Literature DB >> 15908425

Protein L-isoaspartyl methyltransferase catalyzes in vivo racemization of Aspartate-25 in mammalian histone H2B.

Glen W Young1, Sarah A Hoofring, Mark J Mamula, Hester A Doyle, Gerard J Bunick, Yonglin Hu, Dana W Aswad.   

Abstract

Protein L-isoaspartyl methyltransferase (PIMT) has been implicated in the repair or metabolism of proteins containing atypical L-isoaspartyl peptide bonds. The repair hypothesis is supported by previous studies demonstrating in vitro repair of isoaspartyl peptides via formation of a succinimide intermediate. Utilization of this mechanism in vivo predicts that PIMT modification sites should exhibit significant racemization as a side reaction to the main repair pathway. We therefore studied the D/L ratio of aspartic acid at specific sites in histone H2B, a known target of PIMT in vivo. Using H2B from canine brain, we found that Asp25 (the major PIMT target site in H2B) was significantly racemized, exhibiting d/l ratios as high as 0.12, whereas Asp51, a comparison site, exhibited negligible racemization (D/L < or = 0.01). Racemization of Asp25 was independent of animal age over the range of 2-15 years. Using H2B from 2-3-week mouse brain, we found a similar D/L ratio (0.14) at Asp25 in wild type mice, but substantially less racemization (D/L = 0.035) at Asp25 in PIMT-deficient mice. These findings suggest that PIMT functions in the repair, rather than the metabolic turnover, of isoaspartyl proteins in vivo. Because PIMT has numerous substrates in cells, these findings also suggest that D-aspartate may be more common in cellular proteins than hitherto imagined and that its occurrence, in some proteins at least, is independent of animal age.

Entities:  

Keywords:  NASA Discipline Cell Biotechnology; Non-NASA Center

Mesh:

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Year:  2005        PMID: 15908425     DOI: 10.1074/jbc.M503624200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  15 in total

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2.  Comparison of the in vitro and in vivo stability of a succinimide intermediate observed on a therapeutic IgG1 molecule.

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Journal:  MAbs       Date:  2013-04-22       Impact factor: 5.857

3.  Deuteration protects asparagine residues against racemization.

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Journal:  Amino Acids       Date:  2016-05-12       Impact factor: 3.520

Review 4.  Epigenetic histone code and autoimmunity.

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5.  Changes in leukocyte gene expression profiles induced by antineoplastic chemotherapy.

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6.  Localization of D-β-aspartyl residue-containing proteins in various tissues.

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7.  Autoimmunity to isomerized histone H2B in systemic lupus erythematosus.

Authors:  Hester A Doyle; Dana W Aswad; Mark J Mamula
Journal:  Autoimmunity       Date:  2012-12-03       Impact factor: 2.815

8.  The V119I polymorphism in protein L-isoaspartate O-methyltransferase alters the substrate-binding interface.

Authors:  Karen Rutherford; Valerie Daggett
Journal:  Protein Eng Des Sel       Date:  2009-10-03       Impact factor: 1.650

9.  The D-isoAsp-25 variant of histone H2B is highly enriched in active chromatin: potential role in the regulation of gene expression?

Authors:  Zhenxia Qin; Jeff X Zhu; Dana W Aswad
Journal:  Amino Acids       Date:  2015-12-14       Impact factor: 3.520

10.  Brain proteomics supports the role of glutamate metabolism and suggests other metabolic alterations in protein l-isoaspartyl methyltransferase (PIMT)-knockout mice.

Authors:  Hongqian Yang; Jonathan D Lowenson; Steven Clarke; Roman A Zubarev
Journal:  J Proteome Res       Date:  2013-09-10       Impact factor: 4.466

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