@article{d516f3bc6c384a06a7ce901c599d68b2,
title = "Molecular contribution to embryonic aneuploidy and karyotypic complexity in initial cleavage divisions ofmammalian development",
abstract = "Embryonic aneuploidy is highly complex, often leading to developmental arrest, implantation failure or spontaneous miscarriage in both natural and assisted reproduction. Despite our knowledge of mitotic mis-segregation in somatic cells, the molecular pathways regulating chromosome fidelity during the error-prone cleavage-stage of mammalian embryogenesis remain largely undefined. Using bovine embryos and live-cell fluorescent imaging, we observed frequent micro-/multi-nucleation of mis-segregated chromosomes in initial mitotic divisions that underwent unilateral inheritance, re-fused with the primary nucleus or formed a chromatin bridge with neighboring cells. A correlation between a lack of syngamy, multipolar divisions and asymmetric genome partitioning was also revealed, and single-cell DNA-seq showed propagation of primarily non-reciprocal mitotic errors. Depletion of the mitotic checkpoint protein BUB1B (also known as BUBR1) resulted in similarly abnormal nuclear structures and cell divisions, as well as chaotic aneuploidy and dysregulation of the kinase-substrate network that mediates mitotic progression, all before zygotic genome activation. This demonstrates that embryonic micronuclei sustain multiple fates, provides an explanation for blastomeres with uniparental origins, and substantiates defective checkpoints and likely other maternally derived factors as major contributors to the karyotypic complexity afflicting mammalian preimplantation development.",
keywords = "Aneuploidy, BUB1B, BUBR1, Cytokinesis, Embryo, Micronuclei, Mitosis",
author = "Brooks, {Kelsey E.} and Daughtry, {Brittany L.} and Brett Davis and Yan, {Melissa Y.} and Fei, {Suzanne S.} and Selma Shepherd and Lucia Carbone and Chavez, {Shawn L.}",
note = "Funding Information: We gratefully acknowledge Dr Tom Spencer at the University of Missouri-Columbia for the Madin-Darby Bovine Kidney (MDBK) epithelial cells. Drs Crystal Chaw and Stefanie Kaech Petrie in the OHSU Advanced Light Microscopy (ALM) Core were instrumental in developing our imaging protocol, and we very much appreciate all their help and support. We also thank Drs Andrew Adey and Andrew Fields for their assistance and use of the NextSeq500 sequencer. We acknowledge the Oregon National Primate Research Center (ONPRC) Integrated Pathology Core for confocal microscopy (supported by S10RR024585) that operates under the auspices of the ONPRC NIH/OD core grant (P51OD011092). Funding Information: K.E.B. was supported by the National Institutes of Health/Eunice Kennedy Shriver National Institute of Child Health and Human Development Postdoctoral Individual National Research Service Award (5F32HD095550-01). B.L.D. was supported by a P.E.O. Scholar Award, a N. L. Tartar Research Fellowship and a T32 Reproductive Biology National Institutes of Health Training Grant (T32 HD007133). This work was supported by Oregon Health and Science University/Oregon National Primate Research Center start-up funds (to S.L.C.) and by the National Institutes of Health/Eunice Kennedy Shriver National Institute of Child Health and Human Development (R01HD086073-A1). Open Access funding provided by Oregon Health and Science University. Deposited in PMC for immediate release. Publisher Copyright: {\textcopyright} 2022. Published by The Company of Biologists Ltd.",
year = "2022",
month = apr,
doi = "10.1242/dev.198341",
language = "English (US)",
volume = "149",
journal = "Journal of Embryology and Experimental Morphology",
issn = "0950-1991",
publisher = "Company of Biologists Ltd",
number = "7",
}