对巴西铁超载患者体内 BMP6 基因突变的研究

IF 1.8 Q3 HEMATOLOGY

Hematology, Transfusion and Cell Therapy Pub Date : 2024-11-01 DOI:10.1016/j.htct.2024.04.001

Ana Carolina Mourão Toreli , Isabella Toni , Dulcinéia Martins de Albuquerque , Carolina Lanaro , Jersey Heitor Maues , Kleber Yotsumoto Fertrin , Paula de Melo Campos , Fernando Ferreira Costa

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引用次数: 0

摘要

diron overload （IO）是一种复杂的疾病，临床、行为和遗传因素对其表型有影响。在多种族和非高加索人群中，在大多数情况下，HFE基因突变不能单独解释IO，必须调查其他遗传和环境因素。骨形态发生蛋白（BMPs）通过包括SMAD和HJV在内的信号通路调节HAMP转录，在铁稳态中发挥核心作用。在这项研究中，我们旨在探讨BMP6突变在巴西IO患者队列中的临床相关性。方法对41例IO患者进行临床评价。采集血样，通过新序列世代（New Sequence Generations， NGS）分析BMP6突变。分析变异和突变的频率，并将其与临床和环境特征相关联。结果我们在3例IO患者中发现了BMP6突变。在2例患者中鉴定出p.a arg257his突变，在1例患者中鉴定出p.Leu71Val突变。其中2例患者有额外的IO危险因素（HFE突变和糖尿病）。结论bmp6突变与其他遗传及临床危险因素共同作用可能导致IO的发生。为了充分解决BMP6在IO中的作用，有必要进行功能研究和大队列的评估。

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Investigation of BMP6 mutations in Brazilian patients with iron overload

Background

Iron overload (IO) is a complex condition in which clinical, behavioral and genetic factors contribute to the phenotype. In multiethnic and non-Caucasian populations, mutations in HFE gene alone cannot explain IO in most of the cases, and additional genetic and environmental factors must be investigated. Bone Morphogenetic Proteins (BMPs) play a central role in iron homeostasis by modulating HAMP transcription through the signaling pathway that includes SMAD and HJV. In this study, we aimed to explore the clinical relevance of BMP6 mutations in a cohort of Brazilian patients with IO.

Methods

41 patients with IO were evaluated. Blood samples were collected to analyze BMP6 mutations through New Sequence Generations (NGS). Frequency of variants and mutations were analyzed and correlated with clinical and environmental characteristics.

Results

We identified BMP6 mutations in three patients with IO. The p.Arg257His mutation was identified in two patients and the p.Leu71Val mutation was identified in one patient. Two of these patients had additional risk factors for IO (HFE mutations and diabetes mellitus).

Conclusion

BMP6 mutations, when combined to other genetic and clinical risk factors, may contribute to IO. Functional studies and THE evaluation of large cohorts are necessary to fully address BMP6 role in IO.

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