Gathof B S, Sommer M, Podskarbi T, Reichardt J, Braun A, Gresser U, Shin Y S
Medizinische Poliklinik, University of Munich, Germany.
Hum Genet. 1995 Dec;96(6):721-5. doi: 10.1007/BF00210306.
Classical galactosemia, which is caused by deficiency of galactose-1-phosphate uridyltransferase, is characterized by acute problems of hepatocellular dysfunction, sepsis, cataracts and failure to thrive. Galactose limitation reverses these symptoms immediately; however, the long-term complications, such as mental retardation and ovarian failures are major problems in most of these patients. In order to investigate the molecular basis for phenotype variation in galactosemia, we have screened the most common mutation in the GALT gene, Q188R. We have further examined those patients who are heterozygous for Q188R or negative for this mutation by SSCP analysis and direct sequencing. In three male patients, we have identified, for the first time, two stop-codon mutations in the GALT gene, G212X (exon 7) and E340X (exon 10). Two patients of 8 and 28 years of age, respectively, who are compound heterozygotes for Q188R and G212X, have severe mental retardation and their general clinical condition is more severe than that of patients with missense mutations. The third patient, who is 8 years of age and who is homozygous for E340X, the N314D polymorphism and a silent substitution L218L, presents with a relatively normal physical and mental condition to date.
经典型半乳糖血症由1-磷酸半乳糖尿苷转移酶缺乏引起,其特征为肝细胞功能障碍、败血症、白内障和发育不良等急性问题。限制半乳糖摄入可立即逆转这些症状;然而,智力迟钝和卵巢功能衰竭等长期并发症是大多数此类患者的主要问题。为了研究半乳糖血症表型变异的分子基础,我们筛查了GALT基因中最常见的突变Q188R。我们通过单链构象多态性分析和直接测序进一步检测了那些Q188R杂合或该突变阴性的患者。在三名男性患者中,我们首次在GALT基因中鉴定出两个终止密码子突变,即G212X(第7外显子)和E340X(第10外显子)。两名分别为8岁和28岁的患者,是Q188R和G212X的复合杂合子,有严重智力迟钝,其总体临床状况比错义突变患者更严重。第三名患者8岁,是E340X纯合子,同时存在N314D多态性和沉默替代L218L,迄今为止其身体和精神状况相对正常。
