血清基质金属蛋白酶-9（MMP9）和淀粉样β蛋白前体（APP）作为Fragile-X综合征儿童的潜在生物标志物：一项横断面研究。

IF 2.5 3区医学 Q2 MEDICAL LABORATORY TECHNOLOGY Clinical biochemistry Pub Date : 2023-10-04 DOI:10.1016/j.clinbiochem.2023.110659

Mohamed H.Y. Bekheet , Lamiaa A. Mansour , Rasha H. Elkaffas , Mona A. Kamel , Mohamed A. Elmonem

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引用次数: 0

摘要

简介：脆性X综合征（FXS）是一种神经系统疾病，由FMR1基因5'非翻译区的异常重复导致脆性X信使核糖核蛋白-1（FMRP）缺陷引起。尽管它在儿童中相对常见，但通常诊断不足，尤其是在没有常规进行基因筛查的发展中国家。到目前为止，FXS缺乏一种可用于筛查、严重程度评分或潜在新治疗方法的治疗监测的实验室生物标志物。方法：招募110名受试者；80名疑似FXS的男性儿童和30名匹配的健康儿童。我们评估了血清基质金属蛋白酶-9（MMP9）和淀粉样蛋白β蛋白前体（APP）作为FXS潜在生物标志物的临床应用。结果：在80名疑似儿童中，14名儿童具有完全突变，8名儿童具有预突变，58名儿童具有正常基因型。不同基因型儿童在发病年龄（P=0.658）、主要临床表现（P=0.388）、临床严重程度评分（P=0.799）、，患者的病程（P=0.719）和智力残疾（P=0.351）。MMP9和APP在比较不同基因型亚组时显示出统计学上的显著差异（在临床环境中发现FXS病例的P=0.019和95%。结论：在没有FXS基因诊断的情况下筛查循环生物标志物是合理的。我们的研究首次在临床环境下评估疑似FXS儿童的MMP9和APP，并评估它们与疾病表现和严重程度的相关性。

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Serum matrix metalloproteinase-9 (MMP9) and amyloid-beta protein precursor (APP) as potential biomarkers in children with Fragile-X syndrome: A cross sectional study

Introduction

Fragile-X syndrome(FXS) is a neurological disease caused by abnormal repeats in the 5′untranslated region of the FMR1 gene leading to a defective fragile-X-messenger-ribonucleoprotein-1 (FMRP). Although relatively common in children, it is usually under-diagnosed especially in developing countries where genetic screening is not routinely practiced. So far, FXS lacks a laboratory biomarker that can be used for screening, severity scoring or therapeutic monitoring of potential new treatments.

Methods

110 subjects were recruited; 80 male children with suspected FXS and 30 matched healthy children. We evaluated the clinical utility of serum matrix metalloproteinase-9(MMP9) and amyloid-beta protein precursor(APP) as potential biomarkers for FXS.

Results

Out of 80 suspected children, 14 had full mutation, 8 had the premutation and 58 children had normal genotypes. No statistically-significant difference was detected between children with different genotypes concerning age of onset(P = 0.658), main clinical presentation(P = 0.388), clinical severity-score(P = 0.799), patient’s disease-course(P = 0.719) and intellectual disability(P = 0.351). Both MMP9 and APP showed a statistically significant difference when comparing different genotype subgroups(P = 0.019 and < 0.001, respectively). Clinically, MMP9 levels were highest in children presenting with language defects, while APP was highest in children with neurodevelopmental delay. In receiver operating curve analysis, comparing full and premutation with the normal genotype group, MMP9 has an area-under-the-curve of 0.701(95 % CI 0.557–0.845), while APP was marginally better at 0.763(95 % CI 0.620–0.906). When combined together, elevated MMP9 or APP had excellent sensitivity > 95 % for picking-up FXS cases in the clinical setting.

Conclusions

Screening for circulating biomarkers in the absence of FXS genetic diagnosis is justified. Our study is the first to evaluate both MMP9 and APP in FXS suspected children in a clinical setting and to assess their correlation with disease presentation and severity.

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来源期刊

Clinical biochemistry 医学-医学实验技术

CiteScore

5.10

自引率

0.00%

发文量

151

审稿时长

25 days

期刊介绍： Clinical Biochemistry publishes articles relating to clinical chemistry, molecular biology and genetics, therapeutic drug monitoring and toxicology, laboratory immunology and laboratory medicine in general, with the focus on analytical and clinical investigation of laboratory tests in humans used for diagnosis, prognosis, treatment and therapy, and monitoring of disease.