FLNA基因中的一种新型截短突变导致室周结节性异位、埃勒斯-当洛综合征样胶原病和大血小板减少症。

A novel truncating mutation in FLNA causes periventricular nodular heterotopia, Ehlers-Danlos-like collagenopathy and macrothrombocytopenia.

作者信息

Ieda Daisuke, Hori Ikumi, Nakamura Yuji, Ohshita Hironori, Negishi Yutaka, Shinohara Tsutomu, Hattori Ayako, Kato Takenori, Inukai Sachiko, Kitamura Katsumasa, Kawai Tomoki, Ohara Osamu, Kunishima Shinji, Saitoh Shinji

机构信息

Department of Pediatrics and Neonatology, Nagoya City University Graduate School of Medical Sciences, Japan.

Department of Advanced Diagnosis, Clinical Research Center, National Hospital Organization Nagoya Medical Center, Japan.

出版信息

Brain Dev. 2018 Jun;40(6):489-492. doi: 10.1016/j.braindev.2018.01.010. Epub 2018 Feb 12.

DOI:10.1016/j.braindev.2018.01.010

PMID:29449050

Abstract

INTRODUCTION

Filamin A (FLNA) is located in Xq28, and encodes the actin binding protein, filamin A. A mutation in FLNA is the most common cause of periventricular nodular heterotopia (PVNH), but a clear phenotype-genotype correlation has not been established. Indeed, some patients with a FLNA mutation have recently been shown to additionally have Ehlers-Danlos-like collagenopathy or macrothrombocytopenia. In an attempt to establish a clearer correlation between clinical symptoms and genotype, we have investigated a phenotype that involves thrombocytopenia in a patient with a truncation of the FLNA gene.

CASE REPORT

We present the case of a 4-year-old girl who, at birth, showed a ventral hernia. At 2 months of age, she was diagnosed with patent ductus arteriosus (PDA) and aortic valve regurgitation. At 11 months, she underwent ligation of the PDA. She was also diagnosed with diaphragmatic eventration by a preoperative test. At 19 months, motor developmental delay was noted, and brain MRI revealed bilateral PVNH with mega cisterna magna. Presently, there is no evidence of epilepsy, intellectual disability or motor developmental delay. She has chronic, mild thrombocytopenia, and a platelet count that transiently decreases after viral infection. Dilation of the ascending aorta is progressing gradually. Genetic testing revealed a de novo nonsense heterozygous mutation in FLNA (NM_001456.3: c.1621G > T; p.Glu541Ter). Immunofluorescence staining of a peripheral blood smear showed a lack of filamin A expression in 21.1% of her platelets. These filamin A-negative platelets were slightly larger than her normal platelets.

CONCLUSION

Our data suggests immunofluorescence staining of peripheral blood smears is a convenient diagnostic approach to identify patients with a FLNA mutation, which will facilitate further investigation of the correlation between FLNA mutations and patient phenotype.

摘要

引言

细丝蛋白A（FLNA）位于Xq28，编码肌动蛋白结合蛋白细丝蛋白A。FLNA突变是室周结节性异位（PVNH）最常见的病因，但尚未建立明确的表型-基因型相关性。事实上，最近有研究表明，一些FLNA突变患者还伴有埃勒斯-当洛综合征样胶原病或巨大血小板减少症。为了更清楚地建立临床症状与基因型之间的相关性，我们对一名FLNA基因截断患者的血小板减少症进行了研究。

病例报告

我们报告了一名4岁女孩的病例，她出生时患有腹疝。2个月大时，她被诊断为动脉导管未闭（PDA）和主动脉瓣反流。11个月时，她接受了PDA结扎术。术前检查还诊断出膈膨出。19个月时，发现运动发育迟缓，脑部MRI显示双侧PVNH伴大脑大池增大。目前，没有癫痫、智力残疾或运动发育迟缓的证据。她患有慢性轻度血小板减少症，病毒感染后血小板计数会短暂下降。升主动脉扩张正在逐渐进展。基因检测显示FLNA存在新发无义杂合突变（NM_001456.3：c.1621G>T；p.Glu541Ter）。外周血涂片的免疫荧光染色显示，她21.1%的血小板中缺乏细丝蛋白A表达。这些细丝蛋白A阴性血小板比她的正常血小板略大。