Aberrant Complement Activation Is Associated With Structural Brain Damage in Multiple Sclerosis.

Oechtering, Johanna; Schaedelin, Sabine Anna; Stein, Kerstin; Maleska Maceski, Aleksandra; Melie-Garcia, Lester; Benkert, Pascal; Cagol, Alessandro; Leber, Selina; Galbusera, Riccardo; Ruberte, Esther; Hu, Wayne; Qureshi, Ferhan; Orleth, Annette; Demuth, Lilian; Willemse, Eline; Heijnen, Ingmar; Regeniter, Axel; Derfuss, Tobias J; Fischer-Barnicol, Bettina; Achtnichts, Lutz; Mueller, Stefanie; Hoepner, Robert; Lalive, Patrice H; Bridel, Claire; D'Souza, Marcus; Pot, Caroline; Du Pasquier, Renaud A; Gobbi, Claudio; Zecca, Chiara; Wiendl, Heinz; Lieb, Johanna Maria; Lamers, Christina; Kappos, Ludwig; Trendelenburg, Marten; Leppert, David; Granziera, Cristina; Kuhle, Jens; Lünemann, Jan D

doi:10.48620/84984

Publication:
Aberrant Complement Activation Is Associated With Structural Brain Damage in Multiple Sclerosis.

cris.virtualsource.author-orcid	6770ee83-2853-4648-8b9b-9469f8398d22
cris.virtualsource.author-orcid	e13a21b6-1a9c-4a7b-9578-6c695a51c8c0
cris.virtualsource.author-orcid	5fa79f62-a4e6-411a-9284-5239eedad67e
datacite.rights	open.access
dc.contributor.author	Oechtering, Johanna
dc.contributor.author	Schaedelin, Sabine Anna
dc.contributor.author	Stein, Kerstin
dc.contributor.author	Maleska Maceski, Aleksandra
dc.contributor.author	Melie-Garcia, Lester
dc.contributor.author	Benkert, Pascal
dc.contributor.author	Cagol, Alessandro
dc.contributor.author	Leber, Selina
dc.contributor.author	Galbusera, Riccardo
dc.contributor.author	Ruberte, Esther
dc.contributor.author	Hu, Wayne
dc.contributor.author	Qureshi, Ferhan
dc.contributor.author	Orleth, Annette
dc.contributor.author	Demuth, Lilian
dc.contributor.author	Willemse, Eline
dc.contributor.author	Heijnen, Ingmar
dc.contributor.author	Regeniter, Axel
dc.contributor.author	Derfuss, Tobias J
dc.contributor.author	Fischer-Barnicol, Bettina
dc.contributor.author	Achtnichts, Lutz
dc.contributor.author	Mueller, Stefanie
dc.contributor.author	Hoepner, Robert
dc.contributor.author	Lalive, Patrice H
dc.contributor.author	Bridel, Claire
dc.contributor.author	D'Souza, Marcus
dc.contributor.author	Pot, Caroline
dc.contributor.author	Du Pasquier, Renaud A
dc.contributor.author	Gobbi, Claudio
dc.contributor.author	Zecca, Chiara
dc.contributor.author	Wiendl, Heinz
dc.contributor.author	Lieb, Johanna Maria
dc.contributor.author	Lamers, Christina
dc.contributor.author	Kappos, Ludwig
dc.contributor.author	Trendelenburg, Marten
dc.contributor.author	Leppert, David
dc.contributor.author	Granziera, Cristina
dc.contributor.author	Kuhle, Jens
dc.contributor.author	Lünemann, Jan D
dc.date.accessioned	2025-01-29T09:06:32Z
dc.date.available	2025-01-29T09:06:32Z
dc.date.issued	2025-03
dc.description.abstract	Background And Objectives Levels of activated complement proteins in the CSF are increased in people with multiple sclerosis (MS) and are associated with clinical disease severity. In this study, we determined whether complement activation profiles track with quantitative MRI metrics and liquid biomarkers indicative of disease activity and progression. Methods Complement components and activation products (Factor H and I, C1q, C3, C4, C5, Ba, Bb, C3a, C4a, C5a, and sC5b-9) and liquid biomarkers (neurofilament light chain, glial fibrillary acidic protein [GFAP], CXCL-13, CXCL-9, and IL-12b) were quantified in the CSF of 112 patients with clinically isolated syndromes and 127 patients with MS; longitudinal MRIs according to a standardized protocol of the Swiss MS cohort were assessed. We used multivariable models to analyze associations of the 12 complement parameters as individual independent variables and longitudinal brain volumes, T2-weighted (T2w) lesion volumes, contrast-enhancing (CELs) and paramagnetic rim lesions (PRLs), and molecular biomarkers as dependent variables, respectively. Results Strongest associations with accelerated brain atrophy were found for C4a: doubling of C4a CSF levels was associated with an additional brain volume loss of -0.24% (95% CI -0.31% to -0.16%; p < 0.0001) per year, followed by Ba and C3a (-0.22% [-0.29% to -0.15%]) and -0.13% ([-0.21 to -0.06]; both p < 0.001). Doubling of C3a, Ba, and C4a levels correlated with 2.2- (1.6-3.0; p < 0.0001), 2.0- (1.3-3.1; p = 0.0038), and 1.8-fold (1.2-2.6; p = 0.0029) increased longitudinal T2w lesion volumes; C3a and Ba were associated with 2.5- (1.4-4.6; p = 0.0022) and 3.3-fold (1.5-7.2; p = 0.0024) higher odds for CELs and 2.6- (1.7-4.0; p < 0.0001) and 2.3-fold (1.3-4.3; p = 0.006) increased PRL incidence rates. C1q, C3a, and C4a were associated with higher GFAP levels, and CXCL-13, CXCL-9, and IL-12b analyses showed consistent patterns with strongest associations for C1q, followed by Ba, C3a, and C4a. Discussion Intrathecal complement activation is consistently associated with MRI metrics and liquid biomarkers indicative for MS disease activity and progression. Our results demonstrate that aberrant complement activation is strongly associated with structural brain damage in MS. Therapeutic targeting of the complement system might limit disability accumulation due to MS.
dc.description.numberOfPages	12
dc.description.sponsorship	Clinic of Neurology
dc.identifier.doi	10.48620/84984
dc.identifier.pmid	39752618
dc.identifier.publisherDOI	10.1212/NXI.0000000000200361
dc.identifier.uri	https://boris-portal.unibe.ch/handle/20.500.12422/195321
dc.language.iso	en
dc.publisher	Lippincott, Williams & Wilkins
dc.relation.ispartof	Neurology, Neuroimmunology and Neuroinflammation
dc.relation.issn	2332-7812
dc.subject.ddc	600 - Technology::610 - Medicine & health
dc.title	Aberrant Complement Activation Is Associated With Structural Brain Damage in Multiple Sclerosis.
dc.type	article
dspace.entity.type	Publication
dspace.file.type	text
oaire.citation.issue	2
oaire.citation.startPage	e200361
oaire.citation.volume	12
oairecerif.author.affiliation	Clinic of Neurology
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unibe.description.ispublished	pub
unibe.refereed	true
unibe.subtype.article	journal

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Aberrant Complement Activation Is Associated With Structural Brain Damage in Multiple Sclerosis.