Identifying a novel mutation of CYP17A1 gene from five Chinese 17α-hydroxylase/17, 20-lyase deficiency patients

Mutations of CYP17A1 gene could cause complete or partial, combined or isolated 17α-hydroxylase/17,20-lyase enzyme deficiencies (17OHD). We intended to investigate the CYP17A1 mutation in five unrelated patients and analyze its possible influence on phenotype of an atypical 17OHD patient presented w...

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Bibliographic Details
Published in:Gene 2013-03, Vol.516 (2), p.345-350
Main Authors: Han, Bing, Liu, Wei, Zuo, Chun-Lin, Zhu, Hui, Li, Lu, Xu, Chao, Wang, Xia-Juan, Liu, Bing-Li, Pan, Chun-Ming, Lu, Ying-Li, Wu, Wan-Ling, Chen, Ming-Dao, Song, Huai-Dong, Cheng, Kai-Xiang, Qiao, Jie
Format: Article
Language:English
Subjects:
17α-Hydroxylase/17
20-Lyase deficiency
Adolescent
Adrenal Hyperplasia, Congenital - ethnology
Adrenal Hyperplasia, Congenital - genetics
Amino Acid Sequence
Asian Continental Ancestry Group - genetics
Base Sequence
Cells, Cultured
Congenital adrenal hyperplasia
Consanguinity
CYP17A1 gene
DNA Mutational Analysis
enzyme activity
enzyme deficiencies
exons
Female
genes
heterozygosity
homozygosity
Humans
hypertension
hypokalemia
Male
Male pseudohermaphroditism
missense mutation
Models, Molecular
Molecular Sequence Data
mutants
Mutation, Missense - physiology
patients
phenotype
site-directed mutagenesis
Steroid 17-alpha-Hydroxylase - chemistry
Steroid 17-alpha-Hydroxylase - genetics
steroid hormones
Young Adult
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Summary:Mutations of CYP17A1 gene could cause complete or partial, combined or isolated 17α-hydroxylase/17,20-lyase enzyme deficiencies (17OHD). We intended to investigate the CYP17A1 mutation in five unrelated patients and analyze its possible influence on phenotype of an atypical 17OHD patient presented with micropenis, hypertension and intermittent hypokalemia. Steroid hormones were assayed in these patients. A novel missense mutation (c.1169C>G, p. Thr390Arg) located in exon 7 was detected in one of the patients. Homozygous c. 985_987delinsAA, p. Tyr329fs mutation was found in two patients, while compound heterozygous mutations (c. 985_987delinsAA, p. Tyr329fs/c. 932–939 del, p. Val311fs and c. 287G>A, p. Arg96Gln/c. 985_987delinsAA, p. Tyr329fs) were found in two other patients, respectively. Then, steric model analysis of CYP17A1 showed that the novel mutation T390R changed the local structure as well as the electrostatic potential of the nearby beta sheet. Finally, site-directed mutagenesis and in vitro expression were used to analyze the activity of novel mutant CYP17A1. It indicated the T390R mutant retained part of enzyme activity, which was consistent to the clinical features. In conclusion, we identified a novel missense mutation of CYP17A1 gene from a patient with micropenis, hypertension and intermittent hypokalemia, which varied from other four patients. It also expanded our understanding of genotype–phenotype correlation of the disease. ► A novel missense mutation in CYP17A1 was detected in an atypical 17OHD patient.
ISSN:0378-1119
1879-0038
DOI:10.1016/j.gene.2012.12.010