TY - JOUR
T1 - 45,X/46,X,psu dic(Y) gonadal dysgenesis
T2 - influence of the two cell lines on the clinical phenotype, including gonadal histology
AU - Kaprova-Pleskacova, J
AU - Snajderova, M
AU - Stoop, J
AU - Koudova, M
AU - Kocarek, E
AU - Novotna, D
AU - Drop, S L S
AU - Obermannova, B
AU - Lebl, J
AU - Oosterhuis, J W
AU - Looijenga, L H J
N1 - © 2013 S. Karger AG, Basel.
PY - 2013
Y1 - 2013
N2 - A child born with ambiguous genitalia (Prader III) was found to have a 45,X[92.2%]/46,X,psu dic(Y)(p12)[7.8%] karyotype in peripheral blood lymphocytes. The testosterone level was consistent with that of a normal male; however, gonadotropins were elevated. Ultrasound and endoscopy of the urogenital sinus revealed well-developed Müllerian structures. At 3.5 months, the child was operated for right-sided incarcerated hernia, and the gonad situated at the inguinal region was biopsied and classified as primitive testis. Based on the presence of Müllerian structures, anatomy of external genitalia and wish of the parents, the child was assigned female gender. She underwent removal of the left gonad at 4 months during another acute surgery; histology was similar to the right gonad. The rest of the right gonad was removed at 16 months, and feminizing genitoplasty took place at 3 years. The right and left gonad contained 28 and 22% of cells with a Y chromosome, respectively. During further histological examination, dysgenetic features of the gonads were discovered. Some germ cells displayed abnormal development based on the specific expression of immunohistochemical markers (OCT3/4, TSPY, KITLG), indicating a possible risk for future malignant germ cell tumor development. Contribution of the 45,X cell line to the phenotype was also observed: the patient developed celiac disease, and her growth pattern resembled that of Turner syndrome responding to growth hormone treatment.
AB - A child born with ambiguous genitalia (Prader III) was found to have a 45,X[92.2%]/46,X,psu dic(Y)(p12)[7.8%] karyotype in peripheral blood lymphocytes. The testosterone level was consistent with that of a normal male; however, gonadotropins were elevated. Ultrasound and endoscopy of the urogenital sinus revealed well-developed Müllerian structures. At 3.5 months, the child was operated for right-sided incarcerated hernia, and the gonad situated at the inguinal region was biopsied and classified as primitive testis. Based on the presence of Müllerian structures, anatomy of external genitalia and wish of the parents, the child was assigned female gender. She underwent removal of the left gonad at 4 months during another acute surgery; histology was similar to the right gonad. The rest of the right gonad was removed at 16 months, and feminizing genitoplasty took place at 3 years. The right and left gonad contained 28 and 22% of cells with a Y chromosome, respectively. During further histological examination, dysgenetic features of the gonads were discovered. Some germ cells displayed abnormal development based on the specific expression of immunohistochemical markers (OCT3/4, TSPY, KITLG), indicating a possible risk for future malignant germ cell tumor development. Contribution of the 45,X cell line to the phenotype was also observed: the patient developed celiac disease, and her growth pattern resembled that of Turner syndrome responding to growth hormone treatment.
KW - Body Height
KW - Body Weight
KW - Celiac Disease/complications
KW - Chromosomes, Human, Y/genetics
KW - Disorders of Sex Development/genetics
KW - Female
KW - Gonadal Dysgenesis, Mixed/genetics
KW - Gonads/chemistry
KW - Human Growth Hormone/therapeutic use
KW - Humans
KW - Immunohistochemistry
KW - Male
KW - Mosaicism
KW - Octamer Transcription Factor-3/analysis
KW - Phenotype
KW - Sex Chromosome Aberrations
KW - Testis/pathology
KW - Turner Syndrome/genetics
KW - Uterus/pathology
UR - http://www.scopus.com/inward/record.url?scp=84891132596&partnerID=8YFLogxK
U2 - 10.1159/000356173
DO - 10.1159/000356173
M3 - Article
C2 - 24247294
SN - 1661-5425
VL - 7
SP - 282
EP - 288
JO - Sexual development : genetics, molecular biology, evolution, endocrinology, embryology, and pathology of sex determination and differentiation
JF - Sexual development : genetics, molecular biology, evolution, endocrinology, embryology, and pathology of sex determination and differentiation
IS - 6
ER -