DNA double-strand break repair pathway choice - from basic biology to clinical 
exploitation

Jachimowicz, R. D.; Goergens, J.; Reinhardt, H. C.

doi:10.1080/15384101.2019.1618542

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DNA double-strand break repair pathway choice - from basic biology to clinical exploitation

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Jachimowicz, R. D.
Jachimowicz – Mechanisms of DNA Repair, Max Planck Research Groups, Max Planck Institute for Biology of Ageing, Max Planck Society;

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Goergens, J.
Jachimowicz – Mechanisms of DNA Repair, Max Planck Research Groups, Max Planck Institute for Biology of Ageing, Max Planck Society;

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https://www.ncbi.nlm.nih.gov/pubmed/31116084
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Citation

Jachimowicz, R. D., Goergens, J., & Reinhardt, H. C. (2019). DNA double-strand break repair pathway choice - from basic biology to clinical exploitation. Cell Cycle, 18(13), 1423-1434. doi:10.1080/15384101.2019.1618542.

Cite as: https://hdl.handle.net/21.11116/0000-000B-423D-7

Abstract

Mutations in genes encoding components of the DNA damage response (DDR) are among the most frequent aberrations in human tumors. Moreover, a large array of human syndromes is caused by mutations in genes involved in DDR pathways. Among others, homologous recombination repair (HR) of DNA double-strand breaks (DSB) is frequently affected by disabling mutations. While impaired HR is clearly promoting tumorigenesis, it is also associated with an actionable sensitivity against PARP inhibitors. PARP inhibitors have recently received FDA approval for the treatment of breast- and ovarian cancer. However, as with all molecularly targeted agents, acquired resistance limits its use. Both pharmaco-genomic approaches and the study of human genome instability syndromes have led to a profound understanding of PARP inhibitor resistance. These experiments have revealed new insights into the molecular mechanisms that drive mammalian DSB repair. Here, we review recent discoveries in the field and provide a clinical perspective.