Genetic analysis of TMPRSS6 catalytic domain variants in Mexican patients with iron treatment refractoriness.

Rubiceli Hernández-Peña, Eric Jonathan Maciel-Cruz, Lourdes Del Carmen Rizo-De La Torre, Francisco Javier Perea-Díaz, Bertha Ibarra-Cortés
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Abstract

Objective: To identify the TMPRSS6 gene variants in Mexican patients with iron treatment refractoriness, to describe hematological and iron profile parameters, and to use bioinformatic prediction and protein modeling tools to assess a possible biological impact for the detected missense variants.

Methods: Nineteen patients referred with iron treatment refractoriness were studied. Peripheral blood was collected to determine hematic cytometry, iron profile, hemoglobin electrophoresis, and quantification. Molecular screening was carried out for exons 15 through 18 of the TMPRSS6 gene by Sanger sequencing and for frequent thalassemia variants by amplification-refractory mutation system-polymerase chain reaction (PCR) and gap-PCR. The biological impact of the detected missense variants was assessed using bioinformatic prediction and protein modeling tools.

Results: We found 5 genetic variants in the matriptase-2 catalytic domain: 1 at intron-15/exon-16 junction (rs60484081) and 4 exonic, 3 missense (rs377054987, p.Gly626Asp; rs1384127820, p.Ser672Thr; rs855791, p.Val727Ala) and 1 synonymous (rs2235321, p.Tyr730=), with frequencies ranging from 0.18 to 0.53. No significant differences were observed in the hematological parameters or iron profile, considering type and number of variants. Bioinformatic predictions suggested a possible biological impact only for rs377054987.

Conclusions: The TMPRSS6 variants observed in Mexican patients with oral iron treatment refractoriness have high frequencies; nevertheless, their relationship with hematological and iron profile parameters needs further research. The possible biological impact for rs377054987 is due to size and amino acid hydrophobicity changes and hydrogen bond modifications.

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墨西哥铁剂治疗难治性患者中 TMPRSS6 催化域变体的遗传分析。
目的确定墨西哥铁治疗难治性患者的 TMPRSS6 基因变异,描述血液学和铁概况参数,并使用生物信息学预测和蛋白质建模工具评估检测到的错义变异可能产生的生物学影响:研究了19名因铁治疗无效而转诊的患者。收集外周血以测定血细胞计数、铁轮廓、血红蛋白电泳和定量。通过桑格测序对 TMPRSS6 基因的 15 至 18 号外显子进行了分子筛查,并通过扩增-难治性突变系统-聚合酶链反应(PCR)和间隙-PCR 对常见的地中海贫血变异进行了分子筛查。利用生物信息学预测和蛋白质建模工具评估了检测到的错义变异的生物学影响:结果:我们在matriptase-2催化结构域中发现了5个基因变异:其中1个位于内含子-15/外显子-16交界处(rs60484081),4个位于外显子,3个为错义变异(rs377054987,p.Gly626Asp;rs1384127820,p.Ser672Thr;rs855791,p.Val727Ala),1个为同义变异(rs2235321,p.Tyr730=),变异频率从0.18到0.53不等。考虑到变异的类型和数量,在血液学参数或铁概况方面未观察到明显差异。生物信息学预测表明,只有 rs377054987 可能会产生生物学影响:在墨西哥口服铁剂治疗难治性患者中观察到的 TMPRSS6 变异具有较高的频率;然而,它们与血液学和铁概况参数的关系还需要进一步研究。rs377054987可能产生的生物学影响是由于其大小和氨基酸疏水性的变化以及氢键修饰。
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Robert L. Schmidt, MD, PhD, MBA (November 17, 1952-October 25, 2023) A 6-year-old boy with an atypical liver neoplasm harboring a novel RPS6KA3 variant. Evaluating direct amplification from viral transport medium for SARS-CoV-2 detection, strain typing, and angiotensin-converting enzyme genotyping and expression assays. Diagnostic value of pleural effusion Krebs von den Lungen-6 in malignant pleural effusion of patients with non-small cell lung cancer. Genetic analysis of TMPRSS6 catalytic domain variants in Mexican patients with iron treatment refractoriness.
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