probably also on antiinflammatory and antifibrotic activity.
血管紧张素转换酶抑制剂(ACEi)在IgA肾病(IgAN)中的肾脏保护作用的几个方面尚未明确:影响反应性的因素、蛋白尿成分和组织学病变的作用,以及识别可能从ACEi中获益的患者的标准。
在一项对140例IgAN患者的观察性研究中(随访62±36个月),73例未治疗患者和67例接受ACEi治疗53±28个月的患者,评估9个基线危险因素(RFs)(血压、血清肌酐、每日蛋白尿、IgG[FEIgG]和α1-微球蛋白的分数排泄、全球和节段性[SS]肾小球硬化、肾小管间质损伤和小动脉玻璃样变[AH]评分),每个因素根据对疾病进展具有最高敏感性和特异性的临界值分为2个亚组,以预测肾脏保护能力。主要终点:终末期肾病(ESRD)和血清肌酐(sCr)翻倍;次要终点:末次sCr≥1.58mg/dL时sCr升高≥25%;总进展:终点之和。
RFs低于临界值的患者未从ACEi中获益。所有临床、蛋白尿和2个组织学RFs(SS、AH评分)值高于临界值的患者,与未治疗患者相比,接受ACEi治疗的患者进展显著降低;FEIgG对肾脏保护的预测性最高:ESRD/sCrx2:20%对62%(p=0.0004);总进展:40%对85%(p=0.0003)。多因素分析显示,进展的独立预测因素为FEIgG、sCr和未接受ACEi治疗。蛋白尿从-100%降至-30%,无论是自发的还是ACEi治疗后,在治疗组和未治疗组患者中均不影响进展(19%对13%,p=0.85)。蛋白尿增加或减少<30%的患者,如果接受ACEi治疗,总进展会降低(15%对77%,p=0.0002)。存在1个高于临界值的临床或蛋白尿RFs可能是识别可能从ACEi中获益的患者的标准。
ACEi的肾脏保护是一种多因素现象:肾脏保护的最佳预测因素是FEIgG,它是肾小球蛋白质屏障破坏程度的标志物;肾脏保护不仅取决于降低蛋白尿的能力,还可能取决于抗炎和抗纤维化活性。
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