拉脱维亚遗传性血管性水肿患者临床和遗传特征的全国调查。

Adine Kanepa, Inga Nartisa, Dmitrijs Rots, Linda Gailite, Henriette Farkas, Natalja Kurjane
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引用次数: 1

摘要

背景:遗传性血管性水肿(HAE)是一种罕见且危及生命的先天性免疫错误。HAE主要是由丝氨酸蛋白酶抑制剂基因1 (SERPING1)的致病性变异引起的,导致c1抑制剂(C1-INH)缺乏或功能失调,缓激肽过量产生,以及复发性皮下和/或粘膜下水肿的发展。全世界HAE的患病率为5万至10万人中有1人。我们的目的是描述拉脱维亚伴有C1-INH缺乏症(C1-INH- hae)的遗传性血管性水肿的临床特征和遗传谱。方法:从2006年到2022年3月,所有拉脱维亚诊断为HAE (I/II型)的患者都被纳入研究。对实验室检查和临床资料进行分析,并进行Sanger测序和全基因组测序的基因检测。结果:研究确定了来自8个家庭的10例C1-INH-HAE患者(9名女性,1名男性)。拉脱维亚的HAE点流行率为每10万居民0.53例。在所有患者中,7例(70%)为1型HAE, 3例(30%)为2型HAE。患者的中位年龄为54岁,出现症状的中位年龄为15岁。观察到诊断前的显著延迟(中位20.5年),60%的患者有血管性水肿的阳性家族史。所有HAE患者一生中平均住院两次。皮肤(100%)、腹部(80%)和气道(80%)水肿是最常见的症状。涉及触发因素(60%)和前驱症状(90%)。50%的患者发作严重,10%为中度,40%为轻度。在8例患者(6个家族)中鉴定出SERPING1的致病变异,从分子上证实了诊断。在两名患者(两个家庭)中,即使在全基因组测序后也未发现基因的致病性变异。结论:目前的数据显示拉脱维亚HAE的显著延迟和明显的诊断不足。提高对该病的认识,加强医生之间的信息和沟通,将有助于改善HAE的诊断和管理;筛查家庭成员、对抗组胺药和糖皮质激素无反应的复发性血管性水肿患者,以及反复发作严重且原因不明的腹痛患者。
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National survey on clinical and genetic characteristics of patients with hereditary angioedema in Latvia.

Background: Hereditary angioedema (HAE) is a rare and life-threatening inborn error of immunity. HAE is mostly caused by pathogenic variations in the serine protease inhibitor gene 1 (SERPING1), leading to deficient or dysfunctional C1-inhibitor (C1-INH), overproduction of bradykinin, and development of recurrent subcutaneous and/or submucosal oedema. The prevalence of HAE is 1 in 50,000 - 100000 people worldwide. We aimed to describe the clinical features and genetic spectrum of hereditary angioedema with C1-INH deficiency (C1-INH-HAE) in Latvia.

Methods: All patients from Latvia diagnosed with HAE (types I/II) from 2006 to March 2022 were included in the study. Laboratory tests and clinical data were analysed, and genetic tests with Sanger sequencing and whole genome sequencing were performed.

Results: The study identified 10 C1-INH-HAE patients (nine females, one male) from eight families. The point prevalence of HAE in Latvia is 0.53 per 100 000 inhabitants. Of all patients, seven (70%) had HAE type I and three (30%) had HAE type II. The median age of patients was 54 years and the median age at onset of symptoms was 15 years. A significant delay (median 20.5 years) until diagnosis was observed, and 60% of patients had a positive family history of angioedema. All HAE patients have been hospitalised a median two times during their lifetime. Skin (100%), abdominal (80%), and airway (80%) oedema were the most frequent symptoms. Triggering factors (60%) and prodromal symptoms (90%) were referred. Attacks were severe in 50% of patients, moderate in 10%, and mild in 40%. Pathogenic variations of SERPING1 were identified in eight patients (six families), confirming the diagnosis molecularly. In two patients (two families), no pathogenic variations in the genes were found even after whole genome sequencing.

Conclusions: Current data shows a significant delay and clear underdiagnosis of HAE in Latvia. Higher awareness and better information and communication between doctors would improve the diagnosis and management of HAE; as would screening of family members, patients with recurrent angioedema unresponsive to antihistamines and glucocorticoids, and patients with recurrent episodes of severe, unexplained abdominal pain.

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