| Literature DB >> 33597549 |
Chuna Kim1,2, Sanghyun Sung1, Jong-Seo Kim1,3, Hyunji Lee1, Yoonseok Jung3, Sanghee Shin1,3, Eunkyeong Kim1, Jenny J Seo1,3, Jun Kim1, Daeun Kim4,5, Hiroyuki Niida6, V Narry Kim1,3, Daechan Park7,8, Junho Lee9.
Abstract
Telomeres are part of a highly refined system for maintaining the stability of linear chromosomes. Most telomeres rely on simple repetitive sequences and telomerase enzymes to protect chromosomal ends; however, in some species or telomerase-defective situations, an alternative lengthening of telomeres (ALT) mechanism is used. ALT mainly utilises recombination-based replication mechanisms and the constituents of ALT-based telomeres vary depending on models. Here we show that mouse telomeres can exploit non-telomeric, unique sequences in addition to telomeric repeats. We establish that a specific subtelomeric element, the mouse template for ALT (mTALT), is used for repairing telomeric DNA damage as well as for composing portions of telomeres in ALT-dependent mouse embryonic stem cells. Epigenomic and proteomic analyses before and after ALT activation reveal a high level of non-coding mTALT transcripts despite the heterochromatic nature of mTALT-based telomeres. After ALT activation, the increased HMGN1, a non-histone chromosomal protein, contributes to the maintenance of telomere stability by regulating telomeric transcription. These findings provide a molecular basis to study the evolution of new structures in telomeres.Entities:
Year: 2021 PMID: 33597549 DOI: 10.1038/s41467-021-21341-x
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919