A homozygous intronic branch-point deletion in the ALPL gene causes infantile hypophosphatasia
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- 作者:Birgit Mentrupa ; b-mentrup.klh@uni-wuerzburg.de ; Hermann Girschickb ; Franz Jakoba ; Christine Hofmannc
- 关键词:Hypophosphatasia ; Alkaline phosphatase ; Intron deletion ; Splicing ; Branch-point ; Transcript variant
- 刊名:Bone
- 出版年:2017
- 出版时间:January 2017
- 年:2017
- 卷:94
- 期:Complete
- 页码:75-83
- 全文大小:1168 K
- 卷排序:94
文摘
The first functional characterization of a mutation located in an intron of the ALPL gene A 20 bp deletion was discovered in a boy with infantile hypophosphatasia. The homozygous loss of a branch point motif in intron 7 results in a truncated non-functional TNAP enzyme. Nevertheless a certain amount of residual TNAP activity has been preserved probably ensuring the survival of the disease.