Copenhagen University Hospital, Rigshospitalet
Dept. of Neurology, Danish Multiple Sclerosis Center,

Author Of 1 Presentation

Pathogenesis – the Blood-Brain Barrier Poster Presentation

P0955 - Diffuse inflammation relates to demyelination and clinical parameters in primary (PP) and secondary progressive multiple sclerosis (SP). (ID 1181)

Speakers
Presentation Number
P0955
Presentation Topic
Pathogenesis – the Blood-Brain Barrier

Abstract

Background

In primary progressive MS (PP), brain plaques are smaller and remyelinate better than in secondary progressive MS (SP) yet prognosis and response to systemic immunotherapy in PP is poor.

Objectives

To investigate relations between inflammation and myelin injury in PP vs SP and find correlates of clinical progression.

Methods

Large brain sections from clinically well-described post-mortem cohorts (12 PP, 14 SP and 11 controls) were stained with HE and Luxol-fast blue (myelin). Patients were additionally stained for proteolipid protein and CD68. We measured area loads of total plaque, microglia-rimmed slowly expanding plaque and macrophage-filled filled active plaque (% of WM area). Myelin density in the white matter overall, the normally appearing (NAWM), and the diffusely injured white matter (DIWM) was assessed by densitometry in ImageJ. In white matter compartments, we measured the density and mean size of perivascular mononuclear infiltrates (PMI; #/Cm2). The minimal PMI (grade one) had 3-4 perivascular cell rows and 20-50 cells whereas max. grade six had >19 rows and >500 cells. T- and B-cells in PMI’s were confirmed by CD3 and CD20. EDSS was estimated by chart review in a blinded fashion among 20 patients (10 PP and 12SP) from whom charts were available from two time points including one within three yrs. before death. Among these, we calculated Δ EDSS/yr before death.

In parallel, in-vivo cohorts (26 PP, 26 SP and 24 controls) were analyzed for MRI lesions with/without Gadolinium-enhancement and cerebrospinal fluid (CSF)-biomarkers of demyelination (MBP), axonal damage (NFL) and inflammation.

Results

Densities and sizes of PMI’s in NAWM as well as CSF-markers of inflammation (e.g. IgG-indices, CXCL13, MMP9) were equally increased in PP and SP and equally large PMI’s located to periventricular zones (median gr 1,8 IQR 1,5-2,1). Active and total lesion formation were higher in SP than in PP in both post-mortem and in-vivo cohorts and (post-mortem) juxtacortical and meningeal PMI’s were larger in SP than PP. By contrast, more DIWM-pathology was found in PPMS than in SPMS. The overall myelin density (post-mortem) and NAWM magnetic-transfer-ratio (in-vivo) were equally reduced while MBP and NFL levels in the CSF (in-vivo) were equally increased in both groups.

Plaque-distant (NAWM/DIWM) PMI-density (post-mortem cohort) and CSF-inflammation (in-vivo cohort) correlated with active lesion formation in SP, but not in PP. PMI-density and size in NAWM and in the white matter overall correlated with shorter survival. PMI-density in the white matter overall also correlated with slowly exp. plaque load, which in turn, correlated with Δ EDSS/yr before death in PP and in SP.

Conclusions

Perivascular inflammation is pathogenic and may contribute to white matter demyelination in PP and SP. Inflammatory demyelination in the white matter may not differ greatly but may be more diffuse and less focal in PP compared to SP.

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