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Genotype-phenotype correlations in hereditary elliptocytosis and hereditary pyropoikilocytosis

机译:基因型表型与遗传性脂细胞增多症和遗传性焦磷酸细胞增多症的相关性

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摘要

Hereditary elliptocytosis (HE) and hereditary pyropoikilocytosis (HPP) are heterogeneous red blood cell (RBC) membrane disorders that result from mutations in the genes encoding α-spectrin (SPTA1), β-spectrin (SPTB), or protein 4.1R (EPB41). The resulting defects alter the horizontal cytoskeletal associations and affect RBC membrane stability and deformability causing shortened RBC survival. The clinical diagnosis of HE and HPP relies on identifying characteristic RBC morphology on peripheral blood smear and specific membrane biomechanical properties using osmotic gradient ektacytometry. However, this phenotypic diagnosis may not be readily available in patients requiring frequent transfusions, and does not predict disease course or severity. Using Next-Generation sequencing, we identified the causative genetic mutations in fifteen patients with clinically suspected HE or HPP and correlated the identified mutations with the clinical phenotype and ektacytometry profile. In addition to identifying three novel mutations, gene sequencing confirmed and, when the RBC morphology was not evaluable, identified the diagnosis. Moreover, genotypic differences justified the phenotypic differences within families with HE/HPP.
机译:遗传性脂细胞增多症(HE)和遗传性焦磷酸细胞增多症(HPP)是异质性红细胞(RBC)膜疾病,由编码α-血影蛋白(SPTA1),β-血影蛋白(SPTB)或蛋白4.1R(EPB41)的基因突变引起。产生的缺陷改变了水平细胞骨架的关联,影响了红细胞膜的稳定性和可变形性,导致红细胞存活时间缩短。 HE和HPP的临床诊断依赖于使用渗透梯度流式细胞术鉴定外周血涂片的特征性RBC形态和特定的膜生物力学特性。但是,这种表型诊断在需要频繁输血的患者中可能不容易获得,并且不能预测疾病的进程或严重程度。使用下一代测序,我们鉴定了15名临床怀疑的HE或HPP患者的致病性基因突变,并将鉴定出的突变与临床表型和流式细胞仪相关联。除了鉴定出三个新的突变,基因测序得以证实,并且在无法评估RBC形态的情况下,可以鉴定诊断。此外,基因型差异证明了HE / HPP家庭中的表型差异是合理的。

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