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Publication : Chromosome structural anomalies due to aberrant spindle forces exerted at gene editing sites in meiosis.

First Author  Manil-Ségalen M Year  2018
Journal  J Cell Biol Volume  217
Issue  10 Pages  3416-3430
PubMed ID  30082296 Mgi Jnum  J:266008
Mgi Id  MGI:6201843 Doi  10.1083/jcb.201806072
Citation  Manil-Segalen M, et al. (2018) Chromosome structural anomalies due to aberrant spindle forces exerted at gene editing sites in meiosis. J Cell Biol 217(10):3416-3430
abstractText  Mouse female meiotic spindles assemble from acentriolar microtubule-organizing centers (aMTOCs) that fragment into discrete foci. These are further sorted and clustered to form spindle poles, thus providing balanced forces for faithful chromosome segregation. To assess the impact of aMTOC biogenesis on spindle assembly, we genetically induced their precocious fragmentation in mouse oocytes using conditional overexpression of Plk4, a master microtubule-organizing center regulator. Excessive microtubule nucleation from these fragmented aMTOCs accelerated spindle assembly dynamics. Prematurely formed spindles promoted the breakage of three different fragilized bivalents, generated by the presence of recombined Lox P sites. Reducing the density of microtubules significantly diminished the extent of chromosome breakage. Thus, improper spindle forces can lead to widely described yet unexplained chromosomal structural anomalies with disruptive consequences on the ability of the gamete to transmit an uncorrupted genome.
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