关键词: 低钠高钾血症, 基因检测, 先天性肾上腺皮质增生症, 假性醛固酮减少症, 醛固酮减少症, 先天性肾上腺发育不良

Abstract:

Objective    To analyze the causes of infant salt losing syndrome and the application value of gene detection in the diagnosis of the cause. Methods    Four cases of salt losing syndrome with low sodium and high potassium admitted from 2010 to 2014 in Shanghai Children’s Medical Center， Affiliated to Shanghai Jiaotong University School of Medicine were included and clinical data，therapy and follow-up were collected. DNA of children and their parents in the four cases were detected. Results    There were different degrees of salt losing situation in the four cases. It found that the patients had different gene mutations through genetic testing：mutations of splicing site［c.293-13A＞G（heterozygous）］ and small duplication［c.923dupT， p.Leu308Phefs*6（heterozygous）］ were detected in CYP21A2， mutation of small deletion［c.1334delC， p.Ala445Valfs*17（hemizygous）］ was detected in DAX1， mutation of splicing site［c.del1311G， p.Arg438Glyfs*43（heterozygous）］ and point mutation ［c.1439+1G＞C（heterozygous）］ were detected in SCNN1A and mutation of splicing site［c.240-1G＞A（heterozygous）］ and  nonsense mutation［c.1009C＞T， p.Gln337*（heterozygous）］ were detected in CYP11B2， respectively. The four cases were diagnosed as four different diseases： congenital adrenal hyperplasia （21-hydroxylase deficiency）， congenital adrenal hypoplasia， pseudohypoaldosteronism type I and hypoaldosteronism. Conclusion    The cause of infant salt losing syndrome is complex and is misdiagnosed easily. Gene analysis may be helpful for early diagnosis and treatment.

Key words: low sodium hyperkalemia；gene , detection；congenital adrenal hyperplasia；pseudohypoaldosteronism；hypoaldosteronism；congenital adrenal hypoplasia