Kuzucu Fatma-Nur, Kilic Mustafa, Sezer Abdullah, Has-Ozhan Selen, Yildiz Harun, Celen-Yoldas Tuba, Onat Fatma-Nese, Uyanik Melike
Department of Pediatrics, Sami Ulus Children Hospital, Ankara, Turkey.
Department of Pediatrics, University of Health Sciences, Sami Ulus Children Hospital, Metabolism Unit, Babur Cad. No: 44, 06080, Altındag, Ankara, Turkey.
Metab Brain Dis. 2025 Apr 28;40(5):193. doi: 10.1007/s11011-025-01582-1.
Phenylketonuria (PKU) is an autosomal recessive disorder of phenylalanine metabolism, in which especially high phenylalanine concentrations cause brain dysfunction. If untreated, this brain dysfunction results in severe intellectual disability, epilepsy, and behavioural problems. We aimed to investigate demographic, clinical, biochemical, and molecular genetic data in patients with phenylalanine metabolism disorder. This study included 99 predominantly Turkish patients diagnosed with phenylalanine metabolism disorder, primarily referred through newborn screening programs. These patients were evaluated at a single center over a 9-year period, from 2013 to 2021. Demographic, clinical, molecular and laboratory data were collected retrospectively. Among the 99 patients, 93 (93.9%) had hyperphenylalaninemia-phenylketonuria, 2 (2.0%) had tetrahydrobiopterin metabolism disorders [one due to 6-pyruvoyl-tetrahydropterin synthase (PTPS) deficiency and the other due to dihydropteridine reductase (DHPR) deficiency], 3 (3.0%) had maternal PKU syndrome (one of whom also had mild phenylketonuria), and 1 (1.0%) had transient hyperphenylalaninemia. The majority of patients belonged to the mild hyperphenylalaninemia-not requiring treatment group. A total of 33 different alleles and 40 genotypes (59.6% compound heterozygous) were identified in the PAH gene, with missense variants accounting for the largest proportion (72.7%). The most frequent PAH gene variants were c.898G > T p.(Ala300Ser) (14.9%), c.1066-11G > A (8.5%), and c.1208C > T p.(Ala403Val) (8.5%), while the most common genotypes were c.898G > T p.(Ala300Ser)/c.898G > T p.(Ala300Ser) (6.4%) and c.898G > T p.(Ala300Ser) /c.1066-11G > A (6.4%), respectively. Among patients with mild hyperphenylalaninemia-not requiring treatment, the predominant genotypes were c.898G > T p.(Ala300Ser)/c.898G > T p.(Ala300Ser) (11.1%), c.898G > T p.(Ala300Ser)/c.1066-11G > A (11.1%), and c.1208C > T p.(Ala403Val)/c.1208C > T p.(Ala403Val) (7.4%), whereas c.842C > T p.(Pro281Leu)/c.842C > T p.(Pro281Leu) (33.3%) was frequently observed in classic PKU patients. The national newborn screening program has significantly improved the prognosis and quality of life for patients through early diagnosis and timely treatment. While the prevalence of hyperphenylalaninemia-phenylketonuria remains high in Turkey, the higher frequency of the hyperphenylalaninemia-not requiring treatment group, compared to European and Asian countries, is considered a favorable outcome. Additionally, the PAH genotype is identified as the primary determinant of the PKU phenotype.
苯丙酮尿症(PKU)是一种苯丙氨酸代谢的常染色体隐性疾病,其中特别高的苯丙氨酸浓度会导致脑功能障碍。如果不进行治疗,这种脑功能障碍会导致严重智力残疾、癫痫和行为问题。我们旨在调查苯丙氨酸代谢障碍患者的人口统计学、临床、生化和分子遗传学数据。本研究纳入了99例主要为土耳其人的苯丙氨酸代谢障碍患者,这些患者主要通过新生儿筛查项目转诊而来。在2013年至2021年的9年期间,这些患者在单一中心接受了评估。人口统计学、临床、分子和实验室数据均为回顾性收集。99例患者中,93例(93.9%)患有高苯丙氨酸血症 - 苯丙酮尿症,2例(2.0%)患有四氢生物蝶呤代谢障碍[1例因6 - 丙酮酰四氢蝶呤合酶(PTPS)缺乏,另1例因二氢蝶啶还原酶(DHPR)缺乏],3例(3.0%)患有母体苯丙酮尿症综合征(其中1例还患有轻度苯丙酮尿症),1例(1.0%)患有短暂性高苯丙氨酸血症。大多数患者属于轻度高苯丙氨酸血症 - 无需治疗组。在PAH基因中总共鉴定出33种不同的等位基因和40种基因型(59.6%为复合杂合子),错义变异占比最大(72.7%)。最常见的PAH基因变异为c.898G>T p.(Ala300Ser)(14.9%)、c.1066 - 11G>A(8.5%)和c.1208C>T p.(Ala403Val)(8.5%),而最常见的基因型分别为c.898G>T p.(Ala300Ser)/c.898G>T p.(Ala300Ser)(6.4%)和c.898G>T p.(Ala300Ser)/c.1066 - 11G>A(6.4%)。在轻度高苯丙氨酸血症 - 无需治疗的患者中,主要基因型为c.898G>T p.(Ala300Ser)/c.898G>T p.(Ala300Ser)(11.1%)、c.898G>T p.(Ala300Ser)/c.1066 - 11G>A(11.1%)和c.1
