儿童阿尔波特综合征晚期诊断的疗效分析:临床病例

S. Y. Volgina, N. A. Solovyeva, G. A. Kulakova, E. A. Kurmayeva, Liliya I. Mukhametdinova, E. L. Rashitova
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引用次数: 0

摘要

背景。阿尔波特综合征是一种系统性、遗传性、进行性疾病,其特点是由 IV 型胶原基因的致病变异引起肾小球基底膜的超微结构改变。使用血管紧张素转换酶抑制剂(ACEI)保护肾脏在微量血尿和/或白蛋白尿阶段是有效的。如果这类患者出现肾病综合征,治疗策略仍是讨论的主题。临床病例描述。患者被诊断为新生儿期蛋白尿,一个月大时出现血尿。6 岁时确诊为遗传性肾炎;当时服用了 ACEI,但蛋白尿仍在增加。8 岁半时,通过穿刺肾活检确诊为:IV 型胶原病,局灶节段性肾小球硬化。此外,还诊断出慢性双侧感音神经性听力损失和双侧近视散光。此外,还处方了西克洛孢素 A(125 毫克/天)。治疗 14 个月后,患者血液中的胱抑素 C、尿素、尿酸和胆固醇水平有所上升。将环孢素 A 的剂量减至 100 毫克/天后,这些指标有所下降,但蛋白尿却增加了。在患者 10 岁 2 个月时,为了加强肾保护治疗,医生给他开了血管紧张素 II 受体阻滞剂(坎地沙坦 8 毫克/天)。11 岁时,再次增加免疫抑制剂的剂量,导致估计肾小球滤过率下降,血液中的肌酐、胱抑素 C、尿素、胆固醇、尿酸和钾含量增加。这些变化被认为是环孢素依赖性的。环孢素 A 的剂量减至 125 毫克/天,从 14 岁起减至 100 毫克/天。在 15.5 岁时的随访中,慢性肾病没有恶化。结论阿尔波特综合征患儿在出现肾病综合征后开始接受肾脏保护治疗并不能阻止慢性肾病的发展。而相对大剂量的环孢素A虽然减少了蛋白尿,但却导致了肾毒性和环孢素依赖性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Analysis of the Treatment Efficacy in Late Diagnosis of Alport Syndrome in a Child: Clinical Case
Background. Alport syndrome is a systemic, hereditary, progressive disease characterized by ultrastructural changes in the glomerular basement membrane caused by pathogenic variants of type IV collagen genes. The use of angiotensin-converting enzyme inhibitors (ACEI) for nephroprotection is effective at the microhematuria and/or albuminuria stage. Treatment tactics in case of nephrotic syndrome development in such patients remains the subject of discussion. Clinical case description. The patient was diagnosed with proteinuria at the neonatal period and hematuria at the age of one month. The hereditary nephritis was diagnosed at the age of 6 years; the ACEI was administered, however, the proteinuria continued to increase. The diagnosis was confirmed at the age of 8.5 years via the puncture nephrobiopsy: collagenopathy, type IV, focal segmental glomerular sclerosis. Moreover, chronic bilateral sensorineural hearing loss and bilateral myopic astigmatism were diagnosed. Ciclosporin A (125 mg/day) was additionally prescribed. The increase in the cystatin C, urea, uric acid, cholesterol levels in blood was mentioned after 14 months of treatment. These parameters decreased after reducing cyclosporine A dose to 100 mg/day, however, proteinuria has increased. Angiotensin II receptor blocker (candesartan 8 mg/day) was prescribed to enhance nephroprotective therapy at the age of 10 years 2 months. Another increase of the immunodepressant dose was performed at the age of 11, it led to decrease in the estimated glomerular filtration rate and increase of creatinine, cystatin C, urea, cholesterol, uric acid, and potassium levels in the blood. These changes were considered as cyclosporine-dependent. The dose of cyclosporine A was reduced to 125 mg/day, and to 100 mg/day from the age of 14. There was no progression of chronic kidney disease at the follow-up at the age of 15.5 years. Conclusion. Nephroprotective treatment of a child with Alport syndrome initiated after the development of nephrotic syndrome did not stop the chronic kidney disease progression. Whereas relatively high doses of ciclosporin A have reduced proteinuria but led to nephrotoxicity and cyclosporin dependence.
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