| Literature DB >> 35370887 |
Kunio Nakamura1, Oksana Mokliatchouk2, Douglas L Arnold3, Tarek A Yousry4, Ludwig Kappos5, Nancy Richert2, Katherine Ayling-Rouse6, Catherine Miller2, Elizabeth Fisher2.
Abstract
Objective: In the pivotal DEFINE and CONFIRM trials for dimethyl fumarate (DMF), patterns of brain volume changes were different, potentially due to low sample sizes and because MRIs were analyzed at two different reading centers. We evaluated effects of DMF on brain volume change in patients with multiple sclerosis (MS) through reanalysis of pooled images from DEFINE/CONFIRM trials in one reading center.Entities:
Keywords: brain parenchymal fraction; brain volume loss; dimethyl fumarate; multiple sclerosis; pseudoatrophy
Year: 2022 PMID: 35370887 PMCID: PMC8973916 DOI: 10.3389/fneur.2022.809273
Source DB: PubMed Journal: Front Neurol ISSN: 1664-2295 Impact factor: 4.003
Key baseline demographics and disease characteristics.
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| Age, mean ± SD, years | 37.5 ± 9.1 | 38.1 ± 9.0 |
| Female, n (%) | 228 (73) | 217 (72) |
| McDonald criteria, n (%) | ||
| 1 criterion | 268 (85) | 248 (82) |
| 2–4 criteria | 46 (15) | 53 (18) |
| Time since first MS symptoms, mean (range), years | 8.2 (0–32) | 8.3 (0–42) |
| MS relapses in previous year, mean ± SD | 1.3 ± 0.7 | 1.3 ± 0.7 |
| Prior approved MS treatment, n (%) | 159 (51) | 145 (48) |
| Baseline EDSS score, mean ± SD | 2.5 ± 1.2 | 2.4 ± 1.2 |
| T2 lesion volume, mean ± SD, mm3 | 9,957.6 ± 11,280.3 | 10,785.6 ± 11,398.0 |
| T1-hypointense lesion volume, mean ± SD, mm3 | 2,899.7 ± 4,726.6 | 3,201.3 ± 4,700.4 |
| Number of Gd+ lesions, mean ± SD | 1.9 ± 5.5 | 2.0 ± 5.1 |
BID, twice daily; DMF, dimethyl fumarate; EDSS, Expanded Disability Status Scale; Gd+, gadolinium-enhancing; MS, multiple sclerosis; PBO, placebo.
n = 313.
n = 312.
Figure 1Percentage change in brain parenchymal fraction (BPF) from (A) baseline to week 48 and (B) week 48 to 96 in patients with BPF measurements at baseline and week 48, and at week 48 and week 96, respectively. BID twice daily; DMF, dimethyl fumarate; PBO, placebo.
Figure 2Model-based mean BPF changes from baseline, showing temporal patterns of brain volume changes by treatment in the pooled study populations. Results are obtained from a repeated measures model for change from baseline in BPF. The model includes treatment, study, week, and their two-way and three-way interactions, and is adjusted for the following covariates: region, BPF at baseline, and prior multiple sclerosis treatment (yes, no). The model has unstructured variance-covariance structure. BPF, brain parenchymal fraction; BID, twice daily; DMF, dimethyl fumarate; PBO, placebo.
Correlations between percentage change from baseline in brain parenchymal fraction and percentage brain volume change from baseline for each study time point, by study.
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| Week 24 | 0.601 ( | 0.361 ( |
| Week 48 | 0.597 ( | 0.523 ( |
| Week 96 | 0.533 ( | 0.483 ( |
All p-values < 0.0001.
Figure 3Brain volume changes stratified by disability progression and study using (A) PBVC from original analyses and (B) BPF. Original PBVC values shown are model-based estimates, and 95% CIs are based on the mixed-effect model for repeated measures for baseline to week 96 in patients with and without disability progression in the DEFINE and CONFIRM placebo groups. PBVC, percentage brain volume change; BPF, brain parenchymal fraction.
Model-estimated mean brain volume changes in patients with and without baseline Gd+ lesions.
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| Mean (95% CI) BPF change, baseline to week 48 | −0.00377 | −0.00452 | −0.00114 | −0.00198 |
| Mean (95% CI) BPF change, week 48 to week 96 | −0.00441 | −0.00260 | −0.00253 | −0.00182 |
BID, twice daily; BPF, brain parenchymal fraction; DMF, dimethyl fumarate; Gd+, gadolinium-enhancing.