Wragg Ruth, Dias Renuka P, Barrett Timothy, McCarthy Liam
Department of Paediatric Surgery and Urology, Birmingham Children's Hospital, United Kingdom.
Department of Paediatric Endocrinology, Birmingham Children's Hospital, United Kingdom; Institutes of Metabolism and Systems Research, University of Birmingham, Birmingham, United Kingdom.
J Pediatr Surg. 2018 Feb;53(2):321-325. doi: 10.1016/j.jpedsurg.2017.11.025. Epub 2017 Nov 14.
Wolfram syndrome is a rare genetic defect in WFS1 or WSF2(CISD2). It includes diabetes mellitus and insipidis, sensorineural deafness, optic atrophy, but not bladder dysfunction. However, this has appeared a common finding in our national referral clinic, and we sought to quantify this problem.
Data were collected from a multidisciplinary team managing all Wolfram patients in the UK. The following was analyzed: age, date of non-invasive urodynamics (NIU), symptoms, bladder capacity, voided volume, post-void residual and uroflow pattern. Bladder capacity was given as percentage predicted bladder capacity (PBC). Bladders were divided into normal, overactive (OAB), and underactive (UAB). Symptoms, bladder behavior, and genotyping were correlated. Data were expressed as median (interquartile range).
Forty patients with Wolfram syndrome were identified, and 38 underwent NIU. This showed normal bladder function (n=4), OAB (n=9), UAB (n=25). Symptoms were present in only 11 children. The different patterns of bladder behavior (OAB vs. normal vs. UAB) were significantly associated with different %PBC (36 (29-59)% vs. 105 (93-233)% vs. 100 (77.5-337)%; p<0.001), and percentage emptying (100 (80-100)% vs. 100 (87-100)% vs. 69 (48-93)%; p<0.05). There was no association of genotype, symptoms and bladder behavior. Patients with megacystis were older: [13.4 (9.7-16.1) vs. 15.4 (13.9-18.7) years; p<0.05).
Bladder dysfunction is very common in Wolfram syndrome (~90%), but most children cope (symptoms ~30%). With time there is a significant progression to megacystis, which may represent an underlying neuropathic myogenic failure and is likely to require intervention in the future.
Level II (National cohort study of prognosis).
沃尔弗勒姆综合征是一种由WFS1或WSF2(CISD2)基因缺陷引起的罕见疾病。它包括糖尿病和尿崩症、感音神经性耳聋、视神经萎缩,但不包括膀胱功能障碍。然而,这在我们国家的转诊诊所已成为一个常见发现,我们试图对这一问题进行量化。
收集了来自英国管理所有沃尔弗勒姆综合征患者的多学科团队的数据。对以下内容进行了分析:年龄、无创尿动力学检查(NIU)日期、症状、膀胱容量、排尿量、排尿后残余尿量和尿流模式。膀胱容量以预测膀胱容量百分比(PBC)表示。膀胱分为正常、膀胱过度活动(OAB)和膀胱活动低下(UAB)。对症状、膀胱行为和基因分型进行了相关性分析。数据以中位数(四分位间距)表示。
共确定了40例沃尔弗勒姆综合征患者,其中38例接受了NIU检查。结果显示膀胱功能正常(n = 4)、OAB(n = 9)、UAB(n = 25)。只有11名儿童出现症状。不同的膀胱行为模式(OAB与正常与UAB)与不同的PBC百分比(36(29 - 59)%与105(93 - 233)%与100(77.5 - 337)%;p < 0.001)以及排空百分比(100(80 - 100)%与100(87 - 100)%与69(48 - 93)%;p < 0.05)显著相关。基因型、症状和膀胱行为之间无关联。巨膀胱患者年龄较大:[13.4(9.7 - 16.1)岁与15.4(13.9 - 18.7)岁;p < 0.05]。
膀胱功能障碍在沃尔弗勒姆综合征中非常常见(约90%),但大多数儿童能够应对(症状发生率约30%)。随着时间的推移,会显著进展为巨膀胱,这可能代表潜在的神经源性肌源性衰竭,未来可能需要干预。
二级(全国队列预后研究)。
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