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肾上腺皮质抑制会增加肾病综合征复发的风险。

Adrenocortical suppression increases the risk of relapse in nephrotic syndrome.

作者信息

Abeyagunawardena Asiri S, Hindmarsh Peter, Trompeter Richard S

机构信息

Department of Paediatrics, Faculty of Medicine, University of Peradeniya, Peradeniya, Sri Lanka.

出版信息

Arch Dis Child. 2007 Jul;92(7):585-8. doi: 10.1136/adc.2006.108985. Epub 2007 Feb 6.

Abstract

OBJECTIVE

Children with nephrotic syndrome (NS) are usually treated with long-term low dose alternate day prednisolone with or without glucocorticoid sparing therapy, such as levamisole or ciclosporin, to maintain remission. The degree of hypothalamic-pituitary-adrenal axis (HPA) suppression with such therapeutic strategies has not been studied systematically. HPA suppression could cause a relapse or adrenal crisis.

STUDY DESIGN

To study the risks of HPA suppression, a modified low dose synacthen test (0.5 mug) was administered to 32 patients (22 male,10 female) with a mean age of 9.7 years (range 3.8-17.6 years) with NS receiving long-term alternate day prednisolone for over 12 months. Twelve patients received alternate day prednisolone, 11 alternate prednisolone+levamisole and nine alternate prednisolone+ciclosporin. All patients were followed up for 3 years and the relapse rate noted.

RESULTS

20/32 (62.5%) patients had a peak serum cortisol concentration of <500 nmol/l, which suggested suboptimal cortisol secretion and possible HPA suppression. 10/12 children in the prednisolone group and 8/11 in the levamisole group had a suboptimal cortisol response compared with 2/9 in the ciclosporin group. During follow-up, the 20 children who had a suboptimal cortisol response had significantly more relapses (95 relapses) compared to the 12 children with a normal cortisol response who had 24 relapses (p = 0.01).

CONCLUSIONS

Children with NS receiving long-term alternate day prednisolone therapy are at risk of developing HPA suppression and should be evaluated using the modified synacthen test. Children with evidence of HPA suppression are at a greater risk of relapse.

摘要

目的

肾病综合征(NS)患儿通常采用长期低剂量隔日泼尼松龙治疗,联合或不联合糖皮质激素节约疗法,如左旋咪唑或环孢素,以维持缓解状态。目前尚未系统研究此类治疗策略对下丘脑 - 垂体 - 肾上腺轴(HPA)的抑制程度。HPA抑制可能导致复发或肾上腺危象。

研究设计

为研究HPA抑制的风险,对32例(22例男性,10例女性)平均年龄9.7岁(范围3.8 - 17.6岁)的NS患儿进行改良低剂量促肾上腺皮质激素试验(0.5μg),这些患儿接受长期隔日泼尼松龙治疗超过12个月。12例患儿接受隔日泼尼松龙治疗,11例接受隔日泼尼松龙 + 左旋咪唑治疗,9例接受隔日泼尼松龙 + 环孢素治疗。所有患儿随访3年并记录复发率。

结果

20/32(62.5%)例患儿血清皮质醇峰值浓度<500 nmol/l,提示皮质醇分泌欠佳及可能存在HPA抑制。泼尼松龙组10/12例儿童和左旋咪唑组8/11例儿童的皮质醇反应欠佳,而环孢素组为2/9例。随访期间,皮质醇反应欠佳的20例儿童复发次数(95次)明显多于皮质醇反应正常的12例儿童(24次复发,p = 0.01)。

结论

接受长期隔日泼尼松龙治疗的NS患儿有发生HPA抑制的风险,应采用改良促肾上腺皮质激素试验进行评估。有HPA抑制证据的患儿复发风险更高。

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