Abstract 2928: Bortezomib sensitizes glioblastoma with unmethylated <i>MGMT</i> promoter to temozolomide-chemotherapy through MGMT depletion and abrogated autophagy flux

Rahman, Mohummad Aminur; Navarro, Andrea Gras; Brekke, Jorunn; Bindesbøll, Christian; Engelsen, Agnete S.T.; Sarowar, Shahin; Bahador, Marzieh; Gjertsen, Bjørn T.; Goplen, Dorota; Enger, Per Øyvind; Selheim, Frode; Simonsen, Anne; Chekenya, Martha

doi:10.1158/1538-7445.am2018-2928

Cited by 4 publications

(6 citation statements)

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“…7), promoting ATM/Chk2 mediated DNA damage signaling and activating p53-mediated G2/M cell cycle arrest 63 . As we recently demonstrated 59 , BTZ also depleted MGMT protein and mRNA, an additional mechanism that synergized with TMZ to effectively kill GBM cells by enhanced programmed cell death. We anticipate to uncover similar mechanisms of efficacy in the patients undergoing treatment in our phase II clinical trial, NCT03643549 (www.clinicaltrials.gov).…”

Section: Discussionmentioning

confidence: 57%

“…Another mechanism of TMZ resistance in GBM patients is represented by unmethylated MGMT promoter tumors 58 , where the enzyme and proficiently repairs the chemotherapy-induced DNA damage but the cells maintain a high apoptosis threshold. We recently showed that BTZ treatment depletes MGMT protein and mRNA and sensitizes GBM cells to TMZ chemotherapy 59 . In conclusion, BTZ augmented cell death of TMZ resistant tumor cells by accumulating autophagosomes as a result of abrogated autophagic flux (Fig.…”

Section: Discussionmentioning

confidence: 99%

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Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway

Rahman

Engelsen

Sarowar

et al. 2020

Preprint

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Glioblastoma (GBM) is invariably resistant to temozolomide (TMZ) chemotherapy. Inhibiting the proteasomal pathway is an emerging strategy to accumulate damaged proteins and inhibit their lysosomal degradation. We hypothesized that bortezomib (BTZ) might sensitize GBM cells to TMZ. We examined change in autophagic flux after drug treatments and in combination with pharmacological inhibitors or CRISPR cas9 knockout of autophagy-related genes -5 and -7 (ATG5 and ATG7, respectively). Autophagic flux was increased in temozolomide resistant GBM cells as indicated by diminished levels of the autophagy markers LC3A/B-II and p62(SQSTM1), increased localisation of LC3A/B-II with STX17, higher long-lived protein degradation and no induction of apoptosis. In contrast, BTZ treatment abrogated autophagic flux by accumulation of LC3A/B-II and p62(SQSTM1) positive autophagosomes that did not fuse with lysosomes and reduced degradation of long-lived proteins. BTZ synergistically enhanced TMZ efficacy by attenuating cell proliferation, increased DNA damage and apoptosis. CRISPR Cas ATG5 knockout reversed BTZ-induced autophagy blockade and rescued the GBM treated cells from death. We conclude that bortezomib abrogates temozolomide induced autophagy through ATG5 dependent pathway.

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Section: Discussionmentioning

confidence: 57%

Section: Discussionmentioning

confidence: 99%

Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway

Rahman

Engelsen

Sarowar

et al. 2020

Preprint

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“…This was expected due to the BTZ's ability to inhibit the MGMT activity in T98G cells, leading to an increased antiproliferative activity. 8,49 The improved anticancer activity in the MGMT-negative U251 cells can also be explained because BTZ possesses antiproliferative activity by its own (BTZ's survival inhibition curves in Figure S7 in the Supporting Information). Furthermore, we observed a significant reduction in the TMZ concentration required to achieve the same level of survival inhibition when combined with BTZ.…”

Section: Physicochemical Properties Of Tf-mentioning

confidence: 99%

Transferrin-Conjugated PLGA Nanoparticles for Co-Delivery of Temozolomide and Bortezomib to Glioblastoma Cells

Ramalho

Torres

Loureiro

et al. 2023

ACS Appl. Nano Mater.

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Glioblastoma (GBM) represents almost half of primary brain tumors, and its standard treatment with the alkylating agent temozolomide (TMZ) is not curative. Treatment failure is partially related to intrinsic resistance mechanisms mediated by the O6methylguanine-DNA methyltransferase (MGMT) protein, frequently overexpressed in GBM patients. Clinical trials have shown that the anticancer agent bortezomib (BTZ) can increase TMZ's therapeutic efficacy in GBM patients by downregulating MGMT expression. However, the clinical application of this therapeutic strategy has been stalled due to the high toxicity of the combined therapy. The codelivery of TMZ and BTZ through nanoparticles (NPs) of poly(lacticco-glycolic acid) (PLGA) is proposed in this work, aiming to explore their synergistic effect while decreasing the drug's toxicity. The developed NPs were optimized by central composite design (CCD), then further conjugated with transferrin (Tf) to enhance their GBM targeting ability by targeting the blood−brain barrier (BBB) and the cancer cells. The obtained NPs exhibited suitable GBM cell delivery features (sizes lower than 200 nm, low polydispersity, and negative surface charge) and a controlled and sustained release for 20 days. The uptake and antiproliferative effect of the developed NPs were evaluated in in vitro human GBM models. The obtained results disclosed that the NPs are rapidly taken up by the GBM cells, promoting synergistic drug effects in inhibiting tumor cell survival and proliferation. This cytotoxicity was associated with significant cellular morphological changes. Additionally, the biocompatibility of unloaded NPs was evaluated in healthy brain cells, demonstrating the safety of the nanocarrier. These findings prove that co-delivery of BTZ and TMZ in Tf-conjugated PLGA NPs is a promising approach to treat GBM, overcoming the limitations of current therapeutic strategies, such as drug resistance and increased side effects.

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“…Therefore, these trials are not using the optimal schedule identified here. Expanded access would be justified by the lack of long-term effective treatments for this lethal disease [62], and could employ our optimal schedule. Even so, one limitation of our modelling approach should be emphasized: our model incorporates synergistic effectiveness between TMZ and MGMT/APNG inhibition, but does not include synergistic toxicity.…”

Section: Potential For Clinical Translationmentioning

confidence: 99%

Mitigating temozolomide resistance in glioblastoma via DNA damage-repair inhibition

Sorribes

Handelman

Jain

2020

J. R. Soc. Interface.

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Glioblastomas are among the most lethal cancers, with a 5 year survival rate below 25%. Temozolomide is typically used in glioblastoma treatment; however, the enzymes alkylpurine-DNA- N -glycosylase (APNG) and methylguanine-DNA-methyltransferase (MGMT) efficiently mediate the repair of DNA damage caused by temozolomide, reducing treatment efficacy. Consequently, APNG and MGMT inhibition has been proposed as a way of overcoming chemotherapy resistance. Here, we develop a mechanistic mathematical model that explicitly incorporates the effects of chemotherapy on tumour cells, including the processes of DNA damage induction, cell arrest and DNA repair. Our model is carefully parametrized and validated, and then used to virtually recreate the response of heteroclonal glioblastomas to dual treatment with temozolomide and inhibitors of APNG/MGMT. Using our mechanistic model, we identify four combination treatment strategies optimized by tumour cell phenotype, and isolate the strategy most likely to succeed in a pre-clinical and clinical setting. If confirmed in clinical trials, these strategies have the potential to offset chemotherapy resistance in patients with glioblastoma and improve overall survival.

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Abstract 2928: Bortezomib sensitizes glioblastoma with unmethylated MGMT promoter to temozolomide-chemotherapy through MGMT depletion and abrogated autophagy flux

Cited by 4 publications

References 0 publications

Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway

Bortezomib abrogates temozolomide-induced autophagic flux through an ATG5 dependent pathway

Transferrin-Conjugated PLGA Nanoparticles for Co-Delivery of Temozolomide and Bortezomib to Glioblastoma Cells

Mitigating temozolomide resistance in glioblastoma via DNA damage-repair inhibition

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