Vamorolone trial in Duchenne muscular dystrophy shows dose-related improvement of muscle function

Hoffman, Eric P.; Schwartz, Benjamin D.; Mengle-Gaw, L.; Smith, Edward C.; Castro, Diana; Mah, Jean K.; McDonald, Craig; Kuntz, Nancy L.; Finkel, Richard S.; Guglieri, Michela; Bushby, K.; Tulinius, M.; Nevo, Yoram; Ryan, Monique M.; Webster, Richard; Smith, Andrea L.; Morgenroth, Lauren P.; Arrieta, Adrienne; Shimony, Maya; Siener, Catherine; Jaros, Mark; Shale, Phil; McCall, John M.; Nagaraju, Kanneboyina; Anker, John van den; Conklin, Laurie S.; Cnaan, Avital; Gordish‐Dressman, Heather; Damsker, Jesse M.; Clemens, Paula R.

doi:10.1212/wnl.0000000000008168

Cited by 70 publications

(76 citation statements)

References 31 publications

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“…17 First-in-patient phase 2a clinical trials included a 2-week open-label multipleascending-dose (0.25, 0.75, 2, and 6 mg/kg/day) study in 48 DMD boys (4 to <7 years old, steroid naive; VBP15-002) 16 and a subsequent 24-week extension phase (VBP15-003) at the same doses. 18 The phase 2a studies demonstrated that vamorolone was safe at all doses tested, with decreased steroid-associated safety concerns predicted by biomarker studies. Both doseresponsive improvements in clinical outcomes (eg, time to stand from supine velocity and 6-minute walk test, etc.)…”

Section: Vamorolonementioning

confidence: 97%

“…and decreases in proinflammatory corticosteroidresponsive biomarkers were observed. 16,18 The US Food and Drug Administration (FDA) has a guidance regarding the importance of exploring exposure-response relationships in drug development (https://www.fda.gov/media/71277/download). Although PK provides key data to link drug dosing to blood concentrations, in their guidance the FDA notes, "Far less attention has been paid to establishing the relationship between blood concentrations and pharmacodynamic (PD) responses and possible differences among population subsets in these concentrationresponse (often called PK/PD) relationships."…”

Section: Vamorolonementioning

confidence: 99%

“…Further details for all studies have been published. [16][17][18] A summary of these studies is shown in Table 1.…”

Section: Data Sourcesmentioning

confidence: 99%

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Exposure‐Response Analysis of Vamorolone (VBP15) in Boys With Duchenne Muscular Dystrophy

Conklin

Anker

et al. 2020

The Journal of Clinical Pharma

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Exposure‐response relationships of vamorolone, a novel dissociative steroidal anti‐inflammatory drug, were investigated in clinical trials in boys with Duchenne muscular dystrophy. Variables were clinical outcome measures, Fridericia‐corrected QT (QTcF) duration, and pharmacodynamic (PD) biomarkers. Exposure metrics were area under the plasma concentration time curve (AUC) and maximum plasma concentration (Cmax), with a sigmoid Emax model applied. Significant improvement in clinical efficacy outcomes was observed after 24 weeks of daily dosing. The primary outcome, time to stand from supine velocity, exhibited the highest sensitivity to vamorolone, with the lowest AUC value providing 50% of maximum effect (E50 = 186 ng·h/mL), followed by time to climb 4 stairs (E50 = 478 ng·h/mL), time to run/walk 10 m (E50 = 1220 ng·h/mL), and 6‐minute walk test (E50 = 1770 ng·h/mL). Week 2 changes of proinflammatory PD biomarkers showed exposure‐dependent decreases. The E50 was 260 ng·h/mL for insulin‐like growth factor‐binding protein 2, 1200 ng·h/mL for matrix metalloproteinase 12, 1260 ng·h/mL for lymphotoxin α1/β2, 1340 ng·h/mL for CD23, 1420 ng·h/mL for interleukin‐22‐binding protein, and 1600 ng·h/mL for macrophage‐derived chemokine/C‐C motif chemokine 22. No relationship was found between QTcF interval changes from baseline and Cmax in week 2 or 24. This analysis showed that improvements in clinical efficacy end points in week 24 and PD biomarkers in week 2 were achieved at typical vamorolone exposure of 2 mg/kg daily dose with a median AUC dose of 6 mg/kg (3651 ng·h/mL), corresponding to approximately 95% of maximum effects for most response variables.

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Section: Vamorolonementioning

confidence: 97%

Section: Vamorolonementioning

confidence: 99%

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Exposure‐Response Analysis of Vamorolone (VBP15) in Boys With Duchenne Muscular Dystrophy

Conklin

Anker

et al. 2020

The Journal of Clinical Pharma

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“…These were then used to test the anti‐inflammatory effects of a new drug, vamorolone, in Duchenne muscular dystrophy . Initial dose‐ranging pediatric trials in Duchenne muscular dystrophy studied a 24‐fold dose range (0.25– 6.0 mg/kg/day), in which the serum pharmacodynamics biomarkers helped to establish the likely efficacious doses with only a 2‐week exposure study …”

Section: Use Of Biomarkers As Pd End Pointsmentioning

confidence: 99%

“…36 Initial dose-ranging pediatric trials in Duchenne muscular dystrophy studied a 24-fold dose range (0.25-6.0 mg/kg/day), in which the serum pharmacodynamics biomarkers helped to establish the likely efficacious doses with only a 2-week exposure study. 36,37 Clinical end points, as the primary outcome for determining PD in children, can be problematic when end points in pediatric trials differ from those measured in adult trials; use of different outcome measures has been found to be a risk factor for trial failure in children. 28 PD biomarkers show that a biological response has occurred in an individual who has been exposed to a medical product or an environmental agent.…”

Section: Use Of Biomarkers As Pd End Pointsmentioning

confidence: 99%

Developmental Pharmacodynamics and Modeling in Pediatric Drug Development

Conklin

Hoffman

Anker

2019

The Journal of Clinical Pharma

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Challenges in pediatric drug development include small patient numbers, limited outcomes research, ethical barriers, and sparse biosamples. Increasingly, pediatric drug development is focusing on extrapolation: leveraging knowledge about adult disease and drug responses to inform projections of drug and clinical trial performance in pediatric subpopulations. Pharmacokinetic‐pharmacodynamic (PK‐PD) modeling and extrapolation aim to reduce the numbers of patients and data points needed to establish efficacy. Planning for PK‐PD and biomarker studies should begin early in the adult drug development program. Extrapolation relies on the assumption that both the underlying disease and the mechanism of action of the drug used to treat that disease are similar in adults and pediatric subpopulations. Clearly, developmental changes in PK and PD need to be considered to enhance the quality of PK‐PD modeling and, therefore, increase the success of extrapolation. This article focuses on the influence of differences in PD between adults and pediatric subpopulations that are highly relevant for the use of extrapolation.

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