Immunological control of cell cycle aberrations for the avoidance of oncogenesis: The case of tetraploidy

Laura Senovilla, Lorenzo Galluzzi, Maria Castedo, Guido Kroemer

    Research output: Contribution to journalArticlepeer-review

    6 Citations (Scopus)

    Abstract

    Tetraploid cells-cells that contain twice the normal amount of DNA-are more prone to neoplastic transformation than their normal, diploid counterparts since they are genomically unstable and frequently undergo asymmetric, multipolar cell divisions. Similar to many other genomic aberrations, tetraploidization is normally avoided by multiple, nonredundant cell-intrinsic mechanisms that are tied to cell cycle checkpoints. Unexpectedly, tetraploidization is also under the control of a cell-extrinsic mechanism determined by the immune system. Indeed, oncogene- or carcinogen-induced cancers developing in immunodeficient mice contain cells with a higher DNA content than similar tumors growing in immunocompetent hosts. Moreover, cancer cell lines that have been rendered tetraploid in vitro grow normally in immunodeficient mice, yet almost fail to generate tumors in immunocompetent animals. One of the mechanisms whereby the immune system recognizes tetraploid cells originates from tetraploidy causing an endoplasmic reticulum (ER) stress response that culminates in the exposure of the ER protein calreticulin on the cell surface. Hence, tetraploidy exemplifies a potentially oncogenic alteration that is repressed by a combination of cell-autonomous mechanisms and immunosurveillance. Oncogenesis and tumor progression require the simultaneous failure of both such control systems.

    Original languageEnglish
    Pages (from-to)57-61
    Number of pages5
    JournalAnnals of the New York Academy of Sciences
    Volume1284
    Issue number1
    DOIs
    Publication statusPublished - 1 Jan 2013

    Keywords

    • CT26 cells
    • Calreticulin
    • EIF2α phosphorylation
    • HMGB1
    • Nocodazole
    • P53

    Cite this