Mosaic Trisomy 12 Associated with Overgrowth Detected in Fibroblast Cell Lines

Author:

Gasparini Yanca,Montenegro Marília M.,Novo-Filho Gil M.,Ceroni José R.M.,Honjo Rachel S.,Zanardo Évelin A.,Dias Alexandre T.,Nascimento Amon M.,Costa Taís V.M.M.,Madia Fabrícia A.,Chehimi Samar N.,Damasceno Jullian G.,Kim Chong A.,Kulikowski Leslie D.

Abstract

Mosaic trisomy 12 is a rare anomaly, and only 9 cases of live births with this condition have been reported in the literature. The clinical phenotype is variable, including neuropsychomotor developmental delay, congenital heart disease, microcephaly, cutaneous spots, facial asymmetry, prominent ears, hypotonia, retinopathy, and sensorineural hearing loss. A 2-year-old female presented with neuropsychomotor developmental delay, prominent forehead, dolichocephaly, patchy skin pigmentation, and unexpected overgrowth at birth. Cytogenetic analysis of her peripheral blood showed normal results, suggesting the presence of a chromosomal alteration in other tissues. Further studies using G-banding and FISH performed on fibroblasts from both hyper- and hypopigmented regions identified a 47,XX,+12/46,XX karyotype. To the best of our knowledge, no patients with mosaic trisomy 12 associated with overgrowth have been reported to date. Congenital overgrowth and neonatal overgrowth have been frequently linked to Pallister-Killian syndrome (PKS; OMIM 601803). This case suggests the possibility of an association of genes present in the 12p region with fetal overgrowth, considering that chromosomal duplications could lead to an increase in the production of aberrant transcripts and disturbing gene dosage effects. This case highlights the importance of cytogenetic analysis in different tissues to provide relevant information to the specific genotype/phenotype correlation.

Publisher

S. Karger AG

Subject

Genetics(clinical),Genetics,Molecular Biology

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