Weh E, Reis L M, Tyler R C, Bick D, Rhead W J, Wallace S, McGregor T L, Dills S K, Chao M-C, Murray J C, Semina E V
Department of Pediatrics, Children's Research Institute, Medical College of Wisconsin, Children's Hospital of Wisconsin, Milwaukee, WI, USA; Department of Cell Biology, Neurobiology and Anatomy, Medical College of Wisconsin, Milwaukee, WI, USA.
Clin Genet. 2014 Aug;86(2):142-8. doi: 10.1111/cge.12241. Epub 2013 Sep 17.
Peters plus syndrome (PPS) is a rare autosomal-recessive disorder characterized by Peters anomaly of the eye, short stature, brachydactyly, dysmorphic facial features, developmental delay, and variable other systemic abnormalities. In this report, we describe screening of 64 patients affected with PPS, isolated Peters anomaly and PPS-like phenotypes. Mutations in the coding region of B3GALTL were identified in nine patients; six had a documented phenotype of classic PPS and the remaining three had a clinical diagnosis of PPS with incomplete clinical documentation. A total of nine different pathogenic alleles were identified. Five alleles are novel including one frameshift, c.168dupA, p.(Gly57Argfs11), one nonsense, c.1234C>T, p.(Arg412), two missense, c.1045G>A, p.(Asp349Asn) and c.1181G>A, p.(Gly394Glu), and one splicing, c.347+5G>T, mutations. Consistent with previous reports, the c.660+1G>A mutation was the most common mutation identified, seen in eight of the nine patients and accounting for 55% of pathogenic alleles in this study and 69% of all reported pathogenic alleles; while two patients were homozygous for this mutation, the majority had a second rare pathogenic allele. We also report the absence of B3GALTL mutations in 55 cases of PPS-like phenotypes or isolated Peters anomaly, further establishing the strong association of B3GALTL mutations with classic PPS only.
彼得斯综合征(PPS)是一种罕见的常染色体隐性疾病,其特征为眼部彼得斯异常、身材矮小、短指畸形、面部畸形、发育迟缓以及其他各种系统性异常。在本报告中,我们描述了对64例患有PPS、孤立性彼得斯异常和PPS样表型患者的筛查情况。在9例患者中鉴定出B3GALTL编码区的突变;6例具有经典PPS的记录表型,其余3例临床诊断为PPS但临床记录不完整。共鉴定出9种不同的致病等位基因。其中5个等位基因为新发现的,包括1个移码突变,c.168dupA,p.(Gly57Argfs11);1个无义突变,c.1234C>T,p.(Arg(412));2个错义突变,c.1045G>A,p.(Asp349Asn)和c.1181G>A,p.(Gly394Glu);以及1个剪接突变,c.347+5G>T。与先前的报告一致,c.660+1G>A突变是鉴定出的最常见突变,在9例患者中的8例中出现,占本研究中致病等位基因的55%以及所有报告致病等位基因的69%;虽然2例患者为此突变的纯合子,但大多数患者还有另一个罕见的致病等位基因。我们还报告了在55例PPS样表型或孤立性彼得斯异常病例中未发现B3GALTL突变,进一步证实了B3GALTL突变仅与经典PPS密切相关。
