Chromosome instability induced by Mps1 and p53 mutation generates aggressive lymphomas exhibiting aneuploidy-induced stress

Floris Foijer*, Stephanie Z. Xie, Judith E. Simon, Petra L. Bakker, Nathalie Conte, Stephanie H. Davis, Eva Kregel, Jos Jonkers, Allan Bradley, Peter K. Sorger

*Corresponding author voor dit werk

    Onderzoeksoutput: ArticleAcademicpeer review

    78 Citaten (Scopus)

    Samenvatting

    Aneuploidy is a hallmark of human solid cancers that arises from errors in mitosis and results in gain and loss of oncogenes and tumor suppressors. Aneuploidy poses a growth disadvantage for cells grown in vitro, suggesting that cancer cells adapt to this burden. To understand better the consequences of aneuploidy in a rapidly proliferating adult tissue, we engineered a mouse in which chromosome instability was selectively induced in T cells. A flanked by Lox mutation was introduced into the monopolar spindle 1 ( Mps1) spindle-assembly checkpoint gene so that Cre- mediated recombination would create a truncated protein ( Mps1(DK)) that retained the kinase domain but lacked the kinetochore-binding domain and therebyweakened the checkpoint. In a sensitized p53(+/-) background we observed that Mps1(DK/DK) mice suffered from rapid-onset acute lymphoblastic lymphoma. The tumors were highly aneuploid and exhibited a metabolic burden similar to that previously characterized in aneuploid yeast and cultured cells. The tumors nonetheless grew rapidly and were lethal within 3-4 mo after birth.

    Originele taal-2English
    Pagina's (van-tot)13427-13432
    Aantal pagina's6
    TijdschriftProceedings of the National Academy of Sciences of the United States of America
    Volume111
    Nummer van het tijdschrift37
    DOI's
    StatusPublished - 16-sep.-2014

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