JC Self Research Institute of Human Genetics, Greenwood Genetic Center, Greenwood, South Carolina, USA.
Am J Med Genet A. 2010 Mar;152A(3):713-7. doi: 10.1002/ajmg.a.33208.
Alport syndrome with intellectual disability (ID) is a contiguous gene deletion syndrome involving several genes on Xq22.3 including COL4A5 and ACSL4. We report on a family with two males with this disorder and a Xq22.3 deletion. Fluorescent in situ hybridization and genomic analyses mapped the deletion region to between exon 1 of COL4A5 and exon 12 of ACSL4. The patients' mother has microscopic hematuria and was found to be heterozygous for the Xq22.3 deletion. Analysis using reverse transcription polymerase chain reaction of lymphoblastoid cell line RNA from an affected male in the family revealed a stable chimeric transcript with the ACSL4 exons 13-17 replaced by a cryptic exon from intron 1 of the COL4A5 gene. A truncated 54 kDa protein was predicted from this transcript but Western blot analysis and ACSL4 enzyme assay both showed functional nullisomy of ACSL4. We also compared the clinical features of the family with three previously reported families with the ACSL4 gene deletion and found that ID with absent or severely delayed speech, midface hypoplasia, and facial hypotonia are consistent features observed in the absence of ACSL4 gene.
Alport 综合征伴智力障碍(ID)是一种连续基因缺失综合征,涉及 Xq22.3 上的几个基因,包括 COL4A5 和 ACSL4。我们报告了一个有两个男性患有这种疾病和 Xq22.3 缺失的家庭。荧光原位杂交和基因组分析将缺失区域定位在 COL4A5 的外显子 1 和 ACSL4 的外显子 12 之间。患者的母亲有镜下血尿,被发现为 Xq22.3 缺失的杂合子。对来自该家族受影响男性的淋巴母细胞系 RNA 进行逆转录聚合酶链反应分析显示,存在一个稳定的嵌合转录本,其中 ACSL4 的外显子 13-17 被 COL4A5 基因内含子 1 的一个隐蔽外显子取代。从这个转录本中预测到一个截断的 54 kDa 蛋白,但 Western blot 分析和 ACSL4 酶测定均显示 ACSL4 功能的完全缺失。我们还比较了该家系与三个先前报道的 ACSL4 基因缺失家系的临床特征,发现 ID 伴无或严重延迟言语、中面部发育不良和面神经张力减退是 ACSL4 基因缺失的共同特征。
