AI Article Synopsis
- Chromosomal trisomy syndrome can cause various issues, including intellectual disabilities, and partial trisomy of distal 17q is a rare variant with similar problems like growth deficits and facial differences.
- This study describes three patients from two families with terminal trisomy 17q, including a child with a mosaic duplication on chromosome 17 and dizygotic twins with both a deletion on chromosome 15 and a duplication on chromosome 17.
- The research highlights the genetic mechanisms of these abnormalities and offers valuable insights for diagnosing partial trisomy 17q, aiding in understanding genotype-phenotype links for better genetic counseling.
Article Abstract
Chromosomal trisomy syndrome is associated with diverse clinical phenotypes, including intellectual disability. Partial trisomy of the distal 17q is a rare anomaly with similar clinical features, including psychomotor and growth deficits, facial dysmorphism, and microcephaly. Here, we describe three patients from two unrelated families with terminal trisomy 17q. We performed G-banding karyotype and chromosomal microarray analyses. The child in Family 1 had a 31.3 Mb mosaic duplication on chromosome 17. Family 2 comprised dizygotic twins with a 263 kb deletion on chromosome 15 and a 9.2 Mb duplication on chromosome 17; however, normal karyotyping results were obtained for both parents. We also analyzed the genetic mechanisms underlying the occurrence of these chromosomal aberrations and summarized the literature describing known genotype-phenotype correlations. Given the rarity of partial trisomy of terminal 17q, these cases will provide new insights into the diagnosis of this condition and genotype-phenotype correlations, which can aid in the detection of such conditions and genetic counseling.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11605363 | PMC |
| http://dx.doi.org/10.1002/ccr3.9611 | DOI Listing |
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