Two novel mutations in the DNAH11 gene in primary ciliary dyskinesia (CILD7) with considerable variety in the clinical and beating cilia phenotype.

4区 医学 Q4 Medicine
Rüdiger Schultz, Varpu Elenius, Heikki Lukkarinen, Tanja Saarela
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引用次数: 8

Abstract

Background: Diagnosis of primary ciliary dyskinesia (PCD) still remains a challenge, especially with mutations in the Dynein Arm Heavy Chain 11 (DNAH11) gene. Classical diagnostic measures like Transmission Electron Microscopy (TEM) are not applicable for mutations in the DNAH11 gene since ultrastructural defects of the ciliary apparatus are absent. Novel mutations encoding for PCD appear all the time with considerable variation in the clinical picture, making it necessary to update data bases and guidelines for PCD diagnostics.

Methods: In this study we examined two unrelated, Finnish families with symptoms of PCD applying the clinical scoring system: Primary ciliary dyskinesia Rule (PICADAR), high speed video microscopy analysis (HSVMA) for ciliary movement, a commercially available gene panel analysis and nasal Nitric Oxide (nNO) measurements if applicable.

Results: Two, likely pathogenic variants in the DNAH11 gene (c.2341G > A, p. (Glu781Lys) ja c.7645 + 5G > A) were detected. In the first family, compound heterozygous mutations led to disease manifestation in two of 4 children, which showed a similar phenotype of cilia beating pattern but marked differences in disease severity. In the second family, all three children were homozygotes for the c.2341G > A p.(Glu781Lys) mutation and showed a similar degree of disease severity. However, the phenotype of cilia beating pattern was different ranging from stiff, static cilia to a hyperkinetic movement in one of these children.

Conclusions: In this study we describe two Finnish families with PCD, revealing two novel mutations in the DNAH11 gene which show considerable variety in the clinical and beating cilia phenotype. The results of this study show the clinician that PCD can be much milder than generally expected and diagnosis demands a combination of measures which are only successful in experienced hands. Chronic and repeatedly treated wet cough should raise suspicion of PCD, referring the patient for further diagnostics to a specialised PCD centre.

Abstract Image

原发性纤毛运动障碍(CILD7)中DNAH11基因的两个新突变在临床和搏动纤毛表型上有相当大的变化。
背景:原发性纤毛运动障碍(PCD)的诊断仍然是一个挑战,特别是动力蛋白臂重链11 (DNAH11)基因突变。传统的诊断方法,如透射电子显微镜(TEM)不适用于DNAH11基因突变,因为纤毛体的超微结构缺陷不存在。PCD编码的新突变一直出现,在临床图像中有相当大的变化,因此有必要更新PCD诊断的数据库和指南。方法:在这项研究中,我们检查了两个不相关的芬兰PCD症状家庭,应用临床评分系统:原发性纤毛运动障碍规则(PICADAR),高速视频显微镜分析(HSVMA)用于纤毛运动,商业上可用的基因小组分析和鼻一氧化氮(nNO)测量(如果适用)。结果:检测到两种可能致病的DNAH11基因变异(c.2341G > A, p. (Glu781Lys) ja c.7645 + 5G > A)。在第一个家庭中,复合杂合突变导致4个孩子中的2个出现疾病表现,表现出相似的纤毛跳动模式表型,但疾病严重程度有显著差异。在第二个家庭中,所有三个孩子都是c.2341G > A p.(Glu781Lys)突变的纯合子,并且表现出相似的疾病严重程度。然而,在这些儿童中,纤毛跳动模式的表型是不同的,从僵硬,静态纤毛到多动运动。结论:在这项研究中,我们描述了两个芬兰PCD家族,揭示了DNAH11基因的两个新突变,这些突变在临床和跳动纤毛表型中表现出相当大的变化。这项研究的结果向临床医生表明,PCD可能比一般预期的要温和得多,诊断需要综合措施,只有经验丰富的人才能成功。慢性和反复治疗的湿咳应引起对PCD的怀疑,将患者转介到专门的PCD中心进行进一步诊断。
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来源期刊
BMC Medical Genetics
BMC Medical Genetics 医学-遗传学
自引率
0.00%
发文量
0
审稿时长
12 months
期刊介绍: BMC Medical Genetics is an open access journal publishing original peer-reviewed research articles in the effects of genetic variation in individuals, families and among populations in relation to human health and disease. Note: BMC Medical Genetics is now closed. This journal has merged with BMC Medical Genomics, a broad-scope, open access community journal for all medical genetics and genomics research.
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