次黄嘌呤鸟嘌呤磷酸核糖转移酶(HPRT)缺乏症:日本新家族中的HPRT1突变与磷酸核糖焦磷酸(PRPP)浓度
Hypoxanthine guanine phosphoribosyltransferase (HPRT) deficiencies: HPRT1 mutations in new Japanese families and PRPP concentration.
作者信息
Yamada Yasukazu, Nomura Noriko, Yamada Kenichiro, Kimura Reiko, Fukushi Daisuke, Wakamatsu Nobuaki, Matsuda Yasufumi, Yamauchi Takahiro, Ueda Takanori, Hasegawa Hiroshi, Nakamura Makiko, Ichida Kimiyoshi, Kaneko Kiyoko, Fujimori Shin
机构信息
a Department of Genetics, Institute for Developmental Research , Aichi Human Service Center , Aichi , Japan.
出版信息
Nucleosides Nucleotides Nucleic Acids. 2014;33(4-6):218-22. doi: 10.1080/15257770.2013.865743.
Mutation of hypoxanthine guanine phosphoribosyltransferase (HPRT) gives rise to Lesch-Nyhan syndrome, which is characterized by hyperuricemia, severe motor disability, and self-injurious behavior, or HPRT-related gout with hyperuricemia. Four mutations were detected in two Lesch-Nyhan families and two families with partial deficiency since our last report. A new mutation of G to TT (c.456delGinsTT) resulting in a frameshift (p.Q152Hfs3) in exon 3 has been identified in one Lesch-Nyhan family. In the other Lesch-Nyhan family, a new point mutation in intron 7 (c.532+5G>T) causing splicing error (exon 7 excluded, p.L163Cfs4) was detected. In the two partial deficiency cases with hyperuricemia, two missense mutations of p.D20V (c.59A>T) and p.H60R (c.179A>G) were found. An increase of erythrocyte PRPP concentration was observed in the respective phenotypes and seems to be correlated with disease severity.
次黄嘌呤鸟嘌呤磷酸核糖转移酶(HPRT)突变会引发莱施-奈恩综合征,其特征为高尿酸血症、严重运动功能障碍和自伤行为,或伴有高尿酸血症的HPRT相关痛风。自我们上次报告以来,在两个莱施-奈恩家族和两个部分缺乏症家族中检测到了四种突变。在一个莱施-奈恩家族中,已鉴定出一种新的G突变为TT(c.456delGinsTT)的突变,导致外显子3发生移码(p.Q152Hfs3)。在另一个莱施-奈恩家族中,检测到内含子7中的一个新的点突变(c.532+5G>T),导致剪接错误(外显子7被排除,p.L163Cfs4)。在两例伴有高尿酸血症的部分缺乏症病例中,发现了p.D20V(c.59A>T)和p.H60R(c.179A>G)这两种错义突变。在各自的表型中观察到红细胞PRPP浓度升高,且似乎与疾病严重程度相关。
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