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Home > CNS GBM Recurrent - beVACizumab Q2W

CNS GBM Recurrent - beVACizumab Q2W

Treatment Overview

This regimen contains a medicine where one or more biosimilars may exist. Any biosimilars used have been reviewed by the regulator (Medsafe) and relevant specialists were consulted nationally. Where regulators, in consultation with relevant specialists, have agreed that there are no clinically significant differences in either safety or effectiveness between a biosimilar and originator product, these drugs may be used interchangeably.

Cycle 1 (and all further cycles) - 14 days

Cycle length:
14

Cycle details

Cycle 1 (and all further cycles) - 14 days

Medication Dose Route Days Max Duration
beVACizumab 10 mg/kg intravenous 1 90 minutes

Full details

Cycle 1 (and all further cycles) - 14 days

Day: 1

Medication Dose Route Max duration Details
beVACizumab 10 mg/kg intravenous 90 minutes
Instructions:

Blood pressure and urinalysis should be checked before each administration. If urine dipstick protein is less than or equal to 3+, proceed with infusion.

If the initial dose of beVACizumab is well tolerated, the second dose may be administered over 60 minutes, and the third and subsequent doses may be administered over 30 minutes.

Supportive Care Factors

Factor Value
Emetogenicity: Minimal
Hypersensitivity / Infusion related reaction risk: Low - routine premedication not recommended

References

Wong, E. T., S. Gautam, C. Malchow, et al. 2011. "Bevacizumab for recurrent glioblastoma multiforme: a meta-analysis." J Natl Compr Canc Netw 9(4):403-407., PMID: 21464145

Khasraw, M., M. S. Ameratunga, R. Grant, et al. 2014. "Antiangiogenic therapy for high-grade glioma." Cochrane Database Syst Rev 9:CD008218., PMID: 25242542

Hovey, E.J., K.M. Field, M.A. Rosenthal, et al. 2017. "Continuing or ceasing bevacizumab beyond progression in recurrent glioblastoma: an exploratory randomized phase II trial" Neuro-Oncology Practice 4(3): 171-181, PMID: 31386014

Friedman, H. S., M. D. Prados, P. Y. Wen, et al. 2009. "Bevacizumab alone and in combination with irinotecan in recurrent glioblastoma." J Clin Oncol 27(28):4733-4740., PMID: 19720927

Kreisl, T. N., L. Kim, K. Moore, et al. 2009. "Phase II trial of single-agent bevacizumab followed by bevacizumab plus irinotecan at tumor progression in recurrent glioblastoma." J Clin Oncol 27(5):740-745., PMID: 19114704

Field, K. M., J. Simes, A. K. Nowak, et al. 2015. "Randomized phase 2 study of carboplatin and bevacizumab in recurrent glioblastoma." Neuro Oncol 17(11):1504-1513., PMID: 26130744

Taal, W., H. M. Oosterkamp, A. M. Walenkamp, et al. 2014. "Single-agent bevacizumab or lomustine versus a combination of bevacizumab plus lomustine in patients with recurrent glioblastoma (BELOB trial): a randomised controlled phase 2 trial." Lancet Oncol 15(9):943-953., PMID: 25035291

Chamberlain, M. C. and S. K. Johnston. 2010. "Salvage therapy with single agent bevacizumab for recurrent glioblastoma." J Neurooncol 96(2):259-269., PMID: 19593660

Wen, P. Y., D. R. Macdonald, D. A. Reardon, et al. 2010. "Updated response assessment criteria for high-grade gliomas: response assessment in neuro-oncology working group." J Clin Oncol 28(11):1963-1972., PMID: 20231676

Wefel, J. S., T. Cloughesy, J. L. Zazzali, et al. 2011. "Neurocognitive function in patients with recurrent glioblastoma treated with bevacizumab." Neuro Oncol 13(6):660-668., PMID: 21558074

Tabernero J, Vyas M, Giuliani R, Arnold D, Cardoso F, Casali PG, Cervantes A, Eggermont AMM, Eniu A, Jassem J, Pentheroudakis G, Peters S, Rauh S, Zielinski CC, Stahel RA, Voest E, Douillard JY, McGregor K, Ciardiello F. Biosimilars: a position paper of the European Society for Medical Oncology, with particular reference to oncology prescribers. ESMO Open. 2017 Jan 16;1(6):e000142. doi: 10.1136/esmoopen-2016-000142., PMID: 28848668

Lyman GH, Balaban E, Diaz M, Ferris A, Tsao A, Voest E, Zon R, Francisco M, Green S, Sherwood S, Harvey RD, Schilsky RL. American Society of Clinical Oncology Statement: Biosimilars in Oncology. J Clin Oncol. 2018 Apr 20;36(12):1260-1265. doi: 10.1200/JCO.2017.77.4893. Epub 2018 Feb 14., PMID: 29443651

* The medicines, doses, combinations, and schedule in this treatment regimen have been carefully reviewed against international best practice guidelines by specialists in medical oncology around New Zealand and this advice has been accepted for publication by Te Aho o Te Kahu (the Cancer Control Agency). Sometimes medicines that are used in routine clinical practice have not been through a formal review process by the NZ Medicines Regulator Medsafe and are therefore considered unapproved or off-label. These medicines are legally able to be prescribed through sections 25 and 29 of the Medicines Act and by obtaining informed consent from patients. All treatment regimens listed on this website have been through robust peer review and are considered an accepted standard of care, whether prescribed through sections 25 or 29 or carrying formal Medsafe Approval.

s29: This symbol indicates that some formulations of the associated medicine are legally only able to be prescribed under section 29 of the Medicines Act. You can see which formulations are section 29 by hovering over the s29 symbol. You can access full medication details from the New Zealand Formulary by clicking on the medication name. Each clinician retains full responsibility for ensuring they have complied with all relevant obligations and requirements of section 29 including obtaining informed patient consent prior to prescribing the applicable medicine.