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LL-37

Cathelicidin, hCAP-18, FALL-39, CAP-18

Quick Stats
Studies 2230
Trials 95
Score 2
2023 pubmed 21 citations

Bactericidal synergism between phage endolysin Ply2660 and cathelicidin LL-37 against vancomycin-resistant Enterococcus faecalis biofilms.

Zhang. Huihui H; Zhang. Xinyuan X; Liang. Siyu S; Wang. Jing J; Zhu. Yao Y; Zhang. Wanjiang W; Liu. Siguo S; Schwarz. Stefan S; Xie. Fang F

Key Findings

  • Ply2660 and LL‑37 together dramatically lower viable E. faecalis counts compared to single treatments
  • The combo breaks down bacterial cell walls and then punches holes in the cell membrane, leading to strong cell lysis
  • It prevents new biofilm formation and can also destroy established biofilms, reducing infection spread in mice

Practical Outcomes

  • While the results are promising, the approach is still experimental and not ready for personal use. It suggests that future antimicrobial therapies might combine phage enzymes with peptides like LL‑37, but more safety and human studies are needed before any DIY protocols can be recommended.

Summary

Scientists found that mixing a virus‑derived enzyme (Ply2660) with a natural human peptide (LL‑37) kills drug‑resistant Enterococcus faecalis bacteria better than either one alone, both in lab dishes and in infected mice.

Abstract

Antibiotic resistance and the ability to form biofilms of Enterococcus faecalis have compromised the choice of therapeutic options, which triggered the search for new therapeutic strategies, such as the use of phage endolysins and antimicrobial peptides. However, few studies have addressed the synergistic relationship between these two promising options. Here, we investigated the combination of the phage endolysin Ply2660 and the antimicrobial peptide LL-37 to target drug-resistant biofilm-producing E. faecalis. In vitro bactericidal assays were used to demonstrate the efficacy of the Ply2660-LL-37 combination against E. faecalis. Larger reductions in viable cell counts were observed when Ply2660 and LL-37 were applied together than after individual treatment with either substance. Transmission electron microscopy revealed that the Ply2660-LL-37 combination could lead to severe cell lysis of E. faecalis. The mode of action of the Ply2660-LL-37 combination against E. faecalis was that Ply2660 degrades cell wall peptidoglycan, and subsequently, LL-37 destroys the cytoplasmic membrane. Furthermore, Ply2660 and LL-37 act synergistically to inhibit the biofilm formation of E. faecalis. The Ply2660-LL-37 combination also showed a synergistic effect for the treatment of established biofilm, as biofilm killing with this combination was superior to each substance alone. In a murine peritoneal septicemia model, the Ply2660-LL-37 combination distinctly suppressed the dissemination of E. faecalis isolates and attenuated organ injury, being more effective than each treatment alone. Altogether, our findings indicate that the combination of a phage endolysin and an antimicrobial peptide may be a potential antimicrobial strategy for combating E. faecalis.

Study Information

Provider

pubmed

Year

2023

Date

2023-04-06T00:00:00.000Z

DOI

10.1038/s41522-023-00385-5

Citations

21

References

75