Rtid-03. Design and Initiation of Pivotal Studies for Berubicin, a Novel, Potent Topoisomerase Ii Poison for the Treatment of Recurrent Glioblastoma Multiforme (Gbm)

Silberman, Sandra; Hsu, Sigmund; Muczyczenko, Zena; Picker, Donald; Sipowicz, Marek A.; Żak, Ewa; Buczyńska, Agnieszka; Olejniczak, Mariusz; Priebe, Waldemar

doi:10.1093/neuonc/noab196.765

Cited by 4 publications

(7 citation statements)

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“… 61 In a Phase I trial in recurrent GB, 12 of the 35 patients (48%) attained longer PFS. 62 In 2020, the US FDA granted Orphan Drug Designation to berubicin for the treatment of recurrent GB and granted it Fast Track Designation in 2021. An ongoing phase II trial (ClinicalTrials.gov NCT04762069) is comparing berubicin versus lomustine in recurrent GB.…”

Section: Novel Lines Of Research In Glioblastoma and Gliomas In Generalmentioning

confidence: 99%

Recurrent Glioblastoma: Ongoing Clinical Challenges and Future Prospects

Pineda¹,

Doménech²,

Hernández³

et al. 2023

OTT

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Virtually all glioblastomas treated in the first-line setting will recur in a short period of time, and the search for alternative effective treatments has so far been unsuccessful. Various obstacles remain unresolved, and no effective salvage therapy for recurrent glioblastoma can be envisaged in the short term. One of the main impediments to progress is the low incidence of the disease itself in comparison with other pathologies, which will be made even lower by the recent WHO classification of gliomas, which includes molecular alterations. This new classification helps refine patient prognosis but does not clarify the most appropriate treatment. Other impediments are related to clinical trials: glioblastoma patients are often excluded from trials due to their advanced age and limiting neurological symptoms; there is also the question of how best to measure treatment efficacy, which conditions the design of trials and can affect the acceptance of results by oncologists and medicine agencies. Other obstacles are related to the drugs themselves: most treatments cannot cross the blood-brain-barrier or the brain-to-tumor barrier to reach therapeutic drug levels in the tumor without producing toxicity; the drugs under study may have adverse metabolic interactions with those required for symptom control; identifying the target of the drug can be a complex issue. Additionally, the optimal method of treatment – local vs systemic therapy, the choice of chemotherapy, irradiation, targeted therapy, immunotherapy, or a combination thereof – is not yet clear in glioblastoma in comparison with other cancers. Finally, in addition to curing or stabilizing the disease, glioblastoma therapy should aim at maintaining the neurological status of the patients to enable them to return to their previous lifestyle. Here we review currently available treatments, obstacles in the search for new treatments, and novel lines of research that show promise for the future.

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Section: Novel Lines Of Research In Glioblastoma and Gliomas In Generalmentioning

confidence: 99%

Recurrent Glioblastoma: Ongoing Clinical Challenges and Future Prospects

Pineda¹,

Doménech²,

Hernández³

et al. 2023

OTT

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“…Among the tested drug candidates for GBM therapy, a new molecule targeting DNA replication is Berubicin (NCT04915404, NCT04762069). Berubicin is a doxorubicin analog that, contrary to currently used anthracyclines, crosses the BBB and can reach brain tissue [81]. Similar to other anthracyclines, the primary mechanism of action of Berubicin involves the drug's ability to intercalate within DNA base pairs, causing the breakage of DNA strands and inhibition of nucleic acids' synthesis.…”

Section: Dna-targeting Drug Candidates For Gbm Therapymentioning

confidence: 99%

“…Berubicin inhibits the enzyme topoisomerase II (TopoII), causing DNA damage and apoptosis induction [82]. Berubicin demonstrated significantly more cytotoxic activity in an orthotopic GBM murine model than TMZ [81]. Berubicin has already been tested in a phase 1 clinical trial at the MD Anderson Cancer Institute in patients with recurrent glioma [83].…”

Section: Dna-targeting Drug Candidates For Gbm Therapymentioning

confidence: 99%

Looking for the Holy Grail—Drug Candidates for Glioblastoma Multiforme Chemotherapy

Pająk

2022

Biomedicines

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Glioblastoma multiforme (GBM) is the deadliest and the most heterogeneous brain cancer. The median survival time of GBM patients is approximately 8 to 15 months after initial diagnosis. GBM development is determined by numerous signaling pathways and is considered one of the most challenging and complicated-to-treat cancer types. Standard GBM therapy consist of surgery followed by radiotherapy or chemotherapy, and combined treatment. Current standard of care (SOC) does not offer a significant chance for GBM patients to combat cancer, and the selection of available drugs is limited. For almost 20 years, there has been only one drug, Temozolomide (TMZ), approved as a first-line GBM treatment. Due to the limited efficacy of TMZ and the high rate of resistant patients, the implementation of new chemotherapeutics is highly desired. However, due to the unique properties of GBM, many challenges still need to be overcome before reaching a ‘breakthrough’. This review article describes the most recent compounds introduced into clinical trials as drug candidates for GBM chemotherapy.

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“…Berubicin is a chemotherapy medication that has primarily been developed for the treatment of glioblastoma, the most aggressive and treatment-resistant type of brain cancer. − This drug belongs to the family of anthracyclines ,, and is able to cross the blood–brain barrier and reach brain tumors effectively. , Anthracyclines aim mainly at inducing DNA damage in the targeted tumor cells by interfering with the action of topoisomerase II, a nuclear enzyme that fixes topological problems in DNA caused mainly by the processes of replication and transcription. ,− Intercalation into DNA is numbered among the mechanisms of action of anthracyclines due to the existence of an aglycone planar structure that is capable of intercalating between the strands of DNA. , Aglycone is a system of four rings with one of them being a saturated and substituted ring to which a side chain and one or more sugar residues are covalently attached (see Figure a); , it is noted that the characteristic reddish color of anthracyclines is owed to this system of rings. , Berubicin is an O-benzylated derivative of doxorubicin, one of the prototype molecules of the anthracycline class; the difference between them lies only in the sugar moiety. The advantage of berubicin in relation to other anthracyclines is its ability to circumvent the multidrug resistance mechanisms, − in contrast with the other anthracyclines. , This makes it more effective at inducing DNA damage, while at the same time being less lethal, compared to the parental drug, doxorubicin . In addition to the advantages, substituting berubicin for doxorubicin makes the drug more hydrophobic which may be undesired in certain cases.…”

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Interactions of a Novel Anthracycline with Oligonucleotide DNA and Cyclodextrins in an Aqueous Environment

Mikaelian,

Megariotis,

Theodorou

2024

J. Phys. Chem. B

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Rtid-03. Design and Initiation of Pivotal Studies for Berubicin, a Novel, Potent Topoisomerase Ii Poison for the Treatment of Recurrent Glioblastoma Multiforme (Gbm)

Cited by 4 publications

References 0 publications

Recurrent Glioblastoma: Ongoing Clinical Challenges and Future Prospects

Recurrent Glioblastoma: Ongoing Clinical Challenges and Future Prospects

Looking for the Holy Grail—Drug Candidates for Glioblastoma Multiforme Chemotherapy

Interactions of a Novel Anthracycline with Oligonucleotide DNA and Cyclodextrins in an Aqueous Environment

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