Case report

Chromosome r(10)(p15.3q26.12) in a newborn child: case report

Cecilia Gunnarsson¹ , Barbara Graffmann² and Jon Jonasson¹

¹  Division of Pathology and Clinical Genetics, Department of Clinical and Experimental Medicine, Linköping University, University Hospital, S-581 85 Linköping, Sweden

²  Division of Pediatrics, Department of Clinical and Experimental Medicine, Linköping University, University Hospital, S-581 85 Linköping, Sweden

author email corresponding author email

Molecular Cytogenetics 2009, 2:25doi:10.1186/1755-8166-2-25

Published:	7 December 2009

Abstract

Background

Ring chromosome 10 is a rare cytogenetic finding. Of the less than 10 reported cases we have found in the literature, none was characterized using high-resolution microarray analysis. Ring chromosomes are frequently unstable due to sister chromatid exchanges and mitotic failures. When mosaicism is present, the interpretation of genotype-phenotype correlations becomes extremely difficult.

Results

We report on a newborn girl with growth retardation, microcephaly, congenital heart defects, dysmorphic features and psychomotor retardation. Karyotyping revealed a non-mosaic apparently stable ring chromosome 10 replacing one of the normal homologues in all analyzed metaphases. High-resolution oligonucleotide microarray analysis showed a de novo approximately 12.5 Mb terminal deletion 10q26.12 -> qter and a corresponding 285 kb terminal deletion of 10pter -> p15.3.

Conclusion

This case demonstrates that an increased nuchal translucency thickness detected by early ultrasonography should preferably lead to not only QF-PCR for the diagnosis of Down syndrome but also karyotyping. In the future, microarray analysis, which needs further evaluation, might become the method of choice. The clinical phenotype of our patient was in agreement with that of patients with a terminal 10q deletion. For the purpose of genotype-phenotype analysis, there seems to be no need for a "ring syndrome" concept.