IgA-nephropathy in children with alport syndrome

M. Aksenova, E. Stolyarevich, P. Povilaitite
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Abstract

BACKGROUND. The widespread use of genetic methods in clinical practice has shown that pathogenic variants in COL4A3, COL4A4, COL4A5 genes associated with Alport syndrome (AS) are detected in 10 % of sporadic and in 20 % of familial cases of IgA nephropathy (IgAN), which suggested a relationship between the two diseases. THE AIM was to determine the frequency and characteristics of the course of IgAN in children with AS. PATIENTS AND METHODS. A single-centre retrospective pilot study included 102 patients with AS. The inclusion criteria were: age 2-18 years, genetic and/or morphological confirmation of AS, availability of morphological data of pts. The comparison group included children and adolescents 2-18 years with morphologically confirmed primary IgAN; the exclusion criterion was the presence of AS-specific glomerular basement membrane changes. IgAN was classified according to the MESTC scale. Demographic (gender, age), clinical (arterial hypertension, AH) and laboratory data (proteinuria (Pr, mg/m2/day), (Schwartz eGFR, ml/min/1.73m2) at the time of the biopsy and at the last examination of patients were assessed. Arterial pressure ≥95‰ for sex, age, height was defined as AH. Pr >100 mg/m2/day, Pr≥500 mg/m2/day and Pr>1000 mg/m2/day were defined as proteinuria, high-level proteinuria and nephrotic level proteinuria, respectively. The statistic parametric and nonparametric methods were used ("Statistica 10", StatSoft Russia). RESULTS. IgAN was detected in 3 of 102 children with AS (q=0.03): 2 girls had heterozygous variants in COL4A3 and COL4A4, a boy had X-linked AS. Two patients had nephrotic proteinuria, 1 had SRNS at onset of IgAN. The comparison group included 25 children with IgAN (17M). Baseline patients age (9±4.2 vs 13±2.7 years), frequency of AH (q1=0.66 vs q2=0.28), eGFR decrease (q1=0.33 vs q2=0.44), eGFR level (91±24 vs 90.8±24 ml/ min/1.73 m2), morphological characteristics of IgAN did not differ significantly by groups; patients with AS were more likely to have nephrotic proteinuria (q1=1 vs q2=0.32, p=0.023). At follow-up (3.8±1.4 years), the groups were comparable in age (12.3±5.2 vs 15±1.8 years), AH frequency (q1=0.66 vs q2=0.5), eGFR level (87±16 vs 91±13 ml/min/1.73m2); children with AS had higher grade Pr (800[0;1150] vs 30[10;100] mg/m2/day, p=0.048) and more often had high-level Pr (q1=0.66 vs q2=0.06, p=0.006) at follow-up observation. The AS was associated with the development of nephrotic-level Pr at onset (r=0.41, p=0.008) and with high-level Pr (r=0.38, p=0.012) during follow-up. CONCLUSION. IgAN was detected in 3 % of children with AS. The presence of COL4A3, COL4A4, COL4A5 genes variants is associated with more pronounced proteinuria at the onset of IgAN and its preservation in the follow-up, and may be a risk factor for more severe course glomerulonephritis. The main limitations of the study: small sample size and duration of follow-up.
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alport综合征患儿iga肾病
背景。遗传方法在临床实践中的广泛应用表明,与Alport综合征(AS)相关的COL4A3, COL4A4, COL4A5基因的致病变异在10%的散发和20%的IgA肾病(IgAN)家族病例中检测到,这表明这两种疾病之间存在关联。目的是确定AS患儿IgAN病程的频率和特征。患者和方法。一项纳入102例AS患者的单中心回顾性先导研究。纳入标准为:年龄2-18岁,AS的遗传和/或形态学确认,患者形态学资料的可用性。对照组包括2-18岁形态学证实的原发性IgAN的儿童和青少年;排除标准是as特异性肾小球基底膜改变。根据MESTC分级对IgAN进行分类。评估患者在活检时和最后一次检查时的人口统计学(性别、年龄)、临床(动脉高血压、AH)和实验室数据(蛋白尿(Pr, mg/m2/day)、(Schwartz eGFR, ml/min/1.73m2)。动脉压≥95‰,性别、年龄、身高均为AH。Pr>100 mg/m2/day、Pr≥500 mg/m2/day和Pr>1000 mg/m2/day分别定义为蛋白尿、高水平蛋白尿和肾病水平蛋白尿。采用统计参数和非参数方法(“Statistica 10”,StatSoft Russia)。结果。102例AS患儿中有3例检测到IgAN (q=0.03),其中2例女孩有COL4A3和COL4A4杂合变异体,1例男孩有x连锁AS。2例患者有肾病性蛋白尿,1例患者在IgAN发作时出现SRNS。对照组为25例IgAN患儿(17M)。基线患者年龄(9±4.2 vs 13±2.7岁)、AH发病频率(q1=0.66 vs q2=0.28)、eGFR下降(q1=0.33 vs q2=0.44)、eGFR水平(91±24 vs 90.8±24 ml/ min/1.73 m2)、IgAN形态学特征各组间无显著差异;AS患者更容易发生肾病性蛋白尿(q1=1 vs q2=0.32, p=0.023)。在随访(3.8±1.4年)时,两组在年龄(12.3±5.2 vs 15±1.8岁)、AH频率(q1=0.66 vs q2=0.5)、eGFR水平(87±16 vs 91±13 ml/min/1.73m2)方面具有可比性;在随访观察中,AS患儿的Pr水平较高(800[0,1150]vs 30[10,100] mg/m2/day, p=0.048),且Pr水平较高(q1=0.66 vs q2=0.06, p=0.006)。AS与发病时肾水平Pr的发展(r=0.41, p=0.008)和随访期间高水平Pr的发展(r=0.38, p=0.012)相关。结论。3%的AS患儿检测到IgAN。COL4A3, COL4A4, COL4A5基因变异的存在与IgAN发病时更明显的蛋白尿及其在随访中的保存相关,并且可能是更严重的肾小球肾炎病程的危险因素。本研究的主要局限性:样本量小,随访时间长。
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