Unité de Génétique Médicale et Laboratoire Associé INSERM à l'unité UMR_S 910, Faculté de Médecine, Université Saint-Joseph, Beirut, Lebanon.
Clin Genet. 2012 Nov;82(5):489-93. doi: 10.1111/j.1399-0004.2011.01783.x. Epub 2011 Oct 5.
The immunodeficiency, centromeric instability and facial anomalies (ICF) syndrome is a rare autosomal recessive disease characterized by targeted chromosome breakage, directly related to a genomic methylation defect. It manifests with phenotypic and clinical variability, with the most consistent features being developmental delay, facial anomalies, cytogenetic defects and immunodeficiency with a reduction in serum immunoglobulin levels. From the molecular point of view, ICF syndrome was always divided into ICF type I (ICF1) and ICF type 2 (ICF2). Mutations in DNMT3B gene are responsible for ICF1, while mutations in ZBTB24 have been reported to be responsible for ICF2. In this study, we describe a Lebanese family with three ICF2 affected brothers. Sanger sequencing of the coding sequence of ZBTB24 gene was conducted and revealed a novel deletion: c.396_397delTA (p.His132Glnfs*19), resulting in a loss-of-function of the corresponding protein. ZBTB24 belongs to a large family of transcriptional factors and may be involved in DNA methylation of juxtacentromeric DNA. Detailed molecular and functional studies of the ZBTB24 and DNMT3B genes are needed to understand the pathophysiology of ICF syndrome.
免疫缺陷、着丝粒不稳定和面部异常(ICF)综合征是一种罕见的常染色体隐性疾病,其特征是靶向染色体断裂,与基因组甲基化缺陷直接相关。它表现出表型和临床变异性,最一致的特征是发育迟缓、面部异常、细胞遗传学缺陷和免疫缺陷,血清免疫球蛋白水平降低。从分子角度来看,ICF 综合征始终分为 ICF 型 1(ICF1)和 ICF 型 2(ICF2)。DNMT3B 基因突变负责 ICF1,而 ZBTB24 基因突变则负责 ICF2。在这项研究中,我们描述了一个黎巴嫩的 ICF2 受影响的三兄弟家庭。对 ZBTB24 基因的编码序列进行了 Sanger 测序,发现了一个新的缺失:c.396_397delTA(p.His132Glnfs*19),导致相应蛋白的功能丧失。ZBTB24 属于转录因子的大家族,可能参与着丝粒周围 DNA 的甲基化。需要对 ZBTB24 和 DNMT3B 基因进行详细的分子和功能研究,以了解 ICF 综合征的病理生理学。
