The pharmacokinetics and pharmacodynamics of busulfan when combined with melphalan as conditioning in adult autologous stem cell transplant recipients

Willcox, Abbey; Wong, Eric; Nath, Christa E.; Janson, Brett; Harrison, Simon; Hoyt, Rosemary; Bajel, Ashish; Shaw, Peter J.; Ritchie, David; Grigg, Andrew

doi:10.1007/s00277-018-3447-x

Cited by 5 publications

(3 citation statements)

References 44 publications

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“…This is particularly of concern in the case of once-daily dosing, where plasma concentrations reached are high and dose modifications are more considerable to correct the desired exposure in only four administered doses. Dividing the first dose into two half doses counteracts this risk and has been used successfully for many years in some centres (77).…”

Section: Getting the First Dose Of Busulfan Right: First Dose Personalizationmentioning

confidence: 99%

Total Body Irradiation Forever? Optimising Chemotherapeutic Options for Irradiation-Free Conditioning for Paediatric Acute Lymphoblastic Leukaemia

et al. 2021

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Total-body irradiation (TBI) based conditioning prior to allogeneic hematopoietic stem cell transplantation (HSCT) is generally regarded as the gold-standard for children >4 years of age with acute lymphoblastic leukaemia (ALL). Retrospective studies in the 1990's suggested better survival with irradiation, confirmed in a small randomised, prospective study in the early 2000's. Most recently, this was reconfirmed by the early results of the large, randomised, international, phase III FORUM study published in 2020. But we know survivors will suffer a multitude of long-term sequelae after TBI, including second malignancies, neurocognitive, endocrine and cardiometabolic effects. The drive to avoid TBI directs us to continue optimising irradiation-free, myeloablative conditioning. In chemotherapy-based conditioning, the dominant myeloablative effect is provided by the alkylating agents, most commonly busulfan or treosulfan. Busulfan with cyclophosphamide is a long-established alternative to TBI-based conditioning in ALL patients. Substituting fludarabine for cyclophosphamide reduces toxicity, but may not be as effective, prompting the addition of a third agent, such as thiotepa, melphalan, and now clofarabine. For busulfan, it's wide pharmacokinetic (PK) variability and narrow therapeutic window is well-known, with widespread use of therapeutic drug monitoring (TDM) to individualise dosing and control the cumulative busulfan exposure. The development of first-dose selection algorithms has helped achieve early, accurate busulfan levels within the targeted therapeutic window. In the future, predictive genetic variants, associated with differing busulfan exposures and toxicities, could be employed to further tailor individualised busulfan-based conditioning for ALL patients. Treosulfan-based conditioning leads to comparable outcomes to busulfan-based conditioning in paediatric ALL, without the need for TDM to date. Future PK evaluation and modelling may optimise therapy and improve outcome. More recently, the addition of clofarabine to busulfan/fludarabine has shown encouraging results when compared to TBI-based regimens. The combination shows activity in ALL as well as AML and deserves further evaluation. Like busulfan, optimization of chemotherapy conditioning may be enhanced by understanding not just the PK of clofarabine, fludarabine, treosulfan and other agents, but also the pharmacodynamics and pharmacogenetics, ideally in the context of a single disease such as ALL.

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Section: Getting the First Dose Of Busulfan Right: First Dose Personalizationmentioning

confidence: 99%

Total Body Irradiation Forever? Optimising Chemotherapeutic Options for Irradiation-Free Conditioning for Paediatric Acute Lymphoblastic Leukaemia

et al. 2021

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“…9 In adult patients, higher target AUCs (i.e., 4,000 or 5,000 µM/min) have been identified with busulfan. 10 Exposure-effects relationships are less described with other cytotoxics or have emerged from monocentric or retrospective studies, thus lowering the level of evidence necessary to use them at bedside. For instance, a maximum plasma drug concentration (C max ) value of 1.4 µg/mL has been proposed as a target peak value in head and neck cancer patients treated with 120-hour cisplatin as continuous infusion; 11 elsewhere, the duration of plasma exposure > 0.05 µM has been proposed as a marker for hematological toxicities with paclitaxel.…”

Section: Mg•minmentioning

confidence: 99%

“…99 Because carboplatin clearance only depends on urinary excretion, both formulas are based upon a simplified mathematical estimation of the renal function of patients before giving the drug with respect to the target AUC. Model-based adaptive dosing has been well documented, too, with high-dose busulfan as conditioning in autologous stem cell transplant recipients, either in adults 10 or in children. 100 Pharmacokinetically guided dosing has been proposed as well with widely prescribed 5-FU, mostly as a means to reduce the toxicities.…”

Section: Developing Smart Delivery Systemsmentioning

confidence: 99%

Towards Rational Cancer Therapeutics: Optimizing Dosing, Delivery, Scheduling, and Combinations

Ferrer

Fanciullino

Milano

et al. 2020

Clin Pharma and Therapeutics

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The current trend to personalize anticancer therapies mostly relies on selecting the best drug or combination of drugs to achieve optimal efficacy in patients. In addition to the comprehensive genetic and molecular knowledge of each tumor before choosing the drugs to be given, there is probably much room left for improvement by further personalizing the very modes by which the drugs are given, once they have been carefully selected. In particular, shifting from standard dosing to tailored dosing should help in maintaining drug exposure levels in the right therapeutic window, thus ensuring that the efficacy/toxicity balance is optimal. This paper covers the current knowledge regarding pharmacokinetic/pharmacodynamic relationships of anticancer agents, from decades‐old cytotoxics to the latest immune checkpoint inhibitors, the most frequent sources for long‐neglected interpatient variability impacting on drug exposure levels, and what could be done to achieve real personalized medicine in oncology such as implementing therapeutic drug monitoring with adaptive dosing strategies or using model‐driven modalities for personalized dosing and scheduling.

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Antineoplastic drugs

Dasgupta¹,

Krasowski²

2020

Therapeutic Drug Monitoring Data

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The pharmacokinetics and pharmacodynamics of busulfan when combined with melphalan as conditioning in adult autologous stem cell transplant recipients

Cited by 5 publications

References 44 publications

Total Body Irradiation Forever? Optimising Chemotherapeutic Options for Irradiation-Free Conditioning for Paediatric Acute Lymphoblastic Leukaemia

Total Body Irradiation Forever? Optimising Chemotherapeutic Options for Irradiation-Free Conditioning for Paediatric Acute Lymphoblastic Leukaemia

Towards Rational Cancer Therapeutics: Optimizing Dosing, Delivery, Scheduling, and Combinations

Antineoplastic drugs

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