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This bears repeating and repeating. If you've got multiple sclerosis, which I presume you do because you are reading this, it is paramount to do everything in your power to prevent brain volume loss. The two key elements that have shown to do this in repeated trials: disease modifying medication and exercise (in particular aerobic). Don't let up. - Dave
The effect of MRI inflammatory activity and age on the association of brain volume loss with disability progression: per-quartile subgroup analysis
D. Jeffery1, T. Vollmer2, S. Ritter3, E. Verdun Di Cantogno4, D. Piani Meier4, E.-W. Radue5
1Piedmont Healthcare, Mooresville, NC, 2University of Colorado Denver, Denver, CO, 3Novartis Pharmaceuticals Corporation, East Hanover, NJ, United States, 4Novartis Pharma AG, Basel, Switzerland, 5Medical Image Analysis Centre, University of Basel, Basel, Switzerland
Background: Brain volume loss (BVL) reflects both diffuse and focal damage in relapsing MS and correlates with disability progression. Previously, we reported that the quartile of patients with the highest BVL at month (M) 24 experienced the most disability progression at M24 and M48.
Objective: To investigate whether age and MRI inflammatory activity affects concomitant correlation of BVL with disability progression over 24 months and/or its prognostic value over 48 months in RRMS patients.
Methods: Patients (N=1841) from the pooled phase 3 FREEDOMS/FREEDOMS II core (M24) and extension (M48) studies were categorised (post hoc) into quartiles by total percent BV change (PBVC) from baseline (BL) to M24 as assessed by the SIENA method. Mean annualised PBVC was determined for each quartile. Patients were further stratified into subgroups: age (< />40 y, n=1299) at BL, presence/absence of Gd+ lesions at BL (n=1477), or new/enlarging T2 lesions over 24 months (n=819). The proportion of patients at M24 and M48 with 6M-confirmed disability progression (CDP6) and time to EDSS≥6.0 is reported. Odds ratios (OR) and p-values are derived by logistic regression with Q4 as a reference.
Results: PBVC quartile ranges at M24 were: Q1 (n=455), −13.5% to −1.7%; Q2 (n=458), −1.7% to −0.77%; Q3 (n=467), −0.77% to −0.13%; and Q4 (n=461), −0.13% to +4.34%. Within Q1, patients with MRI activity had higher annual BVL than those without; no difference was seen within the other quartiles, and for age. Across all subgroups patients in Q1 were at higher risk for CDP6 compared to those in Q4 and the difference between Q1 and Q4 was similar regardless of lesion activity (OR range: 1.51-2.45) or age (1.81-2.18) over both M24 and M48. During the same time period, correlation of BVL with time to EDSS≥6 was more pronounced (Q1 vs Q4, OR 2.54-5.45). In patients with/without lesion activity (Q1 vs Q4), OR was 3.77-5.45/2.82-4.26, for age < />40 y, OR was 2.54-2.92/3.69-5.24. P< 0.05 for the majority of the comparisons. Over 48 months, patients >40 y had the highest progression rates across Q1 and Q4 for CDP6 (29% and 19%) and time to EDSS≥6 (23% and 7%). Baseline parameters and other outcomes to be presented.
Conclusion: Regardless of baseline or ongoing measures of disease activity, patients with the highest BVL had the worst disease outcome. Lesion activity and age did not have a major impact on the correlation between BVL and disability progression further supporting the clinical relevance of BVL.
The effect of MRI inflammatory activity and age on the association of brain volume loss with disability progression: per-quartile subgroup analysis
D. Jeffery1, T. Vollmer2, S. Ritter3, E. Verdun Di Cantogno4, D. Piani Meier4, E.-W. Radue5
1Piedmont Healthcare, Mooresville, NC, 2University of Colorado Denver, Denver, CO, 3Novartis Pharmaceuticals Corporation, East Hanover, NJ, United States, 4Novartis Pharma AG, Basel, Switzerland, 5Medical Image Analysis Centre, University of Basel, Basel, Switzerland
Background: Brain volume loss (BVL) reflects both diffuse and focal damage in relapsing MS and correlates with disability progression. Previously, we reported that the quartile of patients with the highest BVL at month (M) 24 experienced the most disability progression at M24 and M48.
Objective: To investigate whether age and MRI inflammatory activity affects concomitant correlation of BVL with disability progression over 24 months and/or its prognostic value over 48 months in RRMS patients.
Methods: Patients (N=1841) from the pooled phase 3 FREEDOMS/FREEDOMS II core (M24) and extension (M48) studies were categorised (post hoc) into quartiles by total percent BV change (PBVC) from baseline (BL) to M24 as assessed by the SIENA method. Mean annualised PBVC was determined for each quartile. Patients were further stratified into subgroups: age (< />40 y, n=1299) at BL, presence/absence of Gd+ lesions at BL (n=1477), or new/enlarging T2 lesions over 24 months (n=819). The proportion of patients at M24 and M48 with 6M-confirmed disability progression (CDP6) and time to EDSS≥6.0 is reported. Odds ratios (OR) and p-values are derived by logistic regression with Q4 as a reference.
Results: PBVC quartile ranges at M24 were: Q1 (n=455), −13.5% to −1.7%; Q2 (n=458), −1.7% to −0.77%; Q3 (n=467), −0.77% to −0.13%; and Q4 (n=461), −0.13% to +4.34%. Within Q1, patients with MRI activity had higher annual BVL than those without; no difference was seen within the other quartiles, and for age. Across all subgroups patients in Q1 were at higher risk for CDP6 compared to those in Q4 and the difference between Q1 and Q4 was similar regardless of lesion activity (OR range: 1.51-2.45) or age (1.81-2.18) over both M24 and M48. During the same time period, correlation of BVL with time to EDSS≥6 was more pronounced (Q1 vs Q4, OR 2.54-5.45). In patients with/without lesion activity (Q1 vs Q4), OR was 3.77-5.45/2.82-4.26, for age < />40 y, OR was 2.54-2.92/3.69-5.24. P< 0.05 for the majority of the comparisons. Over 48 months, patients >40 y had the highest progression rates across Q1 and Q4 for CDP6 (29% and 19%) and time to EDSS≥6 (23% and 7%). Baseline parameters and other outcomes to be presented.
Conclusion: Regardless of baseline or ongoing measures of disease activity, patients with the highest BVL had the worst disease outcome. Lesion activity and age did not have a major impact on the correlation between BVL and disability progression further supporting the clinical relevance of BVL.
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