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Advances in synthetic lethality for cancer therapy: cellular mechanism and clinical translation.


ABSTRACT: Synthetic lethality is a lethal phenomenon in which the occurrence of a single genetic event is tolerable for cell survival, whereas the co-occurrence of multiple genetic events results in cell death. The main obstacle for synthetic lethality lies in the tumor biology heterogeneity and complexity, the inadequate understanding of synthetic lethal interactions, drug resistance, and the challenges regarding screening and clinical translation. Recently, DNA damage response inhibitors are being tested in various trials with promising results. This review will describe the current challenges, development, and opportunities for synthetic lethality in cancer therapy. The characterization of potential synthetic lethal interactions and novel technologies to develop a more effective targeted drug for cancer patients will be explored. Furthermore, this review will discuss the clinical development and drug resistance mechanisms of synthetic lethality in cancer therapy. The ultimate goal of this review is to guide clinicians at selecting patients that will receive the maximum benefits of DNA damage response inhibitors for cancer therapy.

SUBMITTER: Topatana W 

PROVIDER: S-EPMC7470446 | biostudies-literature | 2020 Sep

REPOSITORIES: biostudies-literature

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Advances in synthetic lethality for cancer therapy: cellular mechanism and clinical translation.

Topatana Win W   Juengpanich Sarun S   Li Shijie S   Cao Jiasheng J   Hu Jiahao J   Lee Jiyoung J   Suliyanto Kenneth K   Ma Diana D   Zhang Bin B   Chen Mingyu M   Cai Xiujun X  

Journal of hematology & oncology 20200903 1


Synthetic lethality is a lethal phenomenon in which the occurrence of a single genetic event is tolerable for cell survival, whereas the co-occurrence of multiple genetic events results in cell death. The main obstacle for synthetic lethality lies in the tumor biology heterogeneity and complexity, the inadequate understanding of synthetic lethal interactions, drug resistance, and the challenges regarding screening and clinical translation. Recently, DNA damage response inhibitors are being teste  ...[more]

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