Almoguera Berta, He Sijie, Corton Marta, Fernandez-San Jose Patricia, Blanco-Kelly Fiona, López-Molina Maria Isabel, García-Sandoval Blanca, Del Val Javier, Guo Yiran, Tian Lifeng, Liu Xuanzhu, Guan Liping, Torres Rosa J, Puig Juan G, Hakonarson Hakon, Xu Xun, Keating Brendan, Ayuso Carmen
Center for Applied Genomics, The Children's Hospital of Philadelphia, Philadelphia, PA, 19104, USA.
College of Life Sciences, University of Chinese Academy of Sciences, Beijing, 100049, China.
Orphanet J Rare Dis. 2014 Dec 10;9:190. doi: 10.1186/s13023-014-0190-9.
Phosphoribosyl pyrophosphate synthetase (PRS) I deficiency is a rare medical condition caused by missense mutations in PRPS1 that lead to three different phenotypes: Arts Syndrome (MIM 301835), X-linked Charcot-Marie-Tooth (CMTX5, MIM 311070) or X-linked non-syndromic sensorineural deafness (DFN2, MIM 304500). All three are X-linked recessively inherited and males affected display variable degree of central and peripheral neuropathy. We applied whole exome sequencing to a three-generation family with optic atrophy followed by retinitis pigmentosa (RP) in all three cases, and ataxia, progressive peripheral neuropathy and hearing loss with variable presentation.
Whole exome sequencing was performed in two affecteds and one unaffected member of the family. Sanger sequencing was used to validate and segregate the 12 candidate mutations in the family and to confirm the absence of the novel variant in PRPS1 in 191 controls. The pathogenic role of the novel mutation in PRPS1 was assessed in silico and confirmed by enzymatic determination of PRS activity, mRNA expression and sequencing, and X-chromosome inactivation.
A novel missense mutation was identified in PRPS1 in the affected females. Age of onset, presentation and severity of the phenotype are highly variable in the family: both the proband and her mother have neurological and ophthalmological symptoms, whereas the phenotype of the affected sister is milder and currently confined to the eye. Moreover, only the proband displayed a complete lack of expression of the wild type allele in leukocytes that seems to correlate with the degree of PRS deficiency and the severity of the phenotype. Interestingly, optic atrophy and RP are the only common manifestations to all three females and the only phenotype correlating with the degree of enzyme deficiency.
These results are in line with recent evidence of the existence of intermediate phenotypes in PRS-I deficiency syndromes and demonstrate that females can exhibit a disease phenotype as severe and complex as their male counterparts.
磷酸核糖焦磷酸合成酶(PRS)I缺乏症是一种罕见的医学病症,由PRPS1中的错义突变引起,导致三种不同的表型:阿茨综合征(MIM 301835)、X连锁型夏科-马里-图思病(CMTX5,MIM 311070)或X连锁型非综合征性感音神经性耳聋(DFN2,MIM 304500)。这三种病症均为X连锁隐性遗传,受影响的男性表现出不同程度的中枢和周围神经病变。我们对一个三代家族进行了全外显子组测序,该家族的三名患者均先出现视神经萎缩,随后发展为色素性视网膜炎(RP),同时伴有共济失调、进行性周围神经病变和表现各异的听力损失。
对该家族的两名患者和一名未受影响的成员进行了全外显子组测序。采用桑格测序法对家族中的12个候选突变进行验证和分离,并确认191名对照中不存在PRPS1中的新变异。通过计算机模拟评估PRPS1中新突变的致病作用,并通过PRS活性的酶学测定、mRNA表达和测序以及X染色体失活进行确认。
在受影响的女性中,PRPS1中鉴定出一个新的错义突变。该家族中发病年龄、表现和表型严重程度差异很大:先证者及其母亲均有神经和眼科症状,而受影响妹妹的表型较轻,目前仅限于眼部。此外,只有先证者的白细胞中完全缺乏野生型等位基因的表达,这似乎与PRS缺乏程度和表型严重程度相关。有趣且值得注意的是,视神经萎缩和RP是所有三名女性唯一共同的表现,也是唯一与酶缺乏程度相关的表型。
这些结果与最近关于PRS-I缺乏综合征中存在中间表型的证据一致,并表明女性可表现出与男性同样严重和复杂的疾病表型。
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