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Genetic causes and clinical management of pediatric interstitial lung diseases

机译:儿科间质性肺病的遗传原因及临床管理

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Purpose of reviewInterstitial lung disease (ILD) in children (chILD) is an umbrella term for a heterogeneous group of rare respiratory disorders that are mostly chronic and associated with high morbidity and mortality. The pathogenesis of the various chILD is complex and implicates genetic contributors. The purpose of this review is to provide updated information on the molecular defects associated with the development of chILD.Recent findingsCurrently, the main mutations are identified in the surfactant genes SFTPA1, SFTPA2, SFTPB, SFTPC, ABCA3, and NKX2-1. In addition, pulmonary alveolar proteinosis is associated with mutations in CSF2RA, CSF2RB, and MARS, and specific auto-inflammatory forms of chILD implicate STING and COPA disorders. The relationships between the genetic defects and the disease expression remain poorly understood, with no genotype-phenotype correlations identified so far. Although targeted therapies are emerging, the management strategies are still largely empirical, relying mostly on corticosteroids.SummaryGenetic factors play an important role in chILD, and the ongoing development of novel technologies will rapidly broaden the genetic landscape of chILD. Therefore, in the coming years, it is expected that newly identified molecular defects and markers will help predicting disease courses and tailoring individual therapies.
机译:审核肺病(ILD)的目的是儿童(儿童)是一种非均相稀有呼吸系统疾病的伞长,主要是慢性和伴有高发病率和死亡率。各个孩子的发病机制是复杂的并且含有遗传贡献者。本综述的目的是提供有关与孩子发育相关的分子缺陷的更新信息。特征性地,在表面活性剂SFTPA1,SFTPA2,SFTPB,SFTPC,ABCA3和NKX2-1中鉴定主要突变。此外,肺肺泡蛋白病与CSF2RA,CSF2RB和火星的突变有关,以及特异性的自动炎症形式的儿童致命刺痛和科普障碍。遗传缺陷和疾病表达之间的关系仍然明显差,目前没有鉴定基因型 - 表型相关性。虽然有针对性的疗法是出现的,但管理策略仍然主要是经验的,大多数依赖于皮质类固醇。ummaryGenetencetors在孩子中发挥着重要作用,并且新技术的持续发展将迅速扩大孩子的遗传景观。因此,在未来几年,预计新发现的分子缺陷和标记将有助于预测疾病课程和裁缝各个疗法。

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