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Evaluating the capability of soybean peptides as calcium ion carriers: a study through sequence analysis and molecular dynamics simulations. | LitMetric

AI Article Synopsis

  • Calcium homeostasis imbalance can lead to chronic diseases, making effective calcium supplements crucial for health.
  • The study focused on identifying peptide calcium chelates from soybean peptides to enhance calcium absorption while minimizing side effects.
  • Two specific peptides (GGDLVS and YEGVIL) were found to exhibit high calcium binding capacity, and the research aimed to clarify how the amino acid positions influence this binding efficiency.

Article Abstract

Calcium homeostasis imbalance in the body can lead to a variety of chronic diseases. Supplement efficiency is essential. Peptide calcium chelate, a fourth-generation calcium supplement, offers easy absorption and minimal side effects. Its effectiveness relies on peptide's calcium binding capacity. However, research on amino acid sequences in peptides with high calcium binding capacity (HCBC) is limited, affecting the efficient identification of such peptides. This study used soybean peptides (SP), separated and purified by gel chromatography, to obtain HCBC peptide (137.45 μg mg) and normal peptide (≤95.78 μg mg). Mass spectrometry identified the sequences of these peptides, and an analysis of the positional distribution of characteristic amino acids followed. Two HCBC peptides with sequences GGDLVS (271.55 μg mg) and YEGVIL (272.54 μg mg) were discovered. Molecular dynamics showed that when either aspartic acid is located near the N-terminal's middle, or glutamic acid is near the end, or in cases of continuous Asp or Glu, the binding speed, probability, and strength between the peptide and calcium ions are superior compared to those at other locations. The study's goal was to clarify how the positions of characteristic amino acids in peptides affect calcium binding, aiding in developing peptide calcium chelates as a novel calcium supplement.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11089645PMC
http://dx.doi.org/10.1039/d4ra02916jDOI Listing

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