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Usefulness of NGS for Diagnosis of Dominant Beta-Thalassemia and Unstable Hemoglobinopathies in Five Clinical Cases

外显子组测序 医学 地中海贫血 贫血 溶血 溶血性贫血 β地中海贫血 输血 儿科 突变 遗传学 生物信息学 基因 内科学 生物
作者
Valeria Rizzuto,Tamara T. Koopmann,Adoración Blanco,Bárbara Tazón‐Vega,Amira Idrizovic,Cristina Díaz de Heredia,Rafael Del Orbe,Miriam Vara Pampliega,Pablo Velasco,David Benéitez,Gijs W.E. Santen,Quinten Waisfisz,Mariet Elting,Frans J. Smiers,Anne J. de Pagter,Jean‐Louis Kerkhoffs,Cornelis L. Harteveld,María del Mar Mañú‐Pereira
出处
期刊:Frontiers in Physiology [Frontiers Media]
卷期号:12 被引量:15
标识
DOI:10.3389/fphys.2021.628236
摘要

Unstable hemoglobinopathies (UHs) are rare anemia disorders (RADs) characterized by abnormal hemoglobin (Hb) variants with decreased stability. UHs are therefore easily precipitating, causing hemolysis and, in some cases, leading to dominant beta-thalassemia (dBTHAL). The clinical picture of UHs is highly heterogeneous, inheritance pattern is dominant, instead of recessive as in more prevalent major Hb syndromes, and may occur de novo . Most cases of UHs are not detected by conventional testing, therefore diagnosis requires a high index of suspicion of the treating physician. Here, we highlight the importance of next generation sequencing (NGS) methodologies for the diagnosis of patients with dBTHAL and other less severe UH variants. We present five unrelated clinical cases referred with chronic hemolytic anemia, three of them with severe blood transfusion dependent anemia. Targeted NGS analysis was performed in three cases while whole exome sequencing (WES) analysis was performed in two cases. Five different UH variants were identified correlating with patients’ clinical manifestations. Four variants were related to the beta-globin gene (Hb Bristol—Alesha, Hb Debrousse, Hb Zunyi, and the novel Hb Mokum) meanwhile one case was caused by a mutation in the alpha-globin gene leading to Hb Evans. Inclusion of alpha and beta-globin genes in routine NGS approaches for RADs has to be considered to improve diagnosis’ efficiency of RAD due to UHs. Reducing misdiagnoses and underdiagnoses of UH variants, especially of the severe forms leading to dBTHAL would also facilitate the early start of intensive or curative treatments for these patients.
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