Van Kuilenburg A B, Vreken P, Abeling N G, Bakker H D, Meinsma R, Van Lenthe H, De Abreu R A, Smeitink J A, Kayserili H, Apak M Y, Christensen E, Holopainen I, Pulkki K, Riva D, Botteon G, Holme E, Tulinius M, Kleijer W J, Beemer F A, Duran M, Niezen-Koning K E, Smit G P, Jakobs C, Smit L M, Van Gennip A H
Academic Medical Center, University of Amsterdam, Emma Children's Hospital and Department of Clinical Chemistry, The Netherlands.
Hum Genet. 1999 Jan;104(1):1-9. doi: 10.1007/pl00008711.
Dihydropyrimidine dehydrogenase (DPD) deficiency is an autosomal recessive disease characterised by thymine-uraciluria in homozygous deficient patients and has been associated with a variable clinical phenotype. In order to understand the genetic and phenotypic basis for DPD deficiency, we have reviewed 17 families presenting 22 patients with complete deficiency of DPD. In this group of patients, 7 different mutations have been identified, including 2 deletions [295-298delTCAT, 1897delC], 1 splice-site mutation [IVS14+1G>A)] and 4 missense mutations (85T>C, 703C>T, 2658G>A, 2983G>T). Analysis of the prevalence of the various mutations among DPD patients has shown that the G-->A point mutation in the invariant splice donor site is by far the most common (52%), whereas the other six mutations are less frequently observed. A large phenotypic variability has been observed, with convulsive disorders, motor retardation and mental retardation being the most abundant manifestations. A clear correlation between the genotype and phenotype has not been established. An altered beta-alanine, uracil and thymine homeostasis might underlie the various clinical abnormalities encountered in patients with DPD deficiency.
二氢嘧啶脱氢酶(DPD)缺乏症是一种常染色体隐性疾病,其特征是纯合子缺陷患者出现胸腺嘧啶 - 尿嘧啶尿症,并且与多种临床表型相关。为了了解DPD缺乏症的遗传和表型基础,我们回顾了17个家庭,这些家庭中有22名患者存在完全性DPD缺乏。在这组患者中,已鉴定出7种不同的突变,包括2种缺失[295 - 298delTCAT,1897delC],1种剪接位点突变[IVS14 + 1G>A]和4种错义突变(85T>C,703C>T,2658G>A,2983G>T)。对DPD患者中各种突变发生率的分析表明,不变剪接供体位点的G→A点突变是迄今为止最常见的(52%),而其他六种突变较少见。已观察到较大的表型变异性,惊厥性疾病、运动发育迟缓及智力发育迟缓是最常见的表现。尚未确定基因型与表型之间存在明确的相关性。β-丙氨酸、尿嘧啶和胸腺嘧啶内稳态的改变可能是DPD缺乏症患者出现各种临床异常的基础。
