4.4 Article

Inhibition of copper-mediated aggregation of human γD-crystallin by Schiff bases

Journal

JOURNAL OF BIOLOGICAL INORGANIC CHEMISTRY
Volume 22, Issue 4, Pages 505-517

Publisher

SPRINGER
DOI: 10.1007/s00775-016-1433-0

Keywords

Schiff base; Copper complex; gamma-Crystallin; alpha-Crystallin; Cu2+-induced aggregation inhibition

Funding

  1. Science and Engineering Research Board (SERB) under Department of Science and Technology (DST), Govt. of India [SB/FT/LS-277/2012]
  2. DST, New Delhi, India [SB/FT/ CS-008/2013]
  3. DST

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Protein aggregation, due to the imbalance in the concentration of Cu2+ and Zn2+ ions is found to be allied with various physiological disorders. Copper is known to promote the oxidative damage of beta/gamma-crystallins in aged eye lens and causes their aggregation leading to cataract. Therefore, synthesis of a small-molecule 'chelator' for Cu2+ with complementary antioxidant effect will find potential applications against aggregation of beta/gamma-crystallins. In this paper, we have reported the synthesis of different Schiff bases and studied their Cu2+ complexation ability (using UV-Vis, FT-IR and ESI-MS) and antioxidant activity. Further based on their copper complexation efficiency, Schiff bases were used to inhibit Cu2+-mediated aggregation of recombinant human gamma D-crystallin (HGD) and beta/gamma-crystallins (isolated from cataractous human eye lens). Among these synthesized molecules, compound 8 at a concentration of 100 mu M had shown 95% inhibition of copper (100 mu M)-induced aggregation. Compound 8 also showed a positive cooperative effect at a concentration of 5-15 mu M on the inhibitory activity of human alpha A-crystallin (HAA) during Cu2+-induced aggregation of HGD. It eventually inhibited the aggregation process by additional 20%. However, 50% inhibition of copper-mediated aggregation of beta/gamma-crystallins (isolated from cataractous human eye lens) was recorded by compound 8 (100 mu M). Although the reductive aminated products of the imines showed better antioxidant activity due to their lower copper complexing ability, they were found to be non-effective against Cu2+-mediated aggregation of HGD.

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