Bortezomib administered prior to temozolomide depletes MGMT, chemosensitizes glioblastoma with unmethylated MGMT promoter and prolongs animal survival

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

doi:10.1038/s41416-019-0551-1

Cited by 35 publications

(49 citation statements)

References 39 publications

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“…The ultimate aim was to attain combination treatment with BTZ and TMZ at 200 mg/m 2 which was closest to the most effective dose in the preclinical study. 22 Total treatment duration per patient was estimated for 6 to 12 months unless disease progression.…”

Section: Treatment Planmentioning

confidence: 99%

“…It has been established that NF-κB binding sites are present within the MGMT promoter region, that MGMT messenger RNA (mRNA) is induced by NF-κB/ p65, and that MGMT expression correlates with NF-κB activation regardless of promoter methylation status. 15,22 NF-κB activation requires 26S proteasomal processing. 23 Bortezomib (BTZ) is a proteasome inhibitor that has been approved for treatment of multiple myeloma, mantle cell lymphoma and trialed in early phase trials for treatment of GBM.…”

Section: Introductionmentioning

confidence: 99%

“…This correlated with reduced MGMT protein and mRNA expression by 70%-80% and sensitized the GBM cells to TMZ chemotherapy. 22 Two other studies also investigated MGMT depletion via mechanisms associated with activation of NFκB, MAPK, STAT3, and HIF-1α pathways after BTZ treatment. 16,18 As well as depleting the tumor's cytoprotective mechanisms, agents that simultaneously promote tumor recognition by cells of the immune system may be attractive anticancer candidates.…”

Section: Introductionmentioning

confidence: 99%

“…24 Sequential combination of BTZ 48 hours before TMZ 164 mg/m 2 treatment, depleted MGMT mRNA in vivo, attenuated tumor growth and significantly prolonged animal survival. 22 Thus, this phase IB of our BORTEM-17 clinical trial (NCT03643549) was launched to investigate whether pretreatment of recurrent GBM patients with BTZ 1.3 mg/m 2 on days 1, 4, and 7, to deplete MGMT levels 48 hours before TMZ, commencing on days 3 to 7 every 4th week, might sensitize MGMT unmethylated GBM to TMZ chemotherapy. We assessed the maximal safe escalated TMZ dose administered in sensitization schedule with BTZ and whether treatment enhanced differentiation of cytotoxic immune subsets to impact treatment responses.…”

Section: Introductionmentioning

confidence: 99%

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Sequential bortezomib and temozolomide treatment promotes immunological responses in glioblastoma patients with positive clinical outcomes: A phase 1B study

Rahman

Brekke

Arnesen

et al. 2020

Immunity Inflam & Disease

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Background: Glioblastoma (GBM) is an aggressive malignant brain tumor where median survival is approximately 15 months after best available multimodal treatment. Recurrence is inevitable, largely due to O 6 methylguanine DNA methyltransferase (MGMT) that renders the tumors resistant to temozolomide (TMZ). We hypothesized that pretreatment with bortezomib (BTZ) 48 hours prior to TMZ to deplete MGMT levels would be safe and tolerated by patients with recurrent GBM harboring unmethylated MGMT promoter. The secondary objective was to investigate whether 26S proteasome blockade may enhance differentiation of cytotoxic immune subsets to impact treatment responses measured by radiological criteria and clinical outcomes. Methods: Ten patients received intravenous BTZ 1.3 mg/m 2 on days 1, 4, and 7 during each 4th weekly TMZ-chemotherapy starting on day 3 and escalated from 150 mg/m 2 per oral 5 days/wk via 175 to 200 mg/m 2 in cycles 1, 2, and 3, respectively. Adverse events and quality of life were evaluated by CTCAE and EQ-5D-5L questionnaire, and immunological biomarkers evaluated by flow cytometry and Luminex enzyme-linked immunosorbent assay. Results: Sequential BTZ + TMZ therapy was safe and well tolerated. Pain and performance of daily activities had greatest impact on patients' self-reported quality of life and were inversely correlated with Karnofsky performance status. Patients segregated a priori into three groups, where group 1 displayed

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Section: Treatment Planmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Sequential bortezomib and temozolomide treatment promotes immunological responses in glioblastoma patients with positive clinical outcomes: A phase 1B study

Rahman

Brekke

Arnesen

et al. 2020

Immunity Inflam & Disease

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“…Glioblastoma (GBM) is the most common and aggressive intracranial malignant brain tumor with the median survival duration <2 years in spite of chemotherapy, radiation or surgical resection (Natsume et al, 2019). In the current chemotherapies, such as temozolomide, drug resistance is the predominant obstacle (Zhang et al, 2012;Chen et al, 2019;Kim et al, 2019;Rahman et al, 2019;Su et al, 2019;Xingyi et al, 2019). On the basis of the latest experimental results obtained from the large-scale profiling which included the whole exome and RNA sequencing, it can be learnt that genetic and epigenetic mechanisms are involved in the occurrence and progress of glioma cells (Cancer Genome Atlas Research, 2008;Brennan et al, 2013), especially the aberrant epigenetic silencing of genes caused by histone deacetylation (Vaissiere et al, 2008;Cartron et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

Selective Inhibition of HDAC1 by Macrocyclic Polypeptide for the Treatment of Glioblastoma: A Binding Mechanistic Analysis Based on Molecular Dynamics

Wang

Ren

et al. 2020

Front. Mol. Biosci.

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Glioblastoma (GBM) is the most common and aggressive intracranial malignant brain tumor, and the abnormal expression of HDAC1 is closely correlated to the progression, recurrence and metastasis of GBM cells, making selective inhibition of HDAC1 a promising strategy for GBM treatments. Among all available selective HDAC1 inhibitors, the macrocyclic peptides have gained great attention due to their remarkable inhibitory selectivity on HDAC1. However, the binding mechanism underlying this selectivity is still elusive, which increases the difficulty of designing and synthesizing the macrocyclic peptide-based anti-GBM drug. Herein, multiple computational approaches were employed to explore the binding behaviors of a typical macrocyclic peptide FK228 in both HDAC1 and HDAC6. Starting from the docking conformations of FK228 in the binding pockets of HDAC1&6, relatively long MD simulation (500 ns) shown that the hydrophobic interaction and hydrogen bonding of E91 and D92 in the Loop2 of HDAC1 with the Cap had a certain traction effect on FK228, and the sub-pocket formed by Loop1 and Loop2 in HDAC1 could better accommodate the Cap group, which had a positive effect on maintaining the active conformation of FK228. While the weakening of the interactions between FK228 and the residues in the Loop2 of HDAC6 during the MD simulation led to the large deflection of FK228 in the binding site, which also resulted in the decrease in the interactions between the Linker region of FK228 and the previously identified key amino acids (H134, F143, H174, and F203). Therefore, the residues located in Loop1 and Loop2 contributed in maintaining the active conformation of FK228, which would provide valuable hints for the discovery and design of novel macrocyclic polypeptide HDAC inhibitors.

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MGMT inactivation as a new biomarker in patients with advanced biliary tract cancers

et al. 2022

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Biliary tract cancers (BTCs) have poor prognosis and limited therapeutic options. The impact of O6‐methylguanine‐DNA methyltransferase (MGMT) inactivation in advanced BTC patients is not established. We investigated the prevalence, prognostic, and predictive impact of MGMT inactivation in two multicenter cohorts. MGMT inactivation was assessed through PCR and immunohistochemistry (IHC) in an Italian cohort; the results were then externally validated using RNA sequencing (RNA‐seq) data from the BTC subcohort of the Molecularly Aided Stratification for Tumor Eradication Research (MASTER) precision oncology program of the National Center for Tumor Diseases Heidelberg and the German Cancer Consortium. Among 164 Italian cases, 18% presented MGMT promoter hypermethylation (> 14%) and 73% had negative MGMT protein expression. Both were associated with worse overall survival (OS; HR 2.31; P < 0.001 and HR 1.99, P = 0.012, respectively). In the MASTER cohort, patients with lower MGMT mRNA expression showed significantly poorer OS (median OS [mOS] 20.4 vs 31.7 months, unadjusted HR 1.89; P = 0.043). Our results suggest that MGMT inactivation is a frequent epigenetic alteration in BTC, with a significant prognostic impact, and provide the rationale to explore DNA‐damaging agents in MGMT‐inactivated BTCs.

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Bortezomib administered prior to temozolomide depletes MGMT, chemosensitizes glioblastoma with unmethylated MGMT promoter and prolongs animal survival

Cited by 35 publications

References 39 publications

Sequential bortezomib and temozolomide treatment promotes immunological responses in glioblastoma patients with positive clinical outcomes: A phase 1B study

Sequential bortezomib and temozolomide treatment promotes immunological responses in glioblastoma patients with positive clinical outcomes: A phase 1B study

Selective Inhibition of HDAC1 by Macrocyclic Polypeptide for the Treatment of Glioblastoma: A Binding Mechanistic Analysis Based on Molecular Dynamics

MGMT inactivation as a new biomarker in patients with advanced biliary tract cancers

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