Li J et al. (2018), Novel Natural Angiotensin Converting Enzyme (AC...

ECB-ART-46522

Mar Drugs 2018 Aug 04;168:. doi: 10.3390/md16080271.

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Novel Natural Angiotensin Converting Enzyme (ACE)-Inhibitory Peptides Derived from Sea Cucumber-Modified Hydrolysates by Adding Exogenous Proline and a Study of Their Structure⁻Activity Relationship.

Li J , Liu Z , Zhao Y , Zhu X , Yu R , Dong S , Wu H .

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Natural angiotensin converting enzyme (ACE)-inhibitory peptides, which are derived from marine products, are useful as antihypertensive drugs. Nevertheless, the activities of these natural peptides are relatively low, which limits their applications. The aim of this study was to prepare efficient ACE-inhibitory peptides from sea cucumber-modified hydrolysates by adding exogenous proline according to a facile plastein reaction. When 40% proline (w/w, proline/free amino groups) was added, the modified hydrolysates exhibited higher ACE-inhibitory activity than the original hydrolysates. Among the modified hydrolysates, two novel efficient ACE-inhibitory peptides, which are namely PNVA and PNLG, were purified and identified by a sequential approach combining a sephadex G-15 gel column, reverse-phase high-performance liquid chromatography (RP-HPLC) and matrix-assisted laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOF/MS), before we conducted confirmatory studies with synthetic peptides. The ACE-inhibitory activity assay showed that PNVA and PNLG exhibited lower IC50 values of 8.18 ± 0.24 and 13.16 ± 0.39 μM than their corresponding truncated analogs (NVA and NLG), respectively. Molecular docking showed that PNVA and PNLG formed a larger number of hydrogen bonds with ACE than NVA and NLG, while the proline at the N-terminal of peptides can affect the orientation of the binding site of ACE. The method developed in this study may potentially be applied to prepare efficient ACE-inhibitory peptides, which may play a key role in hypertension management.

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Genes referenced: LOC100887844 LOC100893907 LOC574921 LOC578199 pelp1

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	Figure 1. Effect of different amino acids (A), proline proportions (B) and reaction time (C) on the ACE-inhibitory activity. The values of three replicates are shown as mean ± standard deviation. Different lowercase letters indicate significantly different values (p < 0.05).
	Figure 2. Isolation and purification of modified ACE-inhibitory peptides using a Sephadex G-15 gel column (A) and RP-HPLC (B). The corresponding ACE-inhibitory activities of each fraction are shown in (C,D). Different lowercase letters indicate significantly different values (p < 0.05).
	Figure 3. MALDI-TOF/MS spectra of the amino acid sequences of fraction E3. (A) peptide PNVA. (B) peptide PNLG.
	Figure 4. (A–H) show the binding modes of PNVA, PNLG, NVA and NLG with the ACE, respectively. (B,D,F,H) show 2D schematics of the peptide-binding modes. The dashed lines indicate the hydrogen bonds that were formed between the peptide and residues of the binding sites.
	Figure 5. Schematic illustration of the formation of ACE-inhibitory peptides during the plastein reaction.