Literature DB >> 27978798

Combination Platinum-based and DNA Damage Response-targeting Cancer Therapy: Evolution and Future Directions.

Spyridon P Basourakos1, Likun Li1, Ana M Aparicio1, Paul G Corn1, Jeri Kim1, Timothy C Thompson2.   

Abstract

Maintenance of genomic stability is a critical determinant of cell survival and is necessary for growth and progression of malignant cells. Interstrand crosslinking (ICL) agents, including platinum-based agents, are first-line chemotherapy treatment for many solid human cancers. In malignant cells, ICL triggers the DNA damage response (DDR). When the damage burden is high and lesions cannot be repaired, malignant cells are unable to divide and ultimately undergo cell death either through mitotic catastrophe or apoptosis. The activities of ICL agents, in particular platinum-based therapies, establish a "molecular landscape," i.e., a pattern of DNA damage that can potentially be further exploited therapeutically with DDR-targeting agents. If the molecular landscape created by platinum-based agents could be better defined at the molecular level, a systematic, mechanistic rationale(s) could be developed for the use of DDR-targeting therapies in combination/maintenance protocols for specific, clinically advanced malignancies. New therapeutic drugs such as poly(ADP-ribose) polymerase (PARP) inhibitors are examples of DDR-targeting therapies that could potentially increase the DNA damage and replication stress imposed by platinum-based agents in tumor cells and provide therapeutic benefit for patients with advanced malignancies. Recent studies have shown that the use of PARP inhibitors together with platinum-based agents is a promising therapy strategy for ovarian cancer patients with "BRCAness", i.e., a phenotypic characteristic of tumors that not only can involve loss-of-function mutations in either BRCA1 or BRCA2, but also encompasses the molecular features of BRCA-mutant tumors. On the basis of these promising results, additional mechanism-based studies focused on the use of various DDR-targeting therapies in combination with platinum-based agents should be considered. This review discusses, in general, (1) ICL agents, primarily platinum-based agents, that establish a molecular landscape that can be further exploited therapeutically; (2) multiple points of potential intervention after ICL agent-induced crosslinking that further predispose to cell death and can be incorporated into a systematic, therapeutic rationale for combination/ maintenance therapy using DDR-targeting agents; and (3) available agents that can be considered for use in combination/maintenance clinical protocols with platinum-based agents for patients with advanced malignancies. Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.

Entities:  

Keywords:  ATR; Chk-1/Chk-2; DDR targeting agents; PARP; Platinum-based agents; WEE-1

Mesh:

Substances:

Year:  2017        PMID: 27978798      PMCID: PMC5471128          DOI: 10.2174/0929867323666161214114948

Source DB:  PubMed          Journal:  Curr Med Chem        ISSN: 0929-8673            Impact factor:   4.530


  112 in total

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Review 5.  Poly(ADP-ribosyl)ation reactions in the regulation of nuclear functions.

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Review 6.  PARP inhibition: PARP1 and beyond.

Authors:  Michèle Rouleau; Anand Patel; Michael J Hendzel; Scott H Kaufmann; Guy G Poirier
Journal:  Nat Rev Cancer       Date:  2010-03-04       Impact factor: 60.716

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10.  Identification of cisplatin-binding proteins using agarose conjugates of platinum compounds.

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Journal:  PLoS One       Date:  2013-06-03       Impact factor: 3.240

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2.  Loss of the tumor suppressor BIN1 enables ATM Ser/Thr kinase activation by the nuclear protein E2F1 and renders cancer cells resistant to cisplatin.

Authors:  Watson P Folk; Alpana Kumari; Tetsushi Iwasaki; Slovénie Pyndiah; Joanna C Johnson; Erica K Cassimere; Amy L Abdulovic-Cui; Daitoku Sakamuro
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3.  Nuclear translocation of Gasdermin D sensitizes colorectal cancer to chemotherapy in a pyroptosis-independent manner.

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4.  Perspectives on the role of breast cancer susceptibility gene in breast cancer.

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Review 5.  Therapeutic implications of germline vulnerabilities in DNA repair for precision oncology.

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6.  Enhancement of cisplatin cytotoxicity by Retigeric acid B involves blocking DNA repair and activating DR5 in prostate cancer cells.

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Review 7.  Role of BRCA Mutations in the Modulation of Response to Platinum Therapy.

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Journal:  Front Oncol       Date:  2018-02-05       Impact factor: 6.244

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9.  Overexpression of BLM promotes DNA damage and increased sensitivity to platinum salts in triple-negative breast and serous ovarian cancers.

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Review 10.  A review of nutrition and dietary interventions in oncology.

Authors:  Ashley Gray; Brian N Dang; Theodore B Moore; Roger Clemens; Peter Pressman
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