Background

Risk factors previously identified for worse outcomes with SARS-CoV-2 infections include older age, male sex and specific comorbid conditions. An increased risk for poorer COVID-19 outcomes in people with multiple sclerosis (MS) are similar to the general population, but less is known about outcomes in minority groups with MS.

Objectives

To evaluate differences in outcomes of SARS-CoV-2 infection in non-Hispanic White and Black persons with multiple sclerosis.

Methods

COViMS is a North American registry for health care providers to report persons with MS who are infected with SARS-CoV-2, the virus that causes COVID-19 (cases). Cases are reported after 7 days and when the outcome of infection is reasonably certain. MS and clinically isolated syndrome cases were categorized using the Center for Disease Control and Prevention races (non-Hispanic Whites, and Black). Comorbidities related to COVID-19 outcomes were collected. Clinical outcomes examined were mortality alone, mortality and/or admissions to the intensive care unit (ICU) and mortality, ICU admissions and/or hospitalization. Age-adjusted mortality rates as of August 3, 2020 and 95% confidence intervals (CI) were calculated. Multivariable logistic regression was used to assess adjusted differences between races using odds ratios (OR) and 95% CIs. Covariates included sex, age, smoking (current, past, never), MS clinical course (relapsing, progressive), disease duration, ambulation (fully ambulatory, walks with assistance, non-ambulatory), individual comorbidities (cardiovascular disease, cerebrovascular disease, chronic kidney disease, chronic lung disease, diabetes, hypertension, morbid obesity), and disease modifying therapy use (yes vs no).

Results

Of 734 patients reported, 421 (57.4%) Whites, and 194 (26.5%) Black patients were reported. Black cases were more likely to be younger (p=0.002), never smokers (p=0.002), have shorter MS duration (p<0.001), a relapsing MS course (p=0.03) and have comorbidities (p<0.001) compared to Whites. A higher proportion of Black patients had hypertension (40.2% vs 19.5%, p<0.001), and morbid obesity (17.0% vs 9.5%, p=0.007). Mortality rates increased with age and were not statistically different between Whites and Blacks (p=0.156). Black race was associated with increased odds of mortality and/or ICU admission (OR 3.8 [95%CI: 1.60, 8.96], p=0.002) and mortality, ICU admission and/or hospitalization (OR 2.0 [95%CI: 1.14, 3.54], p=0.016) after adjustment for covariates.

Conclusions

Within the COViMS registry, Black MS patients were younger and more likely to have comorbidities than White MS patients. Black MS patients had an increased risk for poorer outcomes compared to Whites even after adjusting for comorbidities at the time of COVID-19.

Background

Background: An improved understanding of the impact of demyelination on multiple sclerosis (MS) related cognitive impairment is crucial for targeting and testing therapies with the potential to slow cognitive decline. Demyelination can be assessed using myelin water imaging, a quantitative magnetic resonance imaging (MRI) technique that measures signal from water in the myelin bilayers, providing a specific measure of myelin (myelin water fraction, MWF).

Objectives

Objective: To determine if there is an anatomical-functional relationship between myelin content and location with cognitive performance.

Methods

Methods: 76 MS participants (mean (SD) age:50.4y(10.6y), 51F) underwent T2 relaxation imaging to calculate MWF maps and cognitive testing (Symbol Digit Modalities Test (SDMT); Selective Reminding Test (SRT); Controlled Oral Word Association Test (COWAT); Brief Visuospatial Memory Test-Revised (BVMT-R)). Nonparametric permutation testing with FSL Randomise was used to determine which white matter (WM) MWF voxels were associated with cognitive test performance for each test (p<0.01, after multiple comparisons correction), creating test-specific maps of associated WM areas. Pearson ́s correlations assessed relationships between mean MWF in the cognitive test-specific WM areas and respective test scores. MS patients were categorized into cognitively impaired, mildly impaired and cognitively preserved groups based on published norms. Kruskal Wallis ANOVA with post hoc pairwise comparisons investigated mean MWF differences between cognitive groups.

Results

Results: MWF in several WM areas was significantly associated with SDMT, SRT and BVMT-R scores but not the COWAT. All tests found voxels within the corona radiata, posterior thalamic radiation and parts of the corpus callosum significant. Unique WM areas were the inferior longitudinal fasciculus and anterior cingulum for SDMT and the retrolenticular part of the internal capsule for the BVMT-R. Mean MWF in the test-specific WM areas correlated significantly with performance on the SDMT (r=0.58, p= 4.11 x 10^-8), SRT (r=0.56, p= 4.14 x 10^-7) and BVMT-R (r=0.56, p= 1.0 x 10^-6). Mean MWF in the test-specific WM areas was significantly lower in the cognitively impaired group relative to the cognitively preserved group (p<0.01).

Conclusions

Conclusions: There is an anatomical-functional relationship between myelin damage and cognitive performance in MS with unique WM patterns for different cognitive domains.

Background

Emergence of SARS CoV-2 causing COVID-19 provoked the need to gather information on the overall outcomes and potential risks associated with morbidity and mortality in multiple sclerosis (MS) patients with COVID-19 infections. The COViMS registry was initiated as a rapid and efficient means to collect this data from North American health care providers.

Objectives

To describe the spectrum of outcomes in SARS CoV-2 infected North American MS patients and to ascertain characteristics associated with severe COVID-19 outcomes.

Methods

The COViMS registry requested that MS, neuromyelitis optica (NMO), myelin oligodendrocyte glycoprotein antibody disease (MOGAD), and radiographically isolated syndrome (RIS) patients with SARS-CoV-2 infection be reported after the outcome was reasonably certain. Data were de-identified and cross-sectional. Effort was made to harmonize with other international registries for COVID-19. Poor clinical outcomes assessed were: mortality, mortality and/or admission to the intensive care unit (ICU), and mortality, ICU admission and/or hospitalization. Associations between patient characteristics and these outcomes were evaluated using multivariable logistic regression. Covariates included sex, age, race, smoking, MS clinical course (relapsing, progressive), MS disease duration, ambulation (fully ambulatory, walks with assistance, non-ambulatory), individual comorbidities (cardiovascular disease, cerebrovascular disease, chronic kidney disease, chronic lung disease, diabetes, hypertension, morbid obesity), and disease modifying therapy (DMT) use.

Results

As of Aug 3, 2020, 764 patients from over 140 different practices were reported; 734 MS, 21 NMO, 4 MOGAD, and 5 RIS. MS patients were 73.4% female (73.4%), 65.2% Caucasian, with mean (SD) age of 48.2 (±13.5) years. Mean disease duration was 13.8 (±9.9) years. 70.9% were fully ambulatory. Ocrelizumab and dimethyl fumarate (DMF) were the top two DMTs used. Most (77.1%) were laboratory confirmed for SARS-CoV-2. Of MS cases, 6.1% died, 13.8% were admitted to the ICU and/or died, and 31.2% were either hospitalized, admitted to the ICU or died. Older age, non-ambulatory status and cardiovascular disease were associated with increased risk of poor outcomes. No specific DMT was associated with increased odds of mortality and mortality and/or ICU admission. Anti-CD20 DMT use showed an increased odds of mortality, ICU admission and/or hospitalization compared to DMF (OR: 2.53 95%CI [1.17, 5.50]).

Conclusions

The data provide reassurance that the MS registry population aligns with reported COVID-19 outcomes in the general North American population. While reported deaths are few, no clear association between a specific therapy and mortality has been seen after adjustment for age, sex, ambulatory status and comorbidities. Data collection continues.

Background

Susac’s Syndrome (SuS) is a rare autoimmune endotheliopathy of the brain, retina and cochlea that mimics multiple sclerosis (MS). Lesions presumed to be microinfarcts classically involve the corpus callosum (CC). While one brain biopsy reported demyelination, and MRI studies have shown reduced fractional anisotropy in the CC, the specific processes underlying SuS pathology are not yet clear. Myelin water imaging (MWI) and diffusion basis spectrum imaging (DBSI) can provide information about microstructural changes occurring in SuS. MWI provides a quantitative measurement of myelin, termed the myelin water fraction (MWF). DBSI yields various physiologically relevant metrics characterized by water diffusion: the apparent diffusion coefficient (ADC) which relates to overall tissue damage; fractional anisotropy (FA), which decreases with white matter (WM) damage; and radial diffusivity (RD) which increases with myelin loss.

Objectives

Determine in vivo WM microstructural changes in Susac Syndrome compared to MS and healthy controls (HC) using MWI and DBSI.

Methods

Participants included 7 SuS patients following the proposed European Susac Consortium diagnostic criteria (mean age 43.3y (30-78y), 6F), 10 MS patients (mean age 43.2y (26-70y), 9F) and 10 HC (MWI: 44y (27-64y), 9F, DBSI: 35.9y (22-47y), 5F). 3T MRI included MWI (48-echo 3D GRASE sequence), DBSI (9 b-values, 0-1500 s/mm², 99 directions) and a 3DT1 for anatomical reference. The CC and global WM (non-lesional tissue) were segmented and registered using FSL and the JHU atlas. One-way ANOVA with Tukey correction compared CC and global WM between groups.

Results

CC: SuS MWF (0.09±0.01) was lower than MS (0.11±0.02, p=0.03) and trending lower than HC (0.11±0.02, p=0.07). SuS ADC (0.84 ± 0.08 x 10^-3μm²/ms) was higher than MS (0.73±0.04 x 10^-3μm²/ms, p<0.001) and controls (0.71±0.04 x 10^-3μm²/ms, p<0.001). SuS FA (0.82±0.02) was lower than HC (0.86±0.02, p= 0.02). SuS RD was higher (0.27±0.03 x 10^-3μm²/ms) than HC (0.21±0.01 x 10^-3μm²/ms, p=0.004) and trending higher than MS (0.23±0.05 x 10^-3μm²/ms, p=0.05).

Global WM: ADC and RD findings in the Global WM were similar to CC, i.e. ADC and RD were significantly higher in SuS compared to MS and HC (all p<=0.03). However, MWF and FA was insignificantly different between the groups.

Conclusions

We report the first use of MWI in SuS. Both CC and the global WM showed non-lesional myelin damage, which was more severe than MS.

Background

Standardized magnetic resonance imaging (MRI) protocols are important for the diagnosis and monitoring of patients with multiple sclerosis (MS). The Consortium of Multiple Sclerosis Centers (CMSC) convened an international panel of MRI experts to review and update the current guidelines.

Objectives

The goal is to update the standardized MRI protocol and clinical guidelines for diagnosis and follow-up of MS and develop strategies for advocacy, dissemination and implementation.

Methods

The CMSC convened an expert panel in October 2019 to update the standardized MRI protocol. Conference attendees included neurologists, radiologists, magnetic resonance technologists, and imaging scientists with expertise in MS. Representatives from CMSC, Magnetic Resonance Imaging in MS (MAGNIMS), North American Imaging in Multiple Sclerosis Cooperative, National MS Society, Multiple Sclerosis Association of America, MRI manufacturers, and commercial image analysis companies were present. Before the meeting, CMSC members were surveyed about standardized MRI protocol, gadolinium, diffusion weighted imaging, and the central vein sign.

Results

95 neurologists completed the survey. 34% use the CMSC protocol. 48% use a standardized MRI protocol but are uncertain if it is similar to CMSC guidelines. 51% continue to use gadolinium for routine imaging. 58% wanted the central vein sign to be included in the diagnostic work up of MS. 87% were interested in monitoring brain volume and 10% were doing it routinely. The panel worked to harmonize CMSC and MAGNIMS MRI protocols so the updated guidelines could ultimately be accepted by international consensus. Advocacy efforts will promote the importance of standardized MRI protocols. Dissemination will include publications, meeting abstracts, educational programming, webinars, “meet the expert” teleconferences and exam cards. Implementation will require comprehensive and coordinated efforts to make the protocol easy to access and use.

Conclusions

The international expert group developed revised clinical MRI guidelines with the vision and action plans for them to be universally useful and useable and become the standard of care for patients with MS.

Background

North American Registry for Care and Research in Multiple Sclerosis (NARCRMS) is a longitudinal registry studying the course of MS in the disease-modifying era.

Objectives

To examine motor performance metrics of upper and lower extremity function in NARCRMS participants at enrollment, using the Expanded Disability Status Scale (EDSS) and 25-foot walk times.

Methods

Recruitment began in 2016 and by June 24, 2020, 737 patients were enrolled at 25 MS sites across the US and Canada. People with any sub type of MS within 15 years of disease onset and an EDSS of up to 6.5 are eligible for enrollment. Various clinical metrics are collected including motor performance for upper and lower extremities. Our initial observations about EDSS, 25-foot timed walk and the 9-hole peg test are reported below

Results

EDSS and 25-foot walk times were available in 632 patients and upper extremity function in 609 patients. A mean walking speed of 4.96 seconds was recorded in patients with an EDSS of 0 (n=105). 5.11 was the mean speed until an EDSS of 3.0 (n=39) where a mean speed of 5.41 seconds was recorded. Walking truly became affected at an EDSS of 3.5 (n=27) where a mean speed of 6.48 seconds was recorded. Thereafter mean speed progressively declined at every EDSS increase. For an EDSS of 4.0 (n=28), mean speed was 7.78 seconds; for an EDSS of 4.5 (n=6), mean speed was 9.16 seconds and continued to increase until an EDSS of 6.5 (n=11) where mean speed was 19.1 seconds. For the 9-hole peg test, patients with an EDSS of 0 (n=101) had a mean speed of 20.3 seconds in the dominant and 21 seconds in the non-dominant hand. Hand function remained unimpaired until an EDSS of 2.0 and significant slowing occurred in patients with EDSS ranging from 2.5 to 6.5. For an EDSS of 2.5 (n=44), mean speed was 25.3 seconds in the dominant and 24.4 seconds in the non-dominant hand. For an EDSS of 4.0 (n=26), mean speed was 26.3 seconds in the dominant and 26.0 seconds in the non-dominant hand. For an EDSS of 6.5 (n=11), hand function had declined to a mean speed of 40.1 seconds for the dominant and 56.4 seconds for the non-dominant hand.

Conclusions

A linear correlation of the 25-foot walk speed to EDSS increases was remarkable, reiterating the commonly held belief that the EDSS is a “walking scale”. Decline in hand function at an EDSS of 2.5 was unexpected since hands are often perceived to be unaffected early in MS and seldom observed as impaired by patients. Progressive decline of hand function at every EDSS increase would suggest that the 9-HP test is a good marker of declining hand function and should be included in clinical monitoring of patients.