| Literature DB >> 22674551 |
Peggy P Ho1, Jennifer L Kanter, Amanda M Johnson, Hrishikesh K Srinagesh, Eun-Ju Chang, Timothy M Purdy, Keith van Haren, William R Wikoff, Tobias Kind, Mohsen Khademi, Laura Y Matloff, Sirisha Narayana, Eun Mi Hur, Tamsin M Lindstrom, Zhigang He, Oliver Fiehn, Tomas Olsson, Xianlin Han, May H Han, Lawrence Steinman, William H Robinson.
Abstract
Lipids constitute 70% of the myelin sheath, and autoantibodies against lipids may contribute to the demyelination that characterizes multiple sclerosis (MS). We used lipid antigen microarrays and lipid mass spectrometry to identify bona fide lipid targets of the autoimmune response in MS brain, and an animal model of MS to explore the role of the identified lipids in autoimmune demyelination. We found that autoantibodies in MS target a phosphate group in phosphatidylserine and oxidized phosphatidylcholine derivatives. Administration of these lipids ameliorated experimental autoimmune encephalomyelitis by suppressing activation and inducing apoptosis of autoreactive T cells, effects mediated by the lipids' saturated fatty acid side chains. Thus, phospholipids represent a natural anti-inflammatory class of compounds that have potential as therapeutics for MS.Entities:
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Year: 2012 PMID: 22674551 PMCID: PMC3953135 DOI: 10.1126/scitranslmed.3003831
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956