Chromosome mis-segregation and cytokinesis failure in trisomic human cells

نویسندگان

  • Joshua M Nicholson
  • Joana C Macedo
  • Aaron J Mattingly
  • Darawalee Wangsa
  • Jordi Camps
  • Vera Lima
  • Ana M Gomes
  • Sofia Dória
  • Thomas Ried
  • Elsa Logarinho
  • Daniela Cimini
چکیده

Cancer cells display aneuploid karyotypes and typically mis-segregate chromosomes at high rates, a phenotype referred to as chromosomal instability (CIN). To test the effects of aneuploidy on chromosome segregation and other mitotic phenotypes we used the colorectal cancer cell line DLD1 (2n = 46) and two variants with trisomy 7 or 13 (DLD1+7 and DLD1+13), as well as euploid and trisomy 13 amniocytes (AF and AF+13). We found that trisomic cells displayed higher rates of chromosome mis-segregation compared to their euploid counterparts. Furthermore, cells with trisomy 13 displayed a distinctive cytokinesis failure phenotype. We showed that up-regulation of SPG20 expression, brought about by trisomy 13 in DLD1+13 and AF+13 cells, is sufficient for the cytokinesis failure phenotype. Overall, our study shows that aneuploidy can induce chromosome mis-segregation. Moreover, we identified a trisomy 13-specific mitotic phenotype that is driven by up-regulation of a gene encoded on the aneuploid chromosome.

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عنوان ژورنال:

دوره 4  شماره 

صفحات  -

تاریخ انتشار 2015