Markers for different glial cell responses in multiple sclerosis: clinical and pathological correlations

Petzold, Axel; Eikelenboom, Merijn; Gverić, Djordje; Keir, Geoff; Chapman, Miles D.; Lazeron, R.H.C.; Cuzner, M. L.; Polman, CH; Uitdehaag, Bernard M. J.; Thompson, Edward H.; Giovannoni, Gavin

doi:10.1093/brain/awf165

Cited by 197 publications

(190 citation statements)

References 56 publications

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“…However gliosis is difficult to quantify by immuncytochemical techniques and usually done by counting cells, and the number and length of extending processes. The finding of grey matter astrogliosis and elevated GFAP levels is in line with previous results from human multiple sclerosis post-mortem tissue [6].…”

Section: Discussionsupporting

confidence: 92%

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Quantification of neurodegeneration by measurement of brain-specific proteins

Petzold

Baker

Pryce

et al. 2003

Journal of Neuroimmunology

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Section: Discussionsupporting

confidence: 92%

“…In immunocytochemistry, GFAP has been used as a marker for astrogliosis and S100B for activation of astrocytes, ferritin as a marker for microglial activation and neurofilaments (Nf) as a marker for axonal damage [3][4][5][6]. This study examines the potential of ELISA-based methods to assess neurodegeneration in CREAE.…”

mentioning

confidence: 99%

Quantification of neurodegeneration by measurement of brain-specific proteins

Petzold

Baker

Pryce

et al. 2003

Journal of Neuroimmunology

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“…This protein has been found in CSF of 13 out of 18 patients with MS, whereas it was undetectable in any of the 11 control patients (19). CSF studies have also found that there is a significant trend for increasing S100β levels from primary progressive (PP) to secondary progressive (SP) to relapsing remitting (RR) MS, and that S100β was significantly higher in RR MS than in control patients, demonstrating that S100β is a good marker for the relapsing phase of the disease (20). S100β immunization and S100β-specific T-cell adoptive transfer can induce EAE and uveoretinitis in the Lewis rat, demonstrating that nonmyelin antigens can have an immunopathogenic role in inflammatory CNS disease (21,22).…”

Section: Introductionmentioning

confidence: 96%

Enolase and Arrestin are Novel Nonmyelin Autoantigens in Multiple Sclerosis

et al. 2007

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Introduction-Although myelin autoimmunity is known to be a major factor in the pathogenesis of multiple sclerosis (MS), the role of nonmyelin antigens is less clear. Given the complexity of this disease, it is possible that autoimmunity against nonmyelin antigens also has a pathogenic role. Autoantibodies against enolase and arrestin have previously been reported in MS patients. The Tcell response to these antigens, however, has not been established.

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“…The proven benefit common to all currently recommended treatments is a reduction in the rate of clinical relapse, which has been associated to a transient slowing of disease progression [3]. During the early phase of MS active disease has been related to elevated levels of S100B [4] and the nitric oxide metabolites nitrate and nitrite (NO x ) [5].…”

Section: Introductionmentioning

confidence: 99%

Treatment response in relation to inflammatory and axonal surrogate marker in multiple sclerosis

Petzold

Brassat²,

Más³

et al. 2004

Mult Scler

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Background: This study aimed to investigate if treatment response could retrospectively be related to inflammatory or axonal pathology as measured by plasma surrogate markers. Methods:In this 1-year observational study 30 MS patients with relapsingremitting disease were treated with intra-muscular IFNβ-1a or subcutaneous IFNβ-1b. Responders and non-responders were defined according to clinical and MRI criteria. The control group consisted of 14 healthy subjects. Plasma levels of surrogate markers for inflammation (nitric oxide metabolites (NO x )), astrocytic activation (S100B) and axonal damage (NfH SMI35 ) were measured using standard assays.Results: There were 11 non-responders and 19 responders to IFNβ treatment. Median S100B levels were elevated in a higher proportion of treatment responders (63%, 42.9 pg/mL) compared to non-responders (18%, 11.7 pg/mL, p<0.05, Fisher's exact test) and controls (0%, 2 pg/mL, p< 0.001). Levels of NO x were found to be more frequently elevated in non-responders (72%, 39 µM) compared to healthy controls (0%, 37 µM, p<0.05). Levels of NfH SMI35 were more frequently elevated in responders (58%, 300 pg/mL, p<0.001) and non-responders (72%, 500 pg/mL, p<0.001) compared to controls (0%, 4.5 pg/mL). Conclusion:Patients with relapsing-remitting MS who had surrogate marker supported evidence for astrocytic activation responded more frequently to treatment with IFNβ.

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Markers for different glial cell responses in multiple sclerosis: clinical and pathological correlations

Cited by 197 publications

References 56 publications

Quantification of neurodegeneration by measurement of brain-specific proteins

Quantification of neurodegeneration by measurement of brain-specific proteins

Enolase and Arrestin are Novel Nonmyelin Autoantigens in Multiple Sclerosis

Treatment response in relation to inflammatory and axonal surrogate marker in multiple sclerosis

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