Wagner Nicole, Wagner Kay-Dietrich, Afanetti Mickael, Nevo Fabien, Antignac Corinne, Michiels Jean-Francois, Schedl Andreas, Berard Etienne
INSERM, U636, Nice, France.
Pediatr Nephrol. 2008 Sep;23(9):1445-53. doi: 10.1007/s00467-008-0845-7. Epub 2008 May 31.
The Wilms' tumor suppressor gene WT1 is an important regulator of development. Mutations in this gene have been associated with Wilms' tumor, Frasier syndrome, and Denys-Drash syndrome, as well as isolated glomerular disease. Here we report the case of a 4-month-old girl, who presented with end-stage renal disease, thrombopenia, anemia, and cardiac hypertrophy accompanied by severe hypertension. Histological analysis of kidney biopsies revealed a massive and diffuse nephroblastomatosis with a dramatic reduction in the number of glomeruli. Although no normal cortical nephrons could be detected, medullary organization was nearly normal. Sequence analysis demonstrated a heterozygous nonsense mutation in exon 9 of WT1, which leads to a truncation of the WT1 protein at the beginning of zinc finger 3. Given the requirement of WT1 for normal development of the kidney and heart, these data raise the hypothesis that the mutation identified was responsible for the severe phenotype observed in our patient.
威尔姆斯肿瘤抑制基因WT1是发育的重要调节因子。该基因的突变与威尔姆斯肿瘤、弗雷泽综合征、丹尼斯-德拉什综合征以及孤立性肾小球疾病有关。在此,我们报告一例4个月大的女孩,她患有终末期肾病、血小板减少症、贫血和伴有严重高血压的心脏肥大。肾脏活检的组织学分析显示大量弥漫性肾母细胞瘤病,肾小球数量显著减少。虽然未检测到正常的皮质肾单位,但髓质结构几乎正常。序列分析表明WT1基因第9外显子存在杂合性无义突变,导致WT1蛋白在锌指3起始处截断。鉴于WT1对肾脏和心脏正常发育的必要性,这些数据提出了一个假设,即所鉴定的突变是导致我们患者出现严重表型的原因。
