Immunoglobulin can be functionally regulated by protein carboxylmethylation in Fc region

Sun Park Jong, Youl Cho Jae, Soo Kim Sung, Jin Bae Hyun, Whan Han Jeung, Woo Lee Hyang, Youl Hong Sung

Research output: Contribution to journalArticlepeer-review

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 γ-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 γ-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.

Original languageEnglish
Pages (from-to)384-393
Number of pages10
JournalArchives of Pharmacal Research
Volume29
Issue number5
DOIs
StatePublished - 31 May 2006

Keywords

  • Immunoglobulin
  • Protein carboxyl-O-methyltransferase
  • Protein carboxylmethylation
  • Structure and function

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