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Pro-inflammatory pattern of IgG1 Fc glycosylation in multiple sclerosis cerebrospinal fluid
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نویسنده
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wuhrer m. ,selman m.h.j. ,mcdonnell l.a. ,kümpfel t. ,derfuss t. ,khademi m. ,olsson t. ,hohlfeld r. ,meinl e. ,krumbholz m.
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منبع
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journal of neuroinflammation - 2015 - دوره : 12 - شماره : 1
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چکیده
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Background: immunoglobulin g (igg) effector functions are regulated by the composition of glycans attached to a conserved n-glycosylation site in the fc part. intrathecal production of igg,especially igg1,is a hallmark of multiple sclerosis (ms),but nothing is known about igg fc glycosylation in ms and in cerebrospinal fluid (csf) in general. methods: we applied mass spectrometry of tryptic fc glycopeptides to analyze igg fc glycosylation (sialylation,galactosylation,fucosylation,and bisecting n-acetylglucosamine (glcnac)) in 48 paired csf and serum samples from adult patients with ms or a first demyelinating event highly suggestive of ms (designated as ms cases),and from healthy volunteers and patients with other non-inflammatory diseases (control group). p values were adjusted for multiple testing. results: our experiments revealed four main results. first,igg1 glycosylation patterns were different in csf vs. serum,in the ms group and even in control donors without intrathecal igg synthesis. second,in ms patients vs. controls,igg1 glycosylation patterns were altered in csf,but not in serum. specifically,in csf from the ms group,bisecting glcnac were elevated,and afucosylation and galactosylation were reduced. elevated bisecting glcnac and reduced galactosylation are known to enhance igg effector functions. third,hypothesis-free regression analysis revealed that alterations of afucosylation and bisecting glcnac in csf from ms cases peaked 2-3 months after the last relapse. fourth,csf igg1 glycosylation correlated with the degree of intrathecal igg synthesis and csf cell count. conclusions: the cns compartment as well as the inflammatory milieu in ms affect igg1 fc glycosylation. in ms,the csf igg1 glycosylation has features that enhance fc effector functions. © 2015 wuhrer et al.
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کلیدواژه
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Cerebrospinal fluid; Glycosylation; Immunoglobulin G; Multiple sclerosis
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آدرس
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leiden university medical center,center for proteomics and metabolomics,leiden,netherlands,vu university medical center,department of molecular cell biology and immunology,amsterdam,netherlands,vu university amsterdam,division of bioanalytical chemistry,amsterdam, Netherlands, leiden university medical center,center for proteomics and metabolomics,leiden, Netherlands, leiden university medical center,center for proteomics and metabolomics,leiden, Netherlands, biomedical center (bmc) and university hospital,lmu munich,institute of clinical neuroimmunology,campus martinsried-grosshadern,munich, Germany, university hospital,departments of neurology and biomedicine,basel, Switzerland, karolinska university hospital,department of clinical neuroscience,neuroimmunology unit,stockholm, Sweden, karolinska university hospital,department of clinical neuroscience,neuroimmunology unit,stockholm, Sweden, biomedical center (bmc) and university hospital,lmu munich,institute of clinical neuroimmunology,campus martinsried-grosshadern,munich,germany,munich cluster of systems neurology (synergy),munich, Germany, biomedical center (bmc) and university hospital,lmu munich,institute of clinical neuroimmunology,campus martinsried-grosshadern,munich, Germany, biomedical center (bmc) and university hospital,lmu munich,institute of clinical neuroimmunology,campus martinsried-grosshadern,munich,germany,university of tübingen,department of neurology and stroke,and hertie institute for clinical brain research,tübingen, Germany
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Authors
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