Callea F, Gregorini G, Sinico A, Consalez G G, Bossolasco M, Salvidio G, Radice A, Tira P, Candiano G, Rossi G, Petti A, Ravera G, Ghiggeri G, Gusmano R
Department of Pathology, Spedali Civili, Brescia, Italy.
Eur J Clin Invest. 1997 Aug;27(8):696-702. doi: 10.1046/j.1365-2362.1997.1720717.x.
A high incidence of alpha 1-antitrypsin (AAT) deficiency has been reported in patients with C-ANCA systemic vasculitis in association with antibodies against proteinase-3 (PR3). To clarify the role of AAT deficiency in the acute vasculitic process as well as in progression of the disease, we studied 84 patients with either C-ANCA or P-ANCA vasculitis with special reference to: (a) the AAT gene, (b) the phenotypic (Pi) variants and (c) the serum levels during both acute illness and remission. The PiZ gene was found in six patients (8% vs. 1.5% controls) irrespective of the type of autoantibodies (C-ANCA vs. P-ANCA). All PiZ patients displayed the ability to raise their AAT serum levels up to the normal range during acute illness. In contrast, 24 patients with the PiM phenotype presented low AAT serum levels during acute illness. In all these patients, the AAT levels returned to normal values during the remission. Low AAT levels were associated with low levels of C-reactive protein (PCR) (P < 0.001), with a less severe renal involvement or a minor risk of death, and, in one tested patient, with a novel point mutation (TCGA-->TCAA) at the enhancer-promoter region of the AAT gene. Low AAT serum levels did not correlate with either type/titre of autoantibody or distribution/severity of the vasculitis process. In the case-control study, high AAT levels emerged as a major determinant of progression towards end-stage renal failure [odds ratio 3 (95% CI 1.1-8.4)]. These results indicate: (a) a high incidence of the PiZ gene of AAT in systemic vasculitis irrespective of the type of autoantibodies; (b) a novel form of AAT deficiency associated with the normal PiM phenotype becoming manifest only during acute illness; (c) dysregulation of the acute-phase response affecting selectively AAT or both AAT and PCR; (d) correlation between low plasma levels of AAT and less severe renal involvement or risk of death.
据报道,在伴有抗蛋白酶3(PR3)抗体的C-ANCA系统性血管炎患者中,α1-抗胰蛋白酶(AAT)缺乏症的发生率很高。为了阐明AAT缺乏在急性血管炎过程以及疾病进展中的作用,我们研究了84例C-ANCA或P-ANCA血管炎患者,特别关注:(a)AAT基因,(b)表型(Pi)变体,以及(c)急性疾病和缓解期的血清水平。无论自身抗体类型(C-ANCA与P-ANCA)如何,在6例患者中发现了PiZ基因(8%对比1.5%的对照组)。所有PiZ患者在急性疾病期间都有能力将其AAT血清水平提高到正常范围。相比之下,24例具有PiM表型的患者在急性疾病期间AAT血清水平较低。在所有这些患者中,AAT水平在缓解期恢复到正常水平。低AAT水平与低水平的C反应蛋白(PCR)相关(P<0.001),与肾脏受累较轻或死亡风险较小相关,并且在一名受试患者中,与AAT基因增强子-启动子区域的一个新的点突变(TCGA→TCAA)相关。低AAT血清水平与自身抗体的类型/滴度或血管炎过程的分布/严重程度均无相关性。在病例对照研究中,高AAT水平是进展至终末期肾衰竭的主要决定因素[比值比3(95%CI 1.1-8.4)]。这些结果表明:(a)无论自身抗体类型如何,系统性血管炎中AAT的PiZ基因发生率都很高;(b)一种与正常PiM表型相关的新型AAT缺乏形式,仅在急性疾病期间才会显现;(c)急性期反应失调,选择性地影响AAT或同时影响AAT和PCR;(d)血浆AAT水平低与肾脏受累较轻或死亡风险之间的相关性。
