4.3 Article

Interaction of insulin with colloidal ZnS quantum dots functionalized by various surface capping agents

Publisher

ELSEVIER SCIENCE BV
DOI: 10.1016/j.msec.2017.04.018

Keywords

Insulin; Quantum dots; Capping agent; ZnS; Denaturation

Funding

  1. University of Tehran
  2. Center of Excellence in Biothermodynamics (CEBiotherm)
  3. International Scientific Studies & Collaboration (CISSC)-Ministry of Science, Research and Technology in Iran
  4. Iran National Science Foundation (INSF)
  5. Iran National Elites Foundation (INEF)
  6. UNESCO Chair on Interdisciplinary Research in Diabetes at University of Tehran
  7. Iran Society of Biophysical Society

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Interaction of quantum dots (QDs) and proteins strongly influenced by the surface characteristics of the QDs at the protein-QD interface. For a precise control of these surface-related interactions, it is necessary to improve our understanding in this field. In this regard, in the present work, the interaction between the insulin and differently functionalized ZnS quantum dots (QDs) were studied. The ZnS QDs were functionalized with various functional groups of hydroxyl (-OH), carboxyl (-COOH), amine (-NH2), and amino acid (-COOH and-NH2). The effect of surface hydrophobicity was also studied by changing the alkyl-chain lengths of mercaptocarboxylic acid capping agents. The interaction between insulin and the ZnS QDs were investigated by fluorescence quenching, synchronous fluorescence, circular dichroism (CD), and thermal aggregation techniques. The results reveal that among the studied QDs, mercaptosuccinic acid functionalized QDs has the strongest interaction (Delta G degrees = -51.50 kJ/mol at 310 K) with insulin, mercaptoethanol functionalized QDs destabilize insulin by increasing the beta-sheet contents, and only cysteine functionalized QDs improves the insulin stability by increasing the alpha-helix contents of the protein, and. Our results also indicate that by increasing the alkyl-chain length of capping agents, due to an increase in hydrophobicity of the QDs surface, the beta-sheet contents of insulin increase which results in the enhancement of insulin instability. (C) 2017 Elsevier B.V. All rights reserved.

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