Ugur Sibel Aylin, Tolun Aslihan
Department of Molecular Biology and Genetics, Boaziçi University, Istanbul 34342, Turkey.
Hum Mol Genet. 2008 Sep 1;17(17):2644-53. doi: 10.1093/hmg/ddn164. Epub 2008 May 30.
Split-Hand/Foot Malformation (SHFM) is a complex limb malformation affecting the central rays of the autopod. We studied a large consanguineous kindred afflicted with autosomal recessive SHFM. Twelve affected members had central feet reductions with or without hand involvement while the remaining one had the mildest phenotype and atypical SHFM. We identified by homozygosity mapping a novel SHFM locus at 12q13.11-q13 with a maximum multipoint lod score of 5.47 and by subsequent candidate gene approach a homozygous missense WNT10b mutation (p.R332W) in all affected individuals but the atypical case plus in an asymptomatic female. We propose that either a second locus contributes to the manifestation of SHFM phenotype or a suppressor locus prevented trait manifestation in the non-penetrant female. We also investigated linkage to the five known SHFM loci. Four of the loci were excluded, while in TP63 [tumor protein p63 (SHFM4)], the only known gene responsible for SHFM, we detected in most affected subjects a rare insertion variant (rs34201045) at the alternate promoter used for transcription of the N-terminal-truncated p63 isotype. This is the first reported WNT10b mutation on the pathogenesis of limb development and recessive mutation in SHFM.
裂手/裂足畸形(SHFM)是一种影响手足中央射线的复杂肢体畸形。我们研究了一个患有常染色体隐性SHFM的大型近亲家族。12名受累成员出现中央足部发育不全,伴或不伴有手部受累,而其余一名成员具有最轻微的表型和非典型SHFM。我们通过纯合性定位在12q13.11-q13确定了一个新的SHFM基因座,最大多点对数计分达到5.47,随后通过候选基因方法在除非典型病例外的所有受累个体以及一名无症状女性中发现了一个纯合错义WNT10b突变(p.R332W)。我们提出,要么是第二个基因座导致了SHFM表型的显现,要么是一个抑制基因座阻止了该性状在非显性女性中的显现。我们还研究了与五个已知SHFM基因座的连锁关系。其中四个基因座被排除,而在TP63 [肿瘤蛋白p63(SHFM4)](唯一已知的与SHFM相关的基因)中,我们在大多数受累受试者中检测到一个罕见的插入变异(rs34201045),该变异位于用于转录N端截短的p63同种型的交替启动子处。这是首次报道的关于肢体发育发病机制的WNT10b突变以及SHFM中的隐性突变。
