4.6 Review

Understanding How Genetic Mutations Collaborate with Genomic Instability in Cancer

Journal

CELLS
Volume 10, Issue 2, Pages -

Publisher

MDPI
DOI: 10.3390/cells10020342

Keywords

aneuploidy; chromosomal instability; genome wide screens; cancer

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Funding

  1. Dutch Cancer Society [2015-RUG-7833]
  2. Chinese Scholarship Council (CSC) fellowship

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Chromosomal instability leads to cells with abnormal numbers of chromosomes, which is detrimental during development and in primary cells, but is also a hallmark of cancer cells. It is believed that premalignant cells need to overcome this instability to become tumorigenic, and some aneuploidy-tolerating pathways may be therapeutically beneficial.
Chromosomal instability is the process of mis-segregation for ongoing chromosomes, which leads to cells with an abnormal number of chromosomes, also known as an aneuploid state. Induced aneuploidy is detrimental during development and in primary cells but aneuploidy is also a hallmark of cancer cells. It is therefore believed that premalignant cells need to overcome aneuploidy-imposed stresses to become tumorigenic. Over the past decade, some aneuploidy-tolerating pathways have been identified through small-scale screens, which suggest that aneuploidy tolerance pathways can potentially be therapeutically exploited. However, to better understand the processes that lead to aneuploidy tolerance in cancer cells, large-scale and unbiased genetic screens are needed, both in euploid and aneuploid cancer models. In this review, we describe some of the currently known aneuploidy-tolerating hits, how large-scale genome-wide screens can broaden our knowledge on aneuploidy specific cancer driver genes, and how we can exploit the outcomes of these screens to improve future cancer therapy.

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