Genetic Dysfunctions of the Surfactant System in Children: Results of a Multicenter Study

D. Ovsyannikov, M. A. Zhestkova, V. Strelnikova, A. Averin, M.A. Atipaeva, O. Brunova, G. Buyanova, N. Weinstein, M.V. Volchikhin, I. V. Girutskaya, I. Davydova, D. Zhakota, I. Kovalenko, K.D. Korol, A. A. Kuznetsova, A. Krushelnitsky, A. Malakhov, L. Malyutina, E. A. Mamaeva, T.V. Marshalkina, A. Migali, A. Orlov, A.Yu. Pastarnak, S. I. Petrova, Е.Е. Petryaikina, Е.S. Petryaikina, G. Prokopiev, A. Pushkov, K. Savostyanov, Yu. A. Sigova, D. Skobeev, O. Sudakova, A. G. Talalaev, O. Topilin, M. Traube, A. Fisenko, A. Kholopova, A. Tsverava, N. B. Tsokova, S. Cherkasova
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Abstract

Aim: Genetic, clinical, laboratory-instrumental and morphological characteristics of genetic dysfunctions of the surfactant system in children, therapy and outcomes of the disease. Design: Multicentre, ambispective, open-label, descriptive pilot longitudinal study. Materials and methods. We observed 17 children from 16 families with identified mutations in the SFTPC, ABCA3, NKX2-1 genes. Methods used: genealogical, Sanger sequencing, clinical exome sequencing, computed tomography and histological examination of the lungs. Results. The study included 8 children with congenital deficiency of surfactant protein C, 8 children with brain-lung-thyroid syndrome and 1 patient with congenital deficiency of protein ABSA3. Based on the results of a genetic examination of patients, nucleotide variants c.218T>C were identified in 2 out of 8 patients with a mutation in the SFTPC gene, which is the most common according to the literature. In 5 children, the mutations were hereditary. Congenital deficiency of surfactant protein C, ABCA3 protein and brain-lung-thyroid syndrome were characterized by clinical, computed tomography, and morphological signs of interstitial lung disease. Despite complex respiratory, anti-inflammatory therapy, the frequency of deaths in congenital deficiency of surfactant protein C was 37.5%. Conclusion. Children with severe respiratory distress syndrome of newborns, interstitial lung disease with the development of severe chronic respiratory failure, burdened with a family history should undergo genetic testing to detect mutations in the genes SFTPB, SFTPC, ABCA3. The patient's combination of respiratory symptoms with congenital hypothyroidism and neurological pathology is the basis for genetic examination for NKX2-1 gene mutations to exclude the brain-lung-thyroid syndrome. Keywords: genetic dysfunctions of the surfactant system, congenital deficiency of surfactant protein C, congenital deficiency of ABCA3 protein, brain-lung-thyroid syndrome, NKX2-1 gene, children.
儿童表面活性剂系统的遗传功能障碍:一项多中心研究的结果
目的:探讨儿童表面活性剂系统遗传性功能障碍的遗传学、临床、实验室仪器和形态学特征、治疗方法和预后。设计:多中心、双视角、开放标签、描述性试点纵向研究。材料和方法。我们观察了来自16个家庭的17名儿童,他们在SFTPC、ABCA3、NKX2-1基因中发现了突变。方法:家谱、Sanger测序、临床外显子组测序、计算机断层扫描和肺组织学检查。结果。本研究纳入8例先天性表面活性剂蛋白C缺乏症患儿、8例脑-肺-甲状腺综合征患儿和1例先天性ABSA3蛋白缺乏症患儿。根据对患者的遗传检查结果,8例SFTPC基因突变患者中有2例发现核苷酸变异C . 218t >C,这是文献中最常见的突变。在5名儿童中,突变是遗传性的。先天性表面活性剂蛋白C、ABCA3蛋白缺乏和脑-肺-甲状腺综合征通过临床、计算机断层扫描和肺间质性疾病的形态学征象表现出来。尽管进行了复杂的呼吸、抗炎治疗,先天性表面活性剂蛋白C缺乏症的死亡率仍为37.5%。结论。新生儿严重呼吸窘迫综合征、间质性肺疾病并发严重慢性呼吸衰竭、有家族史的患儿应进行基因检测,检测SFTPB、SFTPC、ABCA3基因的突变。患者呼吸道症状合并先天性甲状腺功能减退和神经病理学是进行NKX2-1基因突变遗传学检查以排除脑-肺-甲状腺综合征的基础。关键词:表面活性剂系统遗传功能障碍,先天缺乏表面活性剂蛋白C,先天缺乏ABCA3蛋白,脑-肺-甲状腺综合征,NKX2-1基因,儿童
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