Literature DB >> 28650219

Interrogating cell division errors using random and chromosome-specific missegregation approaches.

Peter Ly1, Don W Cleveland1.   

Abstract

Accurate segregation of the duplicated genome in mitosis is essential for maintaining genetic stability. Errors in this process can cause numerical and/or structural chromosome abnormalities - hallmark genomic features commonly associated with both tumorigenesis and developmental disorders. A cell-based approach was recently developed permitting inducible missegregation of the human Y chromosome by selectively disrupting kinetochore assembly onto the Y centromere. Although this strategy initially requires several steps of genetic manipulation, it is easy to use, highly efficient and specific for the Y without affecting the autosomes or the X, and does not require cell cycle synchronization or mitotic perturbation. Here we describe currently available tools for studying chromosome segregation errors, aneuploidy, and micronuclei, as well as discuss how the Y-specific missegregation system has been used to elucidate how chromosomal micronucleation can trigger a class of extensive rearrangements termed chromothripsis. The combinatorial use of these different tools will allow unresolved aspects of cell division defects and chromosomal instability to be experimentally explored.

Entities:  

Keywords:  aneuploidy; centromere; chromosome segregation; chromothripsis; micronuclei; mitosis

Mesh:

Substances:

Year:  2017        PMID: 28650219      PMCID: PMC5531625          DOI: 10.1080/15384101.2017.1325047

Source DB:  PubMed          Journal:  Cell Cycle        ISSN: 1551-4005            Impact factor:   4.534


  56 in total

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Review 2.  Rebuilding Chromosomes After Catastrophe: Emerging Mechanisms of Chromothripsis.

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6.  Chromosome segregation errors generate a diverse spectrum of simple and complex genomic rearrangements.

Authors:  Peter Ly; Simon F Brunner; Ofer Shoshani; Dong Hyun Kim; Weijie Lan; Tatyana Pyntikova; Adrienne M Flanagan; Sam Behjati; David C Page; Peter J Campbell; Don W Cleveland
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  6 in total

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