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Immunoglobulin can be functionally regulated by protein carboxylmethylation in Fc region.

Authors
Park, JS | Cho, JY | Kim, SS  | Bae, HJ | Han, JW | Lee, HW | Hong, SY
Citation
Archives of pharmacal research, 29(5). : 384-393, 2006
Journal Title
Archives of pharmacal research
ISSN
0253-6269
Abstract
Protein carboxylmethylation methylates the free carboxyl groups in various substrate proteins by protein carboxyl O-methyltransferase (PCMT) and is one of the post-translational modifications. There have been many studies on protein carboxylmethylation. However, the precise functional role in mammalian systems is unclear. In this study, immunoglobulin, a specific form of gamma-globulin, which is a well-known substrate for PCMT, was chosen to investigate the regulatory roles of protein carboxylmethylation in the immune system. It was found that the anti-BSA antibody could be carboxylmethylated via spleen PCMT to a level similar to gamma-globulin. This carboxylmethylation increased the hydrophobicity of the anti-BSA antibody up to 11.4%, and enhanced the antigen-binding activity of this antibody up to 24.6%. In particular, the Fc region showed a higher methyl accepting capacity with 80% of the whole structure level. According to the amino acid sequence alignment, indeed, 7 aspartic acids and 5 glutamic acids, as potential carboxylmethylation sites, were found to be conserved in the Fc portion in the human, mouse and rabbit. The carboxylmethylation of the anti-BSA antibody was reversibly demethylated under a higher pH and long incubation time. Therefore, these results suggest that protein carboxylmethylation may reversibly regulate the antibody-mediated immunological events via the Fc region.
MeSH

PMID
16756083
Appears in Collections:
Journal Papers > School of Medicine / Graduate School of Medicine > Anatomy
Ajou Authors
김, 성수
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