AI Article Synopsis

  • The study aimed to assess the effectiveness of array-based comparative genomic hybridization (a-CGH) for detecting chromosomal abnormalities in fetuses of older pregnant women.
  • Over 3,600 amniotic fluid samples were analyzed, revealing a 2.04% rate of chromosomal aberrations, primarily consisting of aneuploidies and pathogenic copy number variations (CNVs).
  • The results indicated that a-CGH is superior to traditional methods in identifying both aneuploidies and pathogenic CNVs, with the detection of aneuploidies increasing with maternal age, but no similar correlation found for pathogenic CNVs.

Article Abstract

Objective: To evaluate the clinical application of array-based comparative genomic hybridization (a-CGH) in the prenatal diagnosis of fetal chromosomal aberrations in gravidas with advanced maternal age (AMA).

Methods: A total of 3 677 amniotic fluid samples from pregnant women who underwent amniocentesis for prenatal diagnosis solely due to AMA were selected. Array-CGH was performed on the Agilent CGX (8X60K) platform and the data were analyzed by the Genoglyphix software.

Results: The overall detection rate of chromosomal aberration was 2.04% (75/3677), with 53.33% (40/75) being aneuploidies, including 22 cases of trisomy-21, 5 cases of trisomy-18, 8 cases with XXY, 3 cases of XYY and 2 cases of mosaic monosomy X, 32.00% (24/75) being pathogenic copy number variations (pCNVs), including 19 cases of microdeletion and 5 cases of microduplication, with the fragment size ranging from 323 kb to 26 780 kb, and 14.67% (11/75) being likely pathogenic CNVs (lpCNVs), including 7 cases of microdeletion and 7 cases of microduplication, with the fragment size ranging from 358 kb to 16 873 kb. Besides, the detection rate of CNVs of unknown clinical significance (VUS) was 0.84% (31/3 677). The detection rate of aneuploidies increased significantly with increased maternal age ( <0.05). However, there were no significant differences in the detection rate of p/lpCNVs among different maternal age groups ( >0.05).

Conclusion: Our findings suggest that, compared with traditional karyotype analysis, a-CGH not only detects aneuploidies, but also detect pathogenic CNVs, including microdeletion/microduplication syndromes. The detection rate of fetal aneuploidies was closely correlated to maternal age. However, no correlation was found between the detection rate of p/lpCNVs and maternal age.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10408947PMC
http://dx.doi.org/10.12182/20210160601DOI Listing

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