Literature DB >> 18158587

Role of the specifically targeted lysine residues in the glycation dependent loss of chaperone activity of alpha A- and alpha B-crystallins.

Edathara C Abraham1, Jin Huaqian, Atya Aziz, Anbarasu Kumarasamy, Poppy Datta.   

Abstract

Earlier studies have shown significant loss of chaperone activity in alpha-crystallin from diabetic lenses. In vitro glycation studies have suggested that glycation of alpha-crystallin could be the major cause of chaperone activity loss. The following lysine (K) residues in alpha-crystallin have been identified as the major glycation sites: K11, K78, and K166 in alpha A-crystallin and K90, K92, and K166 in alpha B-crystallin. The present study was aimed to assess the contribution of each of the above glycation site in the overall glycation and loss of chaperone activity by mutating them to threonine followed by in vitro glycation with fructose. Level of glycated protein (GP) was determined by phenylboronate affinity chromatography, advanced glycation end products (AGEs) by direct ELISA using anti-AGE polyclonal antibody, and chaperone activity by using alcohol dehydrogenase as the target protein. K11T, K78, and K166T mutants of alpha A showed 33, 17, and 27% decrease in GP and 32, 18, and 21% decrease in AGEs, respectively, as compared to alpha A-wt. Likewise, K90T, K92T, K90T/K92T, and K166T mutants of alpha B showed 18, 21, 29, and 12% decrease in GP and 22, 24, 32, and 16% decrease in AGEs, respectively. Chaperone activity also showed concomitant increase with decreasing glycation and AGEs formation. alpha A-K11T and alpha B-K90T/K92T mutants showed the largest decrease in glycation and increase in chaperone activity.

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Year:  2007        PMID: 18158587     DOI: 10.1007/s11010-007-9685-1

Source DB:  PubMed          Journal:  Mol Cell Biochem        ISSN: 0300-8177            Impact factor:   3.396


  21 in total

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2.  Lens protein composition, glycation and high molecular weight aggregation in aging rats.

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4.  Site selectivity in the glycation of alpha A- and alpha B-crystallins by glucose.

Authors:  E C Abraham; M Cherian; J B Smith
Journal:  Biochem Biophys Res Commun       Date:  1994-06-30       Impact factor: 3.575

5.  Advanced glycation end products in human senile and diabetic cataractous lenses.

Authors:  S Zarina; H R Zhao; E C Abraham
Journal:  Mol Cell Biochem       Date:  2000-07       Impact factor: 3.396

Review 6.  Nonenzymatic glycosylation and the pathogenesis of diabetic complications.

Authors:  M Brownlee; H Vlassara; A Cerami
Journal:  Ann Intern Med       Date:  1984-10       Impact factor: 25.391

7.  Diabetes affects alpha-crystallin chaperone function.

Authors:  M Cherian; E C Abraham
Journal:  Biochem Biophys Res Commun       Date:  1995-07-06       Impact factor: 3.575

8.  Thermally induced disintegration of the oligomeric structure of alphaB-crystallin mutant F28S is associated with diminished chaperone activity.

Authors:  Patrick B Kelley; Edathara C Abraham
Journal:  Mol Cell Biochem       Date:  2003-10       Impact factor: 3.396

9.  Progressive changes in lens crystallin glycation and high-molecular-weight aggregate formation leading to cataract development in streptozotocin-diabetic rats.

Authors:  R E Perry; M S Swamy; E C Abraham
Journal:  Exp Eye Res       Date:  1987-02       Impact factor: 3.467

10.  Diabetic cataract formation: potential role of glycosylation of lens crystallins.

Authors:  V J Stevens; C A Rouzer; V M Monnier; A Cerami
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  9 in total

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5.  Transcriptional regulation of crystallin, redox, and apoptotic genes by C-Phycocyanin in the selenite-induced cataractogenic rat model.

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6.  Glycation of nail proteins: from basic biochemical findings to a representative marker for diabetic glycation-associated target organ damage.

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7.  Comparison of modification sites in glycated crystallin in vitro and in vivo.

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Journal:  Anal Bioanal Chem       Date:  2015-01-31       Impact factor: 4.142

8.  Rapid Non-Enzymatic Glycation of the Insulin Receptor under Hyperglycemic Conditions Inhibits Insulin Binding In Vitro: Implications for Insulin Resistance.

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  9 in total

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