Department of Medical Genetics, Faculty of Medical Sciences, Tarbiat Modares University, Tehran, Iran.
PardisGene CO, Tehran, Iran.
BMC Genomics. 2024 Aug 27;25(1):805. doi: 10.1186/s12864-024-10478-w.
Hermansky-Pudlak Syndrome (HPS), a rare autosomal recessive disorder, is characterized by oculocutaneous albinism, bleeding diathesis, and sometimes severe lung problems and inflammatory bowel disease. Symptoms include skin and hair pigmentation variations, along with visual impairments. Variants in eleven genes encoding protein complexes essential for membrane trafficking and intracellular endosomal transport pathways underlie various recognized HPS subtypes. This study focuses on HPS-9, a subtype of Hermansky-Pudlak Syndrome caused by a variant in the BLOC1S6 gene, which is a subunit of the BLOC1 complex. In this study, a novel Copy Number Variation (CNV) in the aforementioned gene in an Iranian family is reported. The study aims to better understand the etiology of HPS-9 symptoms by identifying and confirming the variant and determining whether the gene is expressed despite the deletion. There have only been five reports of this syndrome in the literature thus far. Our novel CNV represents a significant contribution to understanding the genetic basis of HPS-9.
This study investigates a male patient presenting with albinism. Whole Exome Sequencing (WES) identified a homozygous deletion of approximately 350 bp using CNV analysis. The deletion affects the intronic region of the BLOC1S6 gene, causing uncertainties in defining the exact boundaries due to WES limitations. Primer walking and GAP-PCR techniques were used to define the deletion boundaries. Subsequent assessments of this variant across other family members helped identify homozygous affected members and heterozygous carriers. The absence of BLOC1S6 expression in the affected individual was confirmed through Real-time PCR experiments. These findings underscore the importance of understanding the implications for the patient's healthcare and potential therapeutic approaches.
This study introduces a case of Hermansky-Pudlak Syndrome Type 9 (HPS-9) caused by a homozygous deletion in the BLOC1S6 gene. We identified an approximately 7-kb deletion encompassing exon 1 and the intronic region of the gene. The absence of BLOC1S6 expression, confirmed via Real-time PCR, highlights the importance of studying the pathogenicity of the deletion and its impact on the patient's health. Our findings contribute to the sparse knowledge on HPS-9 and underscore the need for further exploration into the genetic causes of this rare disorder.
Hermansky-Pudlak 综合征(HPS)是一种罕见的常染色体隐性遗传病,其特征是眼皮肤白化病、出血素质,有时还伴有严重的肺部问题和炎症性肠病。症状包括皮肤和头发色素沉着的变化,以及视力障碍。十一个编码对膜运输和细胞内内体运输途径至关重要的蛋白复合物的基因变异导致了各种公认的 HPS 亚型。本研究关注的是由 BLOC1S6 基因变异引起的 HPS-9 亚型,该基因是 BLOC1 复合物的一个亚基。本研究报告了在一个伊朗家庭中上述基因的一种新的拷贝数变异(CNV)。该研究旨在通过识别和确认变异体并确定即使存在缺失,基因是否表达,来更好地了解 HPS-9 症状的病因。迄今为止,文献中仅有五例该综合征的报道。我们的新 CNV 代表了对理解 HPS-9 遗传基础的重要贡献。
本研究调查了一名患有白化病的男性患者。全外显子组测序(WES)通过 CNV 分析发现大约 350bp 的纯合缺失。该缺失影响 BLOC1S6 基因的内含子区域,由于 WES 的限制,导致难以确定确切的边界。通过引物步行和 GAP-PCR 技术来定义缺失的边界。随后对其他家族成员进行了该变异的评估,帮助确定了纯合受影响的成员和杂合携带者。通过实时 PCR 实验证实了该变异个体中 BLOC1S6 表达的缺失。这些发现强调了了解对患者的医疗保健和潜在治疗方法的影响的重要性。
本研究介绍了一例由 BLOC1S6 基因纯合缺失引起的 Hermansky-Pudlak 综合征 9 型(HPS-9)病例。我们发现了一个大约 7kb 的缺失,包含了基因的外显子 1 和内含子区域。通过实时 PCR 证实了 BLOC1S6 表达的缺失,突出了研究缺失的致病性及其对患者健康的影响的重要性。我们的发现为 HPS-9 的罕见知识做出了贡献,并强调了进一步探索这种罕见疾病遗传原因的必要性。
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