4.2 Article

New euchromatic variant dup(11)(p15.3p15.1) transmitted through two generations defined by low coverage whole genome sequencing

Journal

AMERICAN JOURNAL OF MEDICAL GENETICS PART A
Volume 185, Issue 10, Pages 3053-3056

Publisher

WILEY
DOI: 10.1002/ajmg.a.62357

Keywords

chromosomal insertion; directly transmitted unbalanced chromosome abnormalities; low‐ coverage whole genome sequencing

Funding

  1. Projekt DEAL

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This report discusses a 14-year-old boy, his father, and paternal uncle, all carriers of a duplication of a chromosomal region. The duplication was transmitted by the grandmother and involved more than 40 genes without apparent clinical effects through two generations. Whole genome sequencing was performed on the boy's father to determine the molecular basis of this structural variant.
We report on a 14-year old boy, his father, and his paternal uncle, all three carriers of a duplication of chromosomal region 11p15.3-p15.1. The aberration was transmitted by the grandmother, who is carrier of a balanced insertion 46,XX,ins(14;11)(q32.1;p15.3p15.1). In order to determine the precise molecular basis of this structural variant, we performed low-coverage whole genome sequencing on the boy's father. This approach allowed precise determination of the genomic breakpoints and revealed a duplication of 6.9 Mb, centromeric to the Beckwith-Wiedemann/Silver-Russell syndrome critical region in 11p15.5, that inserted in inverse orientation into 14q32.12 (according to HGVS nomenclature: NC_000014.8:g.92871000_92871001ins[NC_000011.9:g.12250642_19165928inv;T]). To our knowledge, this is the first report of a duplication of 11p15.3-p15.1 involving more than 40 genes and transmitted through two generations without apparent clinical effects.

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