Development of clinical paroxysmal nocturnal haemoglobinuria in children with aplastic anaemia.
Atsushi NaritaHideki MuramatsuYusuke OkunoYuko SekiyaKyogo SuzukiMotoharu HamadaShinsuke KataokaDaisuke IchikawaRieko TaniguchiNorihiro MurakamiDaiei KojimaEri NishikawaNozomu KawashimaNobuhiro NishioAsahito HamaYoshiyuki TakahashiSeiji KojimaPublished in: British journal of haematology (2017)
The clinical significance of paroxysmal nocturnal haemoglobinuria (PNH) in children with aplastic anaemia (AA) remains unclear. We retrospectively studied 57 children with AA between 1992 and 2010. During the follow-up, five patients developed clinical PNH, in whom somatic PIGA mutations were detected by targeted sequencing. The 10-year probability of clinical PNH development was 10·2% (95% confidence interval, 3·6-20·7%). Furthermore, the detection of minor PNH clones by flow cytometry at AA diagnosis was a risk factor for the subsequent development of clinical PNH. These patients with PNH clones at AA diagnosis should undergo periodic monitoring for potential clinical PNH development.