Inhibition of DNA-repair genes Ercc1 and Mgmt enhances temozolomide efficacy in gliomas treatment: a pre-clinical study

Boccard, Sandra; Marand, Sandie V.; Geraci, Sandra; Pycroft, Laurie; Berger, F.; Pelletier, Laurent

doi:10.18632/oncotarget.4909

Cited by 25 publications

(21 citation statements)

References 60 publications

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“…Resistance mechanisms that lead to tumor progression during alkylator therapy include the repair of TMZ-induced monofunctional alkylation and single strand DNA lesion by methyl-guanyl methyltransferase (MGMT) and repair of double stranded DNA breaks (DSB) by specific DNA repair enzymes in glioma cells and in GSCs (42). Consequently, therapeutic strategies that can potentiate the activity of TMZ are of high clinical relevance.…”

Section: Resultsmentioning

confidence: 99%

Efficacy of Onalespib, a Long-Acting Second-Generation HSP90 Inhibitor, as a Single Agent and in Combination with Temozolomide against Malignant Gliomas

Canella

Welker

Yoo

et al. 2017

Clinical Cancer Research

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Purpose HSP90, a highly conserved molecular chaperone that regulates the function of several oncogenic client proteins is altered in glioblastoma. However, HSP90 inhibitors currently in clinical trials are short-acting, have unacceptable toxicities or are unable to cross the blood brain barrier (BBB). We examined the efficacy of onalespib, a potent, long-acting novel HSP90 inhibitor as a single agent and in combination with temozolomide (TMZ) against gliomas in vitro and in vivo. Experimental Design The effect of onalespib on HSP90, its client proteins, and on the biology of glioma cell lines and patient-derived glioma-initiating cells (GSC) was determined. Brain and plasma pharmacokinetics of onalespib and its ability to inhibit HSP90 in vivo was assessed in non-tumor bearing mice. Its efficacy as a single agent or in combination with TMZ was assessed in vitro and in vivo using zebrafish and patient derived GSC xenograft mouse glioma models. Results Onalespib mediated HSP90 inhibition depleted several survival-promoting client proteins such as EGFR, EGFRvIII and AKT, disrupted their downstream signaling and decreased the proliferation, migration, angiogenesis and survival of glioma cell lines and GSCs. Onalespib effectively crossed the BBB to inhibit HSP90 in vivo and extended survival as a single agent in zebrafish xenografts and in combination with TMZ in both zebrafish and GSC mouse xenografts. Conclusions Our results demonstrate the long-acting effects of onalespib against gliomas in vitro and in vivo which combined with its ability to cross the BBB support its development as a potential therapeutic agent in combination with TMZ against gliomas.

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Section: Resultsmentioning

confidence: 99%

Efficacy of Onalespib, a Long-Acting Second-Generation HSP90 Inhibitor, as a Single Agent and in Combination with Temozolomide against Malignant Gliomas

Canella

Welker

Yoo

et al. 2017

Clinical Cancer Research

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“…On the other hand, activation of the AKT signaling pathway decreased the sensitivity of cells to L-OHP induced apoptosis in 1 5 9 13 17 21 25 29 33 37 41 45 49 53 57 61 65 69 73 77 81 85 89 93 97 101 105 109 113 117 121 125 129 These results demonstrated that Linc00152 contributed to L-OHP resistance at least in part through modulating the miR-193a-3p/ ERBB4/AKT axis. In colon cancer, biomarkers associated with L-OHP resistance, for example, excision repair cross-complementing 1 protein (ERCC1) and G-protein-coupled receptor galanin receptor 1 (GalR 1), have been reported, 50,51 revealing useful targets of L-OHP resistance are clinically important. Nevertheless, these findings have failed to translate to clinical practice and optimal prognostic biomarkers for L-OHP-based chemotherapy have not been established up to now.…”

Section: Discussionmentioning

confidence: 99%

Linc00152 Functions as a Competing Endogenous RNA to Confer Oxaliplatin Resistance and Holds Prognostic Values in Colon Cancer

et al. 2016

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Long noncoding RNAs act as crucial regulators in plenty of human cancers, yet their potential roles and molecular mechanisms in chemoresistance are poorly understood. This study showed that a novel lncRNA, long intergenic noncoding RNA 152 (Linc00152 ), promoted tumor progression and conferred resistance to oxaliplatin (L-OHP)-induced apoptosis in vitro and in vivo. It antagonized chemosensitivity through acting as a competing endogenous RNA to modulate the expression of miR-193a-3p, and then erb-b2 receptor tyrosine kinase 4 (ERBB4). Knockdown of ERBB4 in colon cancer cells decreased AKT phosphorylation, which resulted in decreased L-OHP resistance. Consistent with above findings, the specific AKT signaling inhibitor and activator were used, respectively, which demonstrated that Linc00152 contributed to L-OHP resistance at least partly through activating AKT pathway. Further studies indicated that Linc00152 was increased and appeared to be an independent prognostic factor for decreased survival and increased disease recurrence in stage II and III colon cancer patients undergoing L-OHP-based chemotherapy after surgery. Collectively, our findings established Linc00152 as a candidate prognostic indicator of outcome and drug responsiveness in colon cancer patients, and the involvement of competing endogenous RNAs mechanism in Linc00152/ miR-193a-3p/ERBB4/AKT signaling axis may provide a novel choice in the investigation of drug resistance.

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“…It was also shown that the disruption of Ape1 (Bobola et al, 2001) or DNA polymerase b (Trivedi et al, 2008) activity sensitizes cells to TMZ. Moreover, increased NER activity was detected after treatment with TMZ (Nagel et al, 2017), while downregulation of ERCC1 promoted higher sensitivity to TMZ treatment, similarly to MGMT inhibition (Boccard et al, 2015).…”

Section: Dna Repair and Gbm Resistance To Treatmentmentioning

confidence: 91%

“…The list of significant biomarkers is growing in an astonishing manner and includes a wide range of molecules such as lncRNAs and microRNAs (e.g. HOTAIR and miR-141), and several DNA repair genes (Boccard et al, 2015;Bian et al, 2016;Reon et al, 2016), which are importantly correlated with genome stability and will be explored in more detail in the next sections. Table 3 summarizes the main DNA repair biomarkers discussed in this review.…”

Section: Glioma Classification and Frequent Genetic Alterationsmentioning

confidence: 99%

DNA repair genes in astrocytoma tumorigenesis, progression and therapy resistance

et al. 2020

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Glioblastoma (GBM) is the most common and malignant type of primary brain tumor, showing rapid development and resistance to therapies. On average, patients survive 14.6 months after diagnosis and less than 5% survive five years or more. Several pieces of evidence have suggested that the DNA damage signaling and repair activities are directly correlated with GBM phenotype and exhibit opposite functions in cancer establishment and progression. The functions of these pathways appear to present a dual role in tumorigenesis and cancer progression. Activation and/or overexpression of ATRX, ATM and RAD51 genes were extensively characterized as barriers for GBM initiation, but paradoxically the exacerbated activity of these genes was further associated with cancer progression to more aggressive stages. Excessive amounts of other DNA repair proteins, namely HJURP, EXO1, NEIL3, BRCA2, and BRIP, have also been connected to proliferative competence, resistance and poor prognosis. This scenario suggests that these networks help tumor cells to manage replicative stress and treatment-induced damage, diminishing genome instability and conferring therapy resistance. Finally, in this review we address promising new drugs and therapeutic approaches with potential to improve patient survival. However, despite all technological advances, the prognosis is still dismal and further research is needed to dissect such complex mechanisms.

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Inhibition of DNA-repair genes Ercc1 and Mgmt enhances temozolomide efficacy in gliomas treatment: a pre-clinical study

Cited by 25 publications

References 60 publications

Efficacy of Onalespib, a Long-Acting Second-Generation HSP90 Inhibitor, as a Single Agent and in Combination with Temozolomide against Malignant Gliomas

Efficacy of Onalespib, a Long-Acting Second-Generation HSP90 Inhibitor, as a Single Agent and in Combination with Temozolomide against Malignant Gliomas

Linc00152 Functions as a Competing Endogenous RNA to Confer Oxaliplatin Resistance and Holds Prognostic Values in Colon Cancer

DNA repair genes in astrocytoma tumorigenesis, progression and therapy resistance

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