Conference Coverage

High BMI and Weight in Young Adulthood Are Linked to Younger Age of MS Symptom Onset


 

Glenn S. Williams

Vitamin D Deficiency Predicts Long-Term Disease Activity in Patients Taking Interferon Beta-1b
Correcting vitamin D deficiency early in the course of treatment with interferon beta-1b is likely to improve the outcome for patients with multiple sclerosis (MS), according to data presented.

“The results of this study support the importance of identifying and correcting 25(OH)D insufficiency early in the course of MS,” said Alberto Ascherio, MD, DrPH, and colleagues. “The effects are likely additive to therapy with interferon beta-1b without decreasing its tolerability.”

Dr. Ascherio, from the Harvard School of Public Health in Boston, and colleagues sought to examine the predictive effect of serum 25(OH)D levels on disease activity and progression in patients with clinically isolated syndrome starting interferon beta-1b therapy. They also examined the effect of serum 25(OH)D levels on the occurrence of flu-like symptoms, a common side-effect of interferon beta-1b.

Drawing their study cohort from the BEtaferon/BEtaseron in Newly Emerging MS for Initial Treatment (BENEFIT) study, the researchers randomized patients with clinically isolated syndrome and two or more clinically silent brain MRI lesions to 250 µg of interferon beta-1b (early treatment) or placebo (late treatment) subcutaneously every other day. Serum 25(OH)D concentration measurements were taken at baseline and at six, 12, and 24 months. Cox proportional hazard models or generalized mixed effects models were used to relate season-adjusted 25(OH)D concentrations to clinical and MRI outcomes up to five years. Occurrence of flu-like symptoms in the early treatment group with high or low serum 25(OH)D levels were compared by χ2 test.

Data from 216 patients in the early treatment group and 118 patients in the delayed treatment group were analyzed. When analyzed as a continuous variable, increases in 25(OH)D led to a lower probability of conversion to McDonald MS, with a trend toward lower probability of conversion to clinically definite MS. Increases in 25(OH)D also led to lower rates of newly active lesions, relapses, annual percent change in T2 volume, and annual percent change in brain volume.

Dichotomous 25(OH)D levels were strongly and inversely associated with probability of conversion to clinically definite MS, cumulative number of new lesions on MRI, percent change in T2 volume, and percent change in brain volume. Occurrence of flu-like symptoms did not differ between patients in the early treatment group with high or low serum 25(OH)D levels at months 6, 12, and 24.

Dr. Ascherio and colleagues concluded that among patients who started interferon beta-1b treatment right after clinically isolated syndrome, incremental increases of 25(OH)D levels were associated with reduction of long-term MS disease activity and severity. “These results also suggest that early treatment with interferon beta-1b has an additive effect with 25(OH)D to reduce disease severity and progression on both clinical and imaging outcomes.”

Further research would be needed, the researchers said, to determine whether these results apply to patients with different MS subtypes or those treated with drugs other than interferon beta-1b.

Glenn S. Williams

Late-Onset MS Largely Involves Relapsing-Remitting Course
Eighty-two percent of patients who present with late-onset multiple sclerosis (MS) have a relapsing-remitting course of their disease, and the others have a progressive illness, researchers reported.

Claudia Chaves, MD, and colleagues retrospectively reviewed the database from the Lahey Hospital and Medical Center’s MS Center in Lexington, Massachusetts, and selected patients with new-onset MS at age 50 and older. The investigators sought to determine the clinical characteristics and imaging features among patients with late-onset MS.

Fifty patients who presented to the clinic had late-onset MS, which was 7% of all patients with MS, according to Dr. Chaves. Forty-one patients (30 women; mean age, 55) had a relapsing-remitting course, and nine patients (seven women; mean age, 53.6) had a progressive illness. Gait problems were present in 80% of patients with relapsing-remitting MS and in all patients with progressive disease. Patients with progressive illness were significantly more likely to have motor deficits and a higher Expanded Disability Status Scale (EDSS) score, compared with those with relapsing-remitting MS.

Patients with progressive illness had higher odds of cognitive impairment and more difficulties with coordination, though the rate was not statistically significant. Patients with relapsing-remitting MS had 2.2 times the odds of having sensory abnormalities. “No statistically significant difference was found for MRI measures between the two groups, including the presence of supra- and infratentorial lesions, spinal cord involvement, contrast enhancement, and cerebral atrophy,” noted the investigators.

However, the odds of infratentorial and spinal cord involvement were higher in those patients with relapsing-remitting MS and those with progressive illness, respectively.” Ninety percent of patients with relapsing-remitting MS had been treated with a disease-modifying agent, and 78% of those with progressive illness were treated with a disease-modifying agent.

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