| Literature DB >> 26936114 |
Heleen Masset1, Matthew S Hestand1, Hilde Van Esch1, Pascale Kleinfinger2, Julie Plaisancié3, Alexandra Afenjar4,5, Romain Molignier6, Caroline Schluth-Bolard7,8, Damien Sanlaville7,8, Joris R Vermeesch1.
Abstract
Chromoanagenesis is the process by which a single catastrophic event creates complex rearrangements confined to a single or a few chromosomes. It is usually characterized by the presence of multiple deletions and/or duplications, as well as by copy neutral rearrangements. In contrast, an array CGH screen of patients with developmental anomalies revealed three patients in which a single chromosome carries from 8 to 11 large copy number gains confined to a single chromosome or chromosomal arm, but the absence of deletions. Subsequent fluorescence in situ hybiridization and massive parallel sequencing revealed the duplicons to be clustered together in distinct locations across the altered chromosomes. Breakpoint junction sequences showed both microhomology and non-templated insertions of up to 40 bp. Hence, these patients each demonstrate a single altered chromosome of clustered insertional duplications, no deletions, and breakpoint junction sequences showing microhomology and/or non-templated insertions. These observations are difficult to reconcile with current mechanistic descriptions of chromothripsis and chromoanasynthesis. Therefore, we hypothesize those rearrangements to be of a mechanistically different origin. In addition, we suggest that large untemplated insertional sequences observed at breakpoints are driven by a non-canonical non-homologous end joining mechanism.Entities:
Keywords: chromoanagenesis; chromoanasynthesis; chromothripsis; polymerase theta
Mesh:
Year: 2016 PMID: 26936114 DOI: 10.1002/humu.22984
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878