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LL-37

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

Quick Stats
Studies 2230
Trials 95
Score 3
2010 pubmed 395 citations

Selective antimicrobial action is provided by phenol-soluble modulins derived from Staphylococcus epidermidis, a normal resident of the skin.

Cogen. Anna L AL; Yamasaki. Kenshi K; Sanchez. Katheryn M KM; Dorschner. Robert A RA; Lai. Yuping Y; MacLeod. Daniel T DT; Torpey. Justin W JW; Otto. Michael M; Nizet. Victor V; Kim. Judy E JE; Gallo. Richard L RL

Key Findings

  • PSMγ and PSMĪ“ adopt an alpha‑helical structure and strongly interact with lipid membranes, similar to LL‑37
  • Both peptides cause membrane leakage and selectively kill skin pathogens like Staphylococcus aureus while sparing Staphylococcus epidermidis
  • PSMγ and PSMĪ“ synergize with each other and with LL‑37, enhancing antimicrobial activity and reducing Group A Streptococcus on mouse skin

Practical Outcomes

  • These findings suggest that PSMγ and PSMĪ“ could be added to topical skin or wound care products to reinforce natural defenses, especially when combined with LL‑37‑like peptides, offering pathogen‑killing effects without disturbing the beneficial skin microbiome.

Summary

Researchers found that two small proteins (PSMγ and PSMĪ“) made by a harmless skin bacterium act like the human peptide LL‑37: they form helix shapes, stick to cell membranes, and kill bad skin bugs such as Staph aureus while leaving the good bacteria unharmed. They also boost each other's and LL‑37’s antimicrobial power, especially against Group A Strep on mouse skin.

Abstract

Antimicrobial peptides serve as a first line of innate immune defense against invading organisms such as bacteria and viruses. In this study, we hypothesized that peptides produced by a normal microbial resident of human skin, Staphylococcus epidermidis, might also act as an antimicrobial shield and contribute to normal defense at the epidermal interface. We show by circular dichroism and tryptophan spectroscopy that phenol-soluble modulins (PSMs) gamma and delta produced by S. epidermidis have an alpha-helical character and a strong lipid membrane interaction similar to mammalian AMPs such as LL-37. Both PSMs directly induced lipid vesicle leakage and exerted selective antimicrobial action against skin pathogens such as Staphylococcus aureus. PSMs functionally cooperated with each other and LL-37 to enhance antimicrobial action. Moreover, PSMs reduced Group A Streptococcus (GAS) but not the survival of S. epidermidis on mouse skin. Thus, these data suggest that the production of PSMgamma and PSMdelta by S. epidermidis can benefit cutaneous immune defense by selectively inhibiting the survival of skin pathogens while maintaining the normal skin microbiome.

Study Information

Provider

pubmed

Year

2010

DOI

10.1038/jid.2009.243

Citations

395

References

41