TY - JOUR
T1 - When genotype is not predictive of phenotype
T2 - Implications for genetic counseling based on 21,594 chromosomal microarray analysis examinations
AU - Maya, Idit
AU - Sharony, Reuven
AU - Yacobson, Shiri
AU - Kahana, Sarit
AU - Yeshaya, Josepha
AU - Tenne, Tamar
AU - Agmon-Fishman, Ifaat
AU - Cohen-Vig, Lital
AU - Goldberg, Yael
AU - Berger, Racheli
AU - Basel-Salmon, Lina
AU - Shohat, Mordechai
N1 - Publisher Copyright:
© American College of Medical Genetics and Genomics.
PY - 2018/1/1
Y1 - 2018/1/1
N2 - PurposeTo compare the frequency of copy-number variants (CNVs) of variable penetrance in low-risk and high-risk prenatal samples and postnatal samples.MethodsTwo cohorts were categorized according to chromosomal microarray analysis (CMA) indication: group I, low-risk prenatal - women with uneventful pregnancy (control group); group II, high-risk prenatal - women whose fetuses had congenital malformations; and group III, postnatal - individuals with unexplained developmental delay/intellectual disability, autism spectrum disorders, or multiple congenital anomalies. CNVs were categorized based on clinical penetrance: (i) high (>40%), (ii) moderate (10-40%), and (iii) low (<10%).ResultsFrom 2013 to 2016, 21,594 CMAs were performed. The frequency of high-penetrance CNVs was 0.1% (21/15,215) in group I, 0.9% (26/2,791) in group II, and 2.6% (92/3,588) in group III. Moderate-penetrance CNV frequency was 0.3% (47/15,215), 0.6% (19/2,791), and 1.2% (46/3,588), respectively. These differences were statistically significant. The frequency of low-penetrance CNVs was not significantly different among groups: 0.6% (85/15,215), 0.9% (25/2,791), and 1.0% (35/3,588), respectively.ConclusionHigh-penetrance CNVs might be a major factor in the overall heritability of developmental, intellectual, and structural anomalies. Low-penetrance CNV alone does not seem to contribute to these anomalies. These data may assist pre- and posttest CMA counseling.
AB - PurposeTo compare the frequency of copy-number variants (CNVs) of variable penetrance in low-risk and high-risk prenatal samples and postnatal samples.MethodsTwo cohorts were categorized according to chromosomal microarray analysis (CMA) indication: group I, low-risk prenatal - women with uneventful pregnancy (control group); group II, high-risk prenatal - women whose fetuses had congenital malformations; and group III, postnatal - individuals with unexplained developmental delay/intellectual disability, autism spectrum disorders, or multiple congenital anomalies. CNVs were categorized based on clinical penetrance: (i) high (>40%), (ii) moderate (10-40%), and (iii) low (<10%).ResultsFrom 2013 to 2016, 21,594 CMAs were performed. The frequency of high-penetrance CNVs was 0.1% (21/15,215) in group I, 0.9% (26/2,791) in group II, and 2.6% (92/3,588) in group III. Moderate-penetrance CNV frequency was 0.3% (47/15,215), 0.6% (19/2,791), and 1.2% (46/3,588), respectively. These differences were statistically significant. The frequency of low-penetrance CNVs was not significantly different among groups: 0.6% (85/15,215), 0.9% (25/2,791), and 1.0% (35/3,588), respectively.ConclusionHigh-penetrance CNVs might be a major factor in the overall heritability of developmental, intellectual, and structural anomalies. Low-penetrance CNV alone does not seem to contribute to these anomalies. These data may assist pre- and posttest CMA counseling.
UR - http://www.scopus.com/inward/record.url?scp=85040445363&partnerID=8YFLogxK
U2 - 10.1038/gim.2017.89
DO - 10.1038/gim.2017.89
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AN - SCOPUS:85040445363
SN - 1098-3600
VL - 20
SP - 128
EP - 131
JO - Genetics in Medicine
JF - Genetics in Medicine
IS - 1
ER -