Abstract

BackgroundRing chromosome 15 is a rare genetic entity. Only a few cases have been reported with characterization using molecular techniques. The clinical presentation is quite variable, as a result of differences in the breakpoints, haploinsufficiency of genes involved in deleted segment/s, level of mosaicism and ring instability resulting in a variability of rearrangement of genetic material.Case presentationThe proband, a 2 months old boy, presented with small head size and facial dysmorphism. On examination microcephaly, triangular face, small anterior frontanelle, micrognathia, hypotonia, unilateral simian crease, hypertelorism, umbilical hernia, micropenis with mild phimosis were noted. Karyotype revealed 46,XY,r(15)(p11.2q26). Array-comparative genomic hybridization (aCGH) and targeted gene sequencing for microcephaly was carried out for genotype phenotype correlation. Array-CGH detected a 2.8 Mb terminal deletion at 15q26.3 along with a 496 kb interstitial micro-duplication, encompassing the IGF1R gene, in the affected genomic region, which was otherwise missed on conventional karyotype.ConclusionThe present study highlights the importance of aCGH in not only delineating specific phenotypes through accurate genotypic correlation but also in detection and evaluation of ring chromosome with unexpected complex rearrangements.

Highlights

  • Ring chromosome 15 is a rare genetic entity

  • The present study highlights the importance of Array-comparative genomic hybridization (aCGH) in delineating specific phenotypes through accurate genotypic correlation and in detection and evaluation of ring chromosome with unexpected complex rearrangements

  • Ring chromosome 15 is associated with a rare disorder that was first described by Jacobsen in 1966 [1]

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Summary

Conclusion

The present study highlights the importance of aCGH in delineating specific phenotypes through accurate genotypic correlation and in detection and evaluation of ring chromosome with unexpected complex rearrangements.

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