volume 43 issue 2

Prenatal phenotype of 47, XXY (Klinefelter syndrome)

Kate Swanson 1, 2
Juliet C. Bishop 3, 4
Huda Al-Kouatly 5
Mona Makhamreh 5
Thomas Felton 6
Teresa N. Sparks 1
A. C. Jelin 3, 4
Publication typeJournal Article
Publication date2021-12-07
scimago Q1
wos Q1
SJR0.932
CiteScore5.1
Impact factor2.7
ISSN01973851, 10970223
PubMed ID:  34874073
Genetics (clinical)
Obstetrics and Gynecology
Abstract
There is a paucity of knowledge regarding the prenatal presentation of Klinefelter syndrome, or 47, XXY. Accurate prenatal counseling is critical and in utero diagnosis is currently limited by a poor understanding of the prenatal phenotype of this condition.This is a case series of fetuses with cytogenetically confirmed 47, XXY in the prenatal period or up to age 5 years, with prenatal records available for review from four academic institutions between 2006 and 2019. Ultrasound reports were reviewed in detail to assess for increased nuchal translucency and structural abnormalities. Additionally, we reviewed results of cell-free DNA and serum analyte testing when performed to inform our understanding of the detection of fetal 47, XXY through standard genetic screening tests.Forty-one cases with confirmed cytogenetic diagnosis of 47, XXY and prenatal records available for review were identified: 37 had a prenatal diagnosis and 4 had a postnatal diagnosis. Nuchal translucency was increased ≥3.0 mm in 23.1% (6/26) of cases with a documented measurement. In 29.2% (7/24) of cases with a second trimester anatomical ultrasound available for review, a fetal abnormality was identified (3 brain anomalies, 1 cardiac abnormality, 1 echogenic bowel, and 2 limb abnormalities). Among those who had cell-free DNA and serum analytes performed, 92.6% (25/27) and 36.3% (4/11) had an abnormal result respectively.This case series expands our knowledge of the prenatal presentation of 47, XXY by identifying first and second trimester fetal sonographic abnormalities. Prenatal identification of this condition enables accurate counseling, focused prenatal management, and early postnatal interventions to ameliorate some of the known complications.
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Swanson K. et al. Prenatal phenotype of 47, XXY (Klinefelter syndrome) // Prenatal Diagnosis. 2021. Vol. 43. No. 2.
GOST all authors (up to 50) Copy
Swanson K., Bishop J., Al-Kouatly H., Makhamreh M., Felton T., Vora N. L., Sparks T. N., Jelin A. C. Prenatal phenotype of 47, XXY (Klinefelter syndrome) // Prenatal Diagnosis. 2021. Vol. 43. No. 2.
RIS |
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RIS Copy
TY - JOUR
DO - 10.1002/pd.6071
UR - https://doi.org/10.1002/pd.6071
TI - Prenatal phenotype of 47, XXY (Klinefelter syndrome)
T2 - Prenatal Diagnosis
AU - Swanson, Kate
AU - Bishop, Juliet C.
AU - Al-Kouatly, Huda
AU - Makhamreh, Mona
AU - Felton, Thomas
AU - Vora, Neeta L.
AU - Sparks, Teresa N.
AU - Jelin, A. C.
PY - 2021
DA - 2021/12/07
PB - Wiley
IS - 2
VL - 43
PMID - 34874073
SN - 0197-3851
SN - 1097-0223
ER -
BibTex
Cite this
BibTex (up to 50 authors) Copy
@article{2021_Swanson,
author = {Kate Swanson and Juliet C. Bishop and Huda Al-Kouatly and Mona Makhamreh and Thomas Felton and Neeta L. Vora and Teresa N. Sparks and A. C. Jelin},
title = {Prenatal phenotype of 47, XXY (Klinefelter syndrome)},
journal = {Prenatal Diagnosis},
year = {2021},
volume = {43},
publisher = {Wiley},
month = {dec},
url = {https://doi.org/10.1002/pd.6071},
number = {2},
doi = {10.1002/pd.6071}
}