糖原累积病Ⅰa型分子遗传学家系研究

目的 研究1例糖原累积病Ⅰa型患者发病的分子遗传学机制。方法 从全血中抽提患者及其父母、姐姐和正常人基因组DNA,通过多聚酶链反应扩增葡萄糖-6-磷酸酶(G6Pase)基因的5个外显子,用DNA直接测序法确定其突变位点;测定患者父母亲及其姐姐的相应序列,确定突变的遗传来源。结果 患者G6Pase基因外显子5发生单个碱基纯合突变,突变碱基位于序列第727位,由G转变为T,造成剪切位点突变。患者父母亲和姐姐的G6Pase基因外显子5均发生727G→T杂合突变。结论 糖原累积病Ⅰa型可直接进行DNA分析以明确诊断,葡萄糖-6-磷酸酶外显子5的727G→T突变的发生在中国人中的发生率有待进一步研究。

citrin缺陷导致的新生儿肝内胆汁淤积症12例临床和实验室研究

目的探讨citrin缺陷导致的新生儿肝内胆汁淤积症(NICCD)患儿的临床表现和实验室检查的特点。方法对12例肝内胆汁淤积和黄疸患儿进行常规实验室检查,结合血串联质谱分析、尿气相色谱质谱分析诊断为NICCD。对确诊患儿的临床表现、常规实验室检查、血氨基酸谱和酰基肉碱谱、尿有机酸等进行分析。结果NICCD患儿出生体重偏低。实验室改变包括-γ谷氨酰转移酶、碱性磷酸酶以及甲胎蛋白升高、高胆红素血症、低蛋白血症、凝血酶原时间延长。有明显低血糖6例,有轻度高氨血症3例,有半乳糖血症仅1例。3例肝活检病理提示肝内胆汁淤积和肝细胞脂肪变性。串联质谱分析发现多数患儿有特异性瓜氨酸、蛋氨酸、苏氨酸和酪氨酸明显升高,以及游离肉碱、C2、C3和长链酰基肉碱升高。尿气相色谱质谱有机酸分析有尿4-羟基苯乳酸、4-羟基苯丙酮酸和4-羟基苯乙酸升高。结论不明原因黄疸患儿鉴别诊断应考虑到NICCD,早期进行串联质谱分析对明确NICCD的诊断具有重要意义。[临床儿科杂志,2007,25(12):983-987]

异戊酸血症一例临床及异戊酰辅酶A脱氢酶基因突变研究

目的了解异戊酸血症患儿的临床、实验室特点以及异戊酰辅酶A脱氢酶（IVD）基因突变情况。方法对1例异戊酸血症患儿的病史、实验室检查以及血串联质谱和尿气相色谱质谱结果进行了分析，对IVD基因12个外显子及两端内含子行PCR扩增和DNA测序，限制性内切酶片段长度多态性分析c．466G〉C（G127A）新突变。结果患儿男，2岁7个月，生后3d起出现呕吐和酸中毒，行幽门切开术后仍反复呕吐，伴有酸中毒发作，智力发育明显落后。血串联质谱分析显示C5酰基肉碱水平增高至12．89μmol／L，尿气相色谱质谱分析显示异戊酰甘氨酸明显升高，临床诊断为异戊酸血症。IVD基因DNA测序显示，患儿存在复合杂合突变：c．149G〉A（R21H）和c．466G〉C（G127A），c．466G〉C（G127A）突变在／VD基因第5外显子上，是以往未报道的新突变。结论报道1例异戊酸血症，新生儿期发病，反复呕吐，酸中毒和智力落后，血C5酰基肉碱明显升高，尿中有异戊酰、甘氨酸大量排出，基因诊断发现1个IVD基因新突变。

葡萄糖6磷酸酶基因热点突变检测结合1176多态位点连锁分析快速产前诊断Ia型糖原累积病

目的探讨中国人Ia型糖原累积病简便、快速、准确的产前诊断方法。方法通过限制性内切酶图谱分析了葡萄糖6磷酸酶(glucose-6-phosphatase,G6Pase)基因727G→T和R83H的突变,并结合1176位点单核苷酸多态性连锁分析,对3个Ia型糖原累积病家系进行了基因诊断和产前诊断。对发现的突变及1176位点多态性用DNA测序证实。结果3个家系先证者G6Pase基因的2个等位基因均携带727G→T突变,分别来自其父母。家系1和3胎儿为727G→T突变杂合子;家系2胎儿不携带该突变。1176位点单核苷酸多态性分析显示,3名胎儿1176位点单核苷酸多态性与3名先证者不同。DNA直接测序结果与限制性内切酶图谱分析结果相符。家系1和家系2胎儿已出生,并证实与产前诊断结果相符。结论通过限制性内切酶酶切法筛查727G→T和R83H突变结合1176位点单核苷酸多态性连锁分析可简便、快速、准确地诊断和产前诊断Ia型糖原累积病。

12例多种羧化酶缺乏症的基因突变分析

目的旨在从基因水平证实多种羧化酶缺乏症（multiplecarboxylasedeficiency，MCD）的诊断，探讨我国MCD患儿的基因突变情况。方法12例MCD患儿接受基因诊断。采用PCR及直接测序法分别对4例生物素酶（biotinidase，BT）缺乏症和8例全羧化酶合成酶（holocarboxylasesynthetas，HLCS）缺乏症进行BT基因和HLCS基因突变分析，对基因新突变通过限制性片段长度多态性分析及患儿父母和50名正常对照者基因检测以证实。结果12例患儿基因突变检出率100％。4例BT缺乏症中发现BT基因突变6种：C．98104del7ins3，C．1369G〉A（V457M），C．1157G〉A（W386X），C．1284C〉A（Y428X），C．1384delA，c-493—1494insT，后4种为新突变。8例HLCS缺乏症中发现HLCS基因突变4种：c．126G〉T（E42D）,c．1994G〉C（R665P），c．1088T〉A（V363D），c．1522C〉T（RS08W），后两种为热点突变[75％（12／16）]，c．1994G〉C为新突变。结论本研究从基因水平上证实了12例MCD的诊断。共发现了6种BT基因突变，4种HLCS基因突变，其中5种为新突变；得出2种HLCS基因的热点突变。

Screening for tetrahydrobiopterin deficiency among hyperphenylalaninemia patients in Southern China

Abstract Objectives To assess the incidence of tetrahydrobiopterin (BH4)deficiency among patients with hyperphenylalaninemia (HPA) in southern Chinese and evaluate clinical outcome and gene mutations in tetrahydrobiopterin deficient patients.Methods Urinary neopterin (N) and biopterin (B) was analyzed in 87 patients with hyperphenylalaninemia by high-performance liquid chromatography. Further combined loading tests with phenylalanine(Phe) (100*!mg/kg) and tetrahydrobiopterin (BH4) (7.5*!mg/kg) were performed in suspected patients with abnormal urinary pterin profiles. Gene mutation analysis was performed for patients with BH4 deficiency and their parents. BH4 deficient patients were treated with BH4 and neurotransmitter precursors after diagnosis. Blood phenylalanine levels, clinical symptoms and mental development were followed up.Results Eleven patients were diagnosed as having BH4 deficiency caused by 6-pyruvoyl tetrahydropterin synthase (PTPS) deficiency. The incidence of tetrahydrobiopterin (BH4) deficiency among patients with hyperphenylalaninemia (HPA) in southern Chinese was 10%. Combined loading tests with phenylalanine and oral BH4 were done in 4 of 11 patients and their phenylalanine levels were decreased to normal 4-6h after BH4 administration. Four different mutations (P87S, N52S, D96N and G144R) in the PTPS gene were detected in 5 families. Five PTPS-deficient patients were treated with synthetic BH4, neurotransmitter precursors (L-dopa plus carbidopa, and 5-hydroxytryptophan). They had satisfactory physical and mental development after treatment. One patient with partial PTPS deficiency had normal growth and mental development without treatment. Conclusions Our results emphasize that screening for BH4 deficiency should be carried out in all patients with hyperphenylalaninemia in order to minimize the misdiagnosis. Patients with BH4 deficiency should be treated early with BH4 and a combination of neurotransmitter precursors.