Karolinska Institutet
Browse

High density of REC8 constrains sister chromatid axes and prevents illegitimate synaptonemal complex formation.

Download (42.18 MB)
journal contribution
posted on 2024-10-22, 12:39 authored by Ana Agostinho, Otto Manneberg, Robin van Schendel, Abrahan Hernández-Hernández, Anna KouznetsovaAnna Kouznetsova, Hans Blom, Hjalmar BrismarHjalmar Brismar, Christer HöögChrister Höög
During meiosis, cohesin complexes mediate sister chromatid cohesion (SCC), synaptonemal complex (SC) assembly and synapsis. Here, using super-resolution microscopy, we imaged sister chromatid axes in mouse meiocytes that have normal or reduced levels of cohesin complexes, assessing the relationship between localization of cohesin complexes, SCC and SC formation. We show that REC8 foci are separated from each other by a distance smaller than 15% of the total chromosome axis length in wild-type meiocytes. Reduced levels of cohesin complexes result in a local separation of sister chromatid axial elements (LSAEs), as well as illegitimate SC formation at these sites. REC8 but not RAD21 or RAD21L cohesin complexes flank sites of LSAEs, whereas RAD21 and RAD21L appear predominantly along the separated sister-chromatid axes. Based on these observations and a quantitative distribution analysis of REC8 along sister chromatid axes, we propose that the high density of randomly distributed REC8 cohesin complexes promotes SCC and prevents illegitimate SC formation.

History

File version

  • Accepted manuscript

Publication status

Published

Sub type

Article

Journal

EMBO Rep

ISSN

1469-221X

eISSN

1469-3178

Volume

17

Issue

6

Pagination

901-913

Language

  • eng

Original self archiving date

2016-12-07

Usage metrics

    Articles

    Exports

    RefWorks
    BibTeX
    Ref. manager
    Endnote
    DataCite
    NLM
    DC