| Literature DB >> 35143306 |
Katerina Menelaou1,2, Julia Uraji1,2, Chun So1, Katarina Harasimov1, Anna M Steyer3, K Bianka Seres1,2, Jonas Bucevičius4, Gražvydas Lukinavičius4, Wiebke Möbius3,5, Claus Sibold6, Andreas Tandler-Schneider6, Heike Eckel7, Rüdiger Moltrecht7, Martyn Blayney2, Kay Elder2, Melina Schuh1,5.
Abstract
Human oocytes are prone to assembling meiotic spindles with unstable poles, which can favor aneuploidy in human eggs. The underlying causes of spindle instability are unknown. We found that NUMA (nuclear mitotic apparatus protein)-mediated clustering of microtubule minus ends focused the spindle poles in human, bovine, and porcine oocytes and in mouse oocytes depleted of acentriolar microtubule-organizing centers (aMTOCs). However, unlike human oocytes, bovine, porcine, and aMTOC-free mouse oocytes have stable spindles. We identified the molecular motor KIFC1 (kinesin superfamily protein C1) as a spindle-stabilizing protein that is deficient in human oocytes. Depletion of KIFC1 recapitulated spindle instability in bovine and aMTOC-free mouse oocytes, and the introduction of exogenous KIFC1 rescued spindle instability in human oocytes. Thus, the deficiency of KIFC1 contributes to spindle instability in human oocytes.Entities:
Mesh:
Substances:
Year: 2022 PMID: 35143306 DOI: 10.1126/science.abj3944
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728