Linking DNA Damage and Hormone Signaling Pathways in Cancer

Schiewer, Matthew J.; Knudsen, Karen E.

doi:10.1016/j.tem.2016.02.004

Cited by 53 publications

(46 citation statements)

References 81 publications

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“…Modest DNA-damage (γH2AX) was observed at the higher dose of YM155 with R1881 (FIG 2A). Reductions in γH2AX and cleaved PARP1 were observed in AR-suppressed cells in the control and low-dose YM155 groups, consistent with reduced replicative stress(46) and DNA-repair supportive effects of AR signaling(47) (FIG 2A). Additionally, there was no change in levels of autophagy (as measured by Beclin and AT5 levels) and negligible changes in apoptosis (as measured by cleaved-Caspase3 and PARP1) between the YM155 and control groups (FIG 2A).…”

Section: Resultssupporting

confidence: 60%

Exploiting AR-Regulated Drug Transport to Induce Sensitivity to the Survivin Inhibitor YM155

Nyquist

Corella

Burns

et al. 2017

Molecular Cancer Research

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Androgen receptor (AR) signaling is fundamental to prostate cancer and is the dominant therapeutic target in metastatic disease. However, stringent androgen deprivation therapy (ADT) regimens decrease quality of life and have been largely unsuccessful in curtailing mortality. Recent clinical and pre-clinical studies have taken advantage of the dichotomous ability of AR signaling to elicit growth-suppressive and differentiating effects by administering hyper-physiological levels of testosterone. In this study, high-throughput drug screening identified a potent synergy between high-androgen therapy and YM155, a transcriptional inhibitor of Survivin (BIRC5). This interaction was mediated by the direct transcriptional upregulation of the YM155 transporter SLC35F2 by the AR. Androgen-mediated YM155-induced cell death was completely blocked by the overexpression of multidrug resistance (MDR) transporter ABCB1. SLC35F2 expression was significantly correlated with intra-tumor androgen levels in four distinct patient-derived xenografts (PDX) models, and with AR-activity score in a large gene expression dataset of castration resistant metastases. A subset of tumors had significantly elevated SLC35F2 expression and therefore, may identify patients who are highly responsive to YM155 treatment.Implications-The combination of androgen therapy with YM155 represents a novel drug synergy, and SLC35F2 may serve as a clinical biomarker of response to YM155.

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Section: Resultssupporting

confidence: 60%

Exploiting AR-Regulated Drug Transport to Induce Sensitivity to the Survivin Inhibitor YM155

Nyquist

Corella

Burns

et al. 2017

Molecular Cancer Research

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“…Based on the previous genetic and pathological study, BRCA1-associated breast cancers are more likely to be estrogen (ER) and progesterone receptor (PgR) negative (~90%) matched with sporadic breast cancers (~30%). In contrast, the occurrence of ER and PgR for BRCA2-and BRCAX-associated cancers is not considerably different to sporadic cancers [1,3,6,34].…”

Section: Dna Repair Response and Breast Carcinoma Phenotypesmentioning

confidence: 75%

“…The reason behind the manipulation and subversion of DNA repair response on breast carcinoma is explored in the perspectives of hormonal signaling. There are sound evidences that certain steroid hormones alter the double strand break repair mediated by BRCA1 in case of hereditary type of breast cancer [34]. In BRCA1 and BRCA2 mutation associated cancer, overexpression of HER2 is seldom.…”

Section: Dna Repair Response and Breast Carcinoma Phenotypesmentioning

confidence: 99%

“…The well-crafted DNA damage repair machinery inside the cell is tightly regulated and according the division of work inside the cellular periphery, a specific family of repair team agent is recruited when particular lesion is sensed. Onset of carcinoma changes the DNA damage response which can be the cause of enhanced genotoxic stress which can be considered as targeted therapeutic agents [34].…”

Section: Ber and Their Molecular Actorsmentioning

confidence: 99%

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Base Excision Repair Manipulation in Breast Carcinoma: A Prospective Avenue to Potentiate Genome Insulting Approach

Jain¹,

Yadav²,

Beig³

et al. 2017

Oncomedicine

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Treating breast carcinoma gets tedious due to its invasive molecular subtypes and their various molecular genotypes. Depending upon genotype and phenotype of breast tumor types, they manipulate their survival arms in the form of DNA repair protein player including base excision repair (BER) pathway. Currently, avenues to treat breast cancer ate genotoxic drugs inflicting inter and intra-strand cross links, base modification and changes in the genome combined with inhibitors of BER pathway. This review summarizes the updated information on the relevance of BER response in breast carcinoma phenotypes and their potential therapeutic interference in the last decade.

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“…This was only the beginning of the studies on the role of IRC in human health and disease. It had later become clear that the capacity for DNA repair and management of genomic integrity in humans could have significant effects on the risk for development of many common diseases with late onset, such as diabetes and cancer (Roy et al 2007, Petkova et al 2011b, Schiewer and Knudsen 2016, cardiovascular disease (Chelenkova et al 2014, Wu andRoks 2014), neurodegenerative disease (Coppedè and Migliore 2015, Nayyar et al 2015); and that it could potentially reflect on the susceptibility for disease in different individuals, and at different ages (Cherdyntseva et al 2010, Petkova et al 2013 and the outcomes of different genotoxic treatments (Kan and Zhang 2015, Velic et al 2015, Petkova et al 2014b. DNA damage repair pathways began to be regarded as useful therapeutic targets in cancer therapy, , Khalil et al 2012b, Khalil et al 2012c, Gavande et al 2016.…”

Section: The Discovery Of Individual Repair Capacitymentioning

confidence: 99%

The success of stem cell transplantations and the potential post-transplantation complications may be dependent, among other factors, on the capacity of the recipient and the transplanted cells to repair DNA damage

Reynolds¹

2016

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Cell therapy is presently a treatment of choice for many types of haematological and metabolic diseases and is likely to become a therapeutic option for other severe human diseases and conditions in the near future. The success of cell transplantation depends on a variety of factors, including the degree of HLA match between the donor and the recipient, the infectious burden of the graft, cell dosage, age, general state of the recipient and other incompletely characterised features of the donor and the recipient. It is likely that the individual capacity for identification and repair of DNA damage and maintenance of genomic integrity may account, at least in part, for these elusive factors that modulate transplantation outcome in terms of success rate and both long and short term posttransplantation complications. This paper outlines the role of individual repair capacity of the donor and recipient in cell transplantations, summarising the little knowledge already accumulated in the field whilst analysing the known major issues of the use of different types of stem cells. Attention will be given to their capacity to maintain the integrity of their genome, the ability to renew their own population, differentiate into various cell types and in ‡

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Linking DNA Damage and Hormone Signaling Pathways in Cancer

Cited by 53 publications

References 81 publications

Exploiting AR-Regulated Drug Transport to Induce Sensitivity to the Survivin Inhibitor YM155

Exploiting AR-Regulated Drug Transport to Induce Sensitivity to the Survivin Inhibitor YM155

Base Excision Repair Manipulation in Breast Carcinoma: A Prospective Avenue to Potentiate Genome Insulting Approach

The success of stem cell transplantations and the potential post-transplantation complications may be dependent, among other factors, on the capacity of the recipient and the transplanted cells to repair DNA damage

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