Amino Acids 2015-12-01

Tyrosine- and tryptophan-coated gold nanoparticles inhibit amyloid aggregation of insulin.

Kriti Dubey, Bibin G Anand, Rahul Badhwar, Ganesh Bagler, P N Navya, Hemant Kumar Daima, Karunakar Kar

Index: Amino Acids 47 , 2551-60, (2015)

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Abstract

Here, we have strategically synthesized stable gold (AuNPs(Tyr), AuNPs(Trp)) and silver (AgNPs(Tyr)) nanoparticles which are surface functionalized with either tyrosine or tryptophan residues and have examined their potential to inhibit amyloid aggregation of insulin. Inhibition of both spontaneous and seed-induced aggregation of insulin was observed in the presence of AuNPs(Tyr), AgNPs(Tyr), and AuNPs(Trp) nanoparticles. These nanoparticles also triggered the disassembly of insulin amyloid fibrils. Surface functionalization of amino acids appears to be important for the inhibition effect since isolated tryptophan and tyrosine molecules did not prevent insulin aggregation. Bioinformatics analysis predicts involvement of tyrosine in H-bonding interactions mediated by its C=O, -NH2, and aromatic moiety. These results offer significant opportunities for developing nanoparticle-based therapeutics against diseases related to protein aggregation.


Related Compounds

  • L(-)-Tryptophan
  • Sodium hydroxide
  • Potassium hydroxid...
  • Silver nitrate
  • 3-Ethyl-2,4-pentan...
  • acetic acid
  • L-Tyrosine
  • acetic acid
  • Thioflavine T
  • Stanolone

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