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Fertility and Sterility 2006-May

Investigation of the human stem cell factor KIT ligand gene, KITLG, in women with 46,XX spontaneous premature ovarian failure.

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Emily S Hui
Ekemini A Udofa
Jackeline Soto
Vien H Vanderhoof
Keith Zachman
Zhi-Bin Tong
Lawrence M Nelson

Nyckelord

Abstrakt

OBJECTIVE

To investigate mutations in the human KIT ligand gene (KITLG) gene as a mechanism of 46,XX spontaneous premature ovarian failure. The human KIT ligand gene, known also as human stem cell factor, is the ligand of the c-kit transmembrane tyrosine kinase receptor (KIT). This ligand-receptor interaction is known to play important roles in mouse germ cell migration and proliferation.

METHODS

Cross-sectional study.

METHODS

Clinical research center.

METHODS

Forty women with 46,XX spontaneous premature ovarian failure.

METHODS

None.

METHODS

Single-stranded conformational polymorphism analysis and DNA sequencing.

RESULTS

We found one nucleotide change of the KITLG coding region (811G-->T) that led to an alteration of the amino acid composition of the KITLG protein in one Caucasian patient (Asp210Tyr). However, we found the same alteration in two normal control Caucasian samples. Three nucleotide substitutions were found in the noncoding exon of KITLG (exon 10). We also identified two intronic polymorphisms. Thus, we did not identify a single significant mutation in the coding region of the KITLG gene in any of 40 patients (upper 95% confidence limit is 7.2%).

CONCLUSIONS

Mutations in the coding regions of the KITLG gene appear not to be a common cause of 46,XX spontaneous premature ovarian failure in North American women.

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