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      KCI등재후보

      In silico Analysis of Natural Compounds as Modulators of Type I Collagen

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      https://www.riss.kr/link?id=A102674539

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      다국어 초록 (Multilingual Abstract)

      Collagen plays a vital role in the maintenance of structure and function of a human body. It has been widely applied in various fields including biomedical, cosmeceutical, food, pharmaceutical and tissue engineering. In the present study, the dockin...

      Collagen plays a vital role in the maintenance of structure and function of a human body. It has been widely applied in various fields including biomedical, cosmeceutical, food, pharmaceutical and tissue engineering. In the present study, the docking behaviour of type I collagen with 15 different ligands namely hydroxymethylfurfural, methylglyoxal, methylsyringate, O-methoxyacetophenone, 3-phenyllactic acid, 4- hydroxybenzoic acid, kojic acid, lumichrome, galangin, artoindonesianin F, caffeic acid, 4-coumaric acid, origanol A, thymoquinone and quercetin was evaluated along with their putative binding sites using Discovery Studio Version 3.1. Docking studies and binding free energy calculations revealed that origanol A has maximum interaction energy (-40.48 kcal/mol) and quercetin with the least interaction energy (-15.44 kcal/mol) as compared to the other investigated ligands. Three ligands which are galangin, methylsyringate and origanol A were shown to interact with Asp21 amino acid residue of chain B (type I collagen). Therefore, it is strongly suggested that the outcomes from the present study might provide new insight in understanding these 15 ligands as potential type I collagen modulators for the prevention of collagen associate disorders

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      목차 (Table of Contents)

      • 1. Introduction
      • 2. Materials and methods
      • 2.1. Ligands Preparation
      • 2.2. Target Protein Preparation
      • 2.3. Docking Studies
      • 1. Introduction
      • 2. Materials and methods
      • 2.1. Ligands Preparation
      • 2.2. Target Protein Preparation
      • 2.3. Docking Studies
      • 3. Results and Discussion
      • 4. Conclusion
      • References
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