Département de Biologie des Tumeurs, Institut Curie, Paris, France.
Eur J Hum Genet. 2013 Apr;21(4):460-4. doi: 10.1038/ejhg.2012.186. Epub 2012 Aug 22.
Retinoblastoma (Rb) results from inactivation of both alleles of the RB1 gene located in 13q14.2. Whole-germline monoallelic deletions of the RB1 gene (6% of RB1 mutational spectrum) sometimes cause a variable degree of psychomotor delay and several dysmorphic abnormalities. Breakpoints in 12 Rb patients with or without psychomotor delay were mapped to specifically define the role of chromosomal regions adjacent to RB1 in psychomotor delay. A high-resolution CGH array focusing on RB1 and its flanking region was designed to precisely map the deletion. Comparative analysis detected a 4-Mb critical interval, including a candidate gene protocadherin 8 (PCDH8). PCDH8 is thought to function in signalling pathways and cell adhesion in a central nervous system-specific manner, making loss of PCDH8 one of the probable causes of psychomotor delay in RB1-deleted patients. Consequently, we propose to systematically use high-resolution CGH in cases of partial or complete RB1 deletion encompassing the telomeric flanking region to characterize the putative loss of PCDH8 and to better define genotype/phenotype correlations, eventually leading to optimized genetic counselling and psychomotor follow-up.
视网膜母细胞瘤(Rb)是由于位于 13q14.2 上的 RB1 基因的两个等位基因失活引起的。RB1 基因的全种系单等位基因缺失(RB1 突变谱的 6%)有时会导致不同程度的精神运动发育迟缓以及多种发育异常。有或没有精神运动发育迟缓的 12 名 Rb 患者的断裂点被定位,以专门确定 RB1 附近染色体区域在精神运动发育迟缓中的作用。设计了一个针对 RB1 及其侧翼区域的高分辨率 CGH 阵列,以精确绘制缺失图。比较分析检测到一个包含候选基因原钙黏蛋白 8(PCDH8)的 4Mb 关键间隔。PCDH8 被认为以中枢神经系统特异性的方式在信号通路和细胞黏附中发挥作用,因此 PCDH8 的缺失是 RB1 缺失患者精神运动发育迟缓的可能原因之一。因此,我们建议在包含端粒侧翼区域的部分或完全 RB1 缺失的情况下系统地使用高分辨率 CGH,以表征 PCDH8 的潜在缺失,并更好地定义基因型/表型相关性,最终导致优化的遗传咨询和精神运动随访。
