4.4 Article

Chondroitin sulfate N-acetylgalactosyltransferase-1 knockout shows milder phenotype in experimental autoimmune encephalomyelitis than in wild type

GLYCOBIOLOGY (2021)

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Journal

GLYCOBIOLOGY
Volume 31, Issue 3, Pages 260-265

Publisher

OXFORD UNIV PRESS INC
DOI: 10.1093/glycob/cwaa072

Keywords

chondroitin sulfate; experimental autoimmune encephalomyelitis; glycosaminoglycan; multiple sclerosis; N-acetylgalactosaminyltransferase-1

Categories

Biochemistry & Molecular Biology

Funding

  1. Ministry of Health, Labor, and Welfare of Japan
  2. MEXT (Ministry of Education, Sciences, Culture, Sports, and Technology) [24110518, 26110721]
  3. KAKENHI from JSPS (Japan Society for Promoting Sciences) [18H04013, 18H04670]
  4. AMED-CREST from AMED of Japan (Japan Agency for Medical Research and Development) [19gm1210007s0101]
  5. Grants-in-Aid for Scientific Research [18H04670, 18H04013] Funding Source: KAKEN

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Proteoglycans, including chondroitin sulfate (CS) and keratin sulfate (KS), have been found to inhibit axon regeneration. However, the influence of these glycosaminoglycans (GAGs) on the pathogenicity of neuroimmunological diseases is still unclear. Studies on mice lacking certain enzymes for CS synthesis suggest that CS contributes to the induction phase of experimental autoimmune encephalomyelitis (EAE), with different GAG sugar chains potentially serving as therapeutic targets for diseases like multiple sclerosis.
Proteoglycans (PGs) are one of the main components in the extracellular matrix of the central nervous system. Chondroitin sulfate (CS) is a glycosaminoglycan (GAG), which is composed of major PGs. Similar to keratin sulfate (KS), another GAG, CS inhibits axon regeneration. However, the influence of these GAGs on the pathogenicity of neuroimmunological diseases is unclear. Here, we induced experimental autoimmune encephalomyelitis (EAE) in mice lacking CS N-acetylgalactosaminyltransferase-1 (CSGalNAcT1-KO), an important enzyme for CS synthesis. In our study, CSGalNAcT1-KO mice showed milder EAE symptoms than those in wild-type (WT) mice. The recall response of antigen-specific lymphocytes showed that CSGalNAcT1-KO-derived lymphocytes had a milder cell proliferation response than that in WT-derived lymphocytes. These results suggest that CS contributes toward the induction phase of EAE. We previously performed EAE experiments in GlcNAc-6-O-sulfotransferase KO (GlcNAc6ST-KO) and C6ST1-KO mice, which had reduced KS and reduced CS-C, respectively. EAE in CSGalNAcT1-KO mice was more similar to that in GlcNAc6ST-KO mice than in C6ST1-KO mice. In conclusion, the distinct GAG sugar chains are associated with severe or mild phenotypes of EAE and are therefore potential new therapeutic targets for neuroimmunological diseases, including multiple sclerosis.

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