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Exome sequencing results in successful diagnosis and treatment of a severe congenital anemia

机译:外显子组测序可成功诊断和治疗严重的先天性贫血

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摘要

Whole-exome sequencing is increasingly used for diagnosis and identification of appropriate therapies in patients. Here, we present the case of a 3-yr-old male with a lifelong and severe transfusion-dependent anemia of unclear etiology, despite an extensive clinical workup. Given the difficulty of making the diagnosis and the potential side effects from performing interventions in patients with a congenital anemia of unknown etiology, we opted to perform whole-exome sequencing on the patient and his parents. This resulted in the identification of homozygous loss-of-function mutations in the EPB41 gene, encoding erythrocyte protein band 4.1, which therefore causes a rare and severe form of hereditary elliptocytosis in the patient. Based on prior clinical experience in similar patients, a surgical splenectomy was performed that resulted in subsequent transfusion independence in the patient. This case illustrates how whole-exome sequencing can lead to accurate diagnoses (and exclusion of diagnoses where interventions, such as splenectomy, would be contraindicated), thereby resulting in appropriate and successful therapeutic intervention—a major goal of precision medicine.
机译:全外显子测序越来越多地用于诊断和鉴定患者的适当疗法。在这里,我们介绍了一个3岁男性,尽管经过大量的临床检查,但仍存在病因不明的终身严重输血依赖性贫血。鉴于对病因不明的先天性贫血患者进行诊断的困难和进行干预的潜在副作用,我们选择对患者及其父母进行全基因组测序。这导致鉴定出编码红细胞蛋白条带4.1的EPB41基因的纯合功能丧失突变,因此在患者中引起罕见且严重的遗传性细胞增多症。根据类似患者的先前临床经验,进行了手术脾切除术,导致患者随后的输血独立性。该案例说明了全外显子测序如何能够导致准确的诊断(并排除了禁止进行脾切除等干预措施的诊断),从而导致了适当而成功的治疗干预,这是精密医学的主要目标。

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