Targeting BRCA1‐BER deficient breast cancer by ATM or DNA‐PKcs blockade either alone or in combination with cisplatin for personalized therapy

Albarakati, Nada; Abdel-Fatah, Tarek M.A.; Doherty, Rachel; Russell, Roslin; Agarwal, Devika; Moseley, Paul M.; Perry, Christina; Arora, Arvind; Alsubhi, Nouf; Seedhouse, Claire; Rakha, Emad A.; Green, Andrew; Ball, Graham; Chan, Sy; Caldas, Carlos; Ellis, Ian O.; Madhusudan, Srinivasan

doi:10.1016/j.molonc.2014.08.001

Cited by 68 publications

(52 citation statements)

References 49 publications

(67 reference statements)

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“…It has been suggested that BRCA1-BER-deficient cells may show improved sensitivity to treatment when cisplatin is concomitantly administered with ATM and DNA-PKcs inhibitors. These types of drugs/inhibitors combination treatment options will provide better options for personalized therapy 15,62. In preliminary findings, a new class of drugs, an imidazopyridine derivative, targeting the DNA damage response pathway was administered in combination with Doxorubicin to assess cytotoxicity in breast carcinoma.…”

Section: Small Molecule Inhibition and Non-homologous End Joiningmentioning

confidence: 99%

Aberrant DNA Double-strand Break Repair Threads in Breast Carcinoma: Orchestrating Genomic Insult Survival

2016

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Breast carcinoma is a heterogeneous disease that has exhibited rapid resistance to treatment in the last decade. Depending genotype and phenotype of breast cancer, there are discernible differences in DNA repair protein responses including DNA double strand break repair. It is a fact that different molecular sub-types of breast carcinoma activate these dedicated protein pathways in a distinct manner. The DNA double-strand damage repair machinery is manipulated by breast carcinoma to selectively repair the damage or insults inflicted by the genotoxic effects of chemotherapy or radiation therapy. The two DNA double-strand break repair pathways employed by breast carcinoma are homologous recombination and non-homologous end joining. In recent decades, therapeutic interventions targeting one or more factors involved in repairing DNA double-strand breaks inflicted by chemo/radiation therapy have been widely studied. Herein, this review paper summarizes the recent evidence and ongoing clinical trials citing potential therapeutic combinatorial interventions targeting DNA double-strand break repair pathways in breast carcinoma.

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Section: Small Molecule Inhibition and Non-homologous End Joiningmentioning

confidence: 99%

Aberrant DNA Double-strand Break Repair Threads in Breast Carcinoma: Orchestrating Genomic Insult Survival

2016

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“…Patient demographics are summarized in Supplementary Table S3. This is a well-characterized series of patients with long-term follow-up that have been investigated in a wide range of biomarker studies (12)(13)(14)(15)(16)(17)(18)(19)(20). All patients were treated in a uniform way in a single institution with standard surgery (mastectomy or wide local excision) with radiotherapy.…”

Section: Blm Protein Expression In Breast Cancermentioning

confidence: 99%

“…The TMAs were immunohistochemically profiled for BLM and other biologic antibodies (Supplementary Table S4) as previously described (12)(13)(14)(15)(16)(17)(18)(19)(20). Immunohistochemical (IHC) staining was performed using the Thermo Scientific Shandon Sequenza chamber system (REF: 72110017), in combination with the Novolink Max Polymer Detection System (RE7280-K: 1,250 tests), and the Leica Bond Primary Antibody Diluent (AR9352), each used according to the manufacturer's instructions (Leica Microsystems).…”

Section: Tissue Microarrays and Immunohistochemistrymentioning

confidence: 99%

Transcriptomic and Protein Expression Analysis Reveals Clinicopathological Significance of Bloom Syndrome Helicase (BLM) in Breast Cancer

Arora

Abdel-Fatah

Agarwal

et al. 2015

Molecular Cancer Therapeutics

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Bloom syndrome helicase (BLM) has key roles in homologous recombination repair, telomere maintenance, and DNA replication. Germ-line mutations in the BLM gene causes Bloom syndrome, a rare disorder characterized by premature aging and predisposition to multiple cancers, including breast cancer. The clinicopathologic significance of BLM in sporadic breast cancers is unknown. We investigated BLM mRNA expression in the Molecular Taxonomy of Breast Cancer International Consortium cohort (n ¼ 1,950) and validated in an external dataset of 2,413 tumors. BLM protein level was evaluated in the Nottingham Tenovus series comprising 1,650 breast tumors. BLM mRNA overexpression was significantly associated with high histologic grade, larger tumor size, estrogen receptor-negative (ER À ), progesterone receptor-negative (PR À ), and triple-negative phenotypes (ps < 0.0001). BLM mRNA overexpression was also linked to aggressive molecular phenotypes, including PAM50.Her2 (P < 0.0001), PAM50. Basal (P < 0.0001), and PAM50.LumB (P < 0.0001) and Genufu subtype (ER þ /Her2 À /high proliferation; P < 0.0001). PAM50. LumA tumors and Genufu subtype (ER þ /Her2 À /low proliferation) were more likely to express low levels of BLM mRNA (ps < 0.0001). Integrative molecular clusters (intClust) intClust.1 (P < 0.0001), intClust.5 (P < 0.0001), intClust.9 (P < 0.0001), and intClust.10 (P < 0.0001) were also more likely in tumors with high BLM mRNA expression. BLM mRNA overexpression was associated with poor breast cancer-specific survival (BCSS; ps < 0.000001). At the protein level, altered subcellular localization with high cytoplasmic BLM and low nuclear BLM was linked to aggressive phenotypes. In multivariate analysis, BLM mRNA and BLM protein levels independently influenced BCSS. This is the first and the largest study to provide evidence that BLM is a promising biomarker in breast cancer.

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“…XRCC1 is ubiquitously expressed in normal tissues, but low levels of XRCC1 causing impaired BER may occur in terminally differentiated muscle cells and neurons [14, 15]. Variations in XRCC1 expression levels have been observed in breast cancer patient samples [16–18], and breast cancers with low expression levels of XRCC1 have been proposed as targets for PARPi treatment [16–19]. Defects in BER and XRCC1 may sensitize breast cancer cells to PARPi, similar to homologous recombination and BRCA1/2 defects [16, 18, 20, 21].…”

Section: Introductionmentioning

confidence: 99%

Defective base excision repair in the response to DNA damaging agents in triple negative breast cancer

Lee

Piett

Andrews

et al. 2019

Preprint

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21 22 23DNA repair defects have been increasingly focused on as therapeutic targets. In hormone 24 positive breast cancer, XRCC1-deficient tumors have been identified and proposed as 25 targets for combination therapies that damage DNA and inhibit DNA repair pathways. 26XRCC1 is a scaffold protein that functions in base excision repair (BER) by mediating 27 essential interactions between DNA glycosylases, AP endonuclease, poly(ADP-ribose) 28 polymerase 1, DNA polymerase β (POL β), and DNA ligases. Loss of XRCC1 confers 29 BER defects and hypersensitivity to DNA damaging agents. BER defects have not been 30 evaluated in triple negative breast cancer (TNBC), for which new therapeutic targets and 31 therapies are needed. To evaluate the potential of XRCC1 as an indicator of BER defects 32 in TNBC, we examined XRCC1 expression and localization in the TCGA database and in 33 TNBC cell lines. High XRCC1 expression was observed for TNBC tumors in the TCGA 34 database and expression of XRCC1 varied between TNBC cell lines. We also observed 35 changes in XRCC1 subcellular localization in TNBCs that alter the ability to repair base 36 lesions and single-strand breaks. Subcellular localization changes were also observed for 37 POL β that did not correlate with XRCC1 localization. Basal levels of DNA damage were 38 also measured in the TNBC cell lines, and damage levels correlated with observed 39 changes in XRCC1 expression, localization, and repair functions. The results confirmed 40 that XRCC1 expression changes may indicate DNA repair capacity changes but 41 emphasize that basal DNA damage levels along with expression and localization are 42 better indicators of DNA repair defects. Given the observed over-expression of XRCC1 in 43 TNBC preclinical models and the TCGA database, XRCC1 expression levels should be 44 considered when evaluating treatment responses of TNBC preclinical model cells. 45 3 Keywords: triple negative breast cancer, base excision repair, XRCC1, PARP1, DNA 46 repair, DNA damage, nuclear localization 47 48 Defects in DNA damage response and repair are driving factors in carcinogenesis 49and key determinants in the response to chemotherapy. Breast cancers may display 50 defects in DNA repair such as mutations in key DNA damage response and repair 51 proteins such as breast cancer-susceptibility (BRCA1/2) and tumor suppressor protein 52 p53 (TP53), and altered expression levels of DNA repair proteins thymine-DNA 53 glycosylase (TDG) and poly(ADP-ribose) polymerase 1 (PARP1) [1-3]. Therapeutic 54 outcomes may be improved by exploiting DNA repair defects present in cancer cells but 55 absent in normal cells, as in the use of PARP-inhibitors (PARPi) in cancers that have 56 BRCA1/2 deficiencies. However, characterization of DNA repair pathways often is lacking 57 in preclinical models and cell lines. Examining DNA repair defects in preclinical models 58 and patients is essential for evaluating the efficacy of therapeutic agents. 59 In breast cancer, DNA repair defects often extend beyond homologous 60 re...

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Targeting BRCA1‐BER deficient breast cancer by ATM or DNA‐PKcs blockade either alone or in combination with cisplatin for personalized therapy

Cited by 68 publications

References 49 publications

Aberrant DNA Double-strand Break Repair Threads in Breast Carcinoma: Orchestrating Genomic Insult Survival

Aberrant DNA Double-strand Break Repair Threads in Breast Carcinoma: Orchestrating Genomic Insult Survival

Transcriptomic and Protein Expression Analysis Reveals Clinicopathological Significance of Bloom Syndrome Helicase (BLM) in Breast Cancer

Defective base excision repair in the response to DNA damaging agents in triple negative breast cancer

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