A case of a mild Wolfram Syndrome with concomitant ATP7B mutation.

CellR4-- repair, replacement, regeneration, & reprogramming Pub Date : 2019-01-01 Epub Date: 2019-08-28 DOI:10.32113/cellr4_20198_2735

R Squitti, G Cerchiaro, I Giovannoni, P Francalanci, M Siotto, P Maffei, C Ricordi, M C Rongioletti

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引用次数: 2

Abstract

Background: Wolfram Syndrome 1 (WS1) has been characterized on the basis of mutation in the WFS1 gene encoding a calcium storage wolframin endoplasmatic reticulum transmembrane glycoprotein.

Patients and methods: We observed a WS 10-years old female subject, with Type 1 diabetes-mellitus (DM), that had compound heterozygous WSF1 mutations but without other symptoms generally observed in WS subjects, such as optic atrophy or neurodegeneration.

Results: Decreased copper, ceruloplasmin, and transferrin levels, pointing to a copper deficiency, were associated with a new c.18703A>G mutation in the ATP7B gene, while lower calcium levels were associated with WSF1 mutations. An omega-3 fatty acids therapy was administrated to the subject in the attempt to ameliorate diabetes symptoms, restored copper deficiency, and normal calcium levels.

Conclusions: This specific case report provides new insights into the potential interplay of ATP7B mutation in shaping a milder WS clinical picture.

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伴有ATP7B突变的轻度Wolfram综合征1例。

背景:Wolfram综合征1 (WS1)的特征是编码钙储存Wolfram内质网跨膜糖蛋白的WFS1基因突变。患者和方法:我们观察了一名10岁的WS女性受试者，患有1型糖尿病(DM)，她有WSF1复合杂合突变，但没有WS受试者通常观察到的其他症状，如视神经萎缩或神经变性。结果:铜、铜蓝蛋白和转铁蛋白水平降低，表明铜缺乏，与ATP7B基因中新的c.18703A>G突变有关，而钙水平降低与WSF1突变有关。为了改善糖尿病症状，恢复缺铜和正常钙水平，对受试者进行了omega-3脂肪酸治疗。结论:这一特殊的病例报告为ATP7B突变在形成较温和的WS临床图景中的潜在相互作用提供了新的见解。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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CellR4-- repair, replacement, regeneration, & reprogramming

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