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LL-37

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

Quick Stats
Studies 2230
Trials 95
Score 3
2023 pubmed 2 citations

Safety of multiple administrations of spermicidal LL-37 antimicrobial peptide into the mouse female reproductive tract.

Lee. Seung Gee SG; Kiattiburut. Wongsakorn W; Burke Schinkel. Stephanie C SC; Angel. Jonathan J; Tanphaichitr. Nongnuj N

Key Findings

  • Multiple doses of LL‑37 (36 µM, 10Ă— spermicidal dose) caused no histological damage to mouse vagina, cervix, or uterus
  • Mice treated with LL‑37 regained 100% fertility after treatment, matching PBS controls
  • Positive control (nonoxynol‑9 foam) damaged tissues and reduced fertility to 50%

Practical Outcomes

  • LL‑37 looks promising as a safe spermicidal component for multipurpose prevention gels, but more testing in primates and humans is needed before anyone should try it. For now, biohackers can note the dosage and safety window demonstrated in mice, but it isn’t ready for DIY use.

Summary

In mice, giving the antimicrobial peptide LL‑37 into the female reproductive tract several times didn’t hurt the vaginal, cervical or uterine tissue and didn’t affect the ability to get pregnant later, unlike a common spermicide that caused damage. This suggests LL‑37 could be a safe ingredient for a future birth‑control gel, but it’s still only tested in mice.

Abstract

We have previously demonstrated spermicidal activity of LL-37 antimicrobial peptide on mouse/human sperm and its contraceptive effects in female mice. With its microbicidal action against Neisseria gonorrhoeae, LL-37 warrants development into a multipurpose prevention technology (MPT) agent for administering into the female reproductive tract (FRT). However, it is important to verify that multiple administrations of LL-37 do not lead to damage of FRT tissues and/or irreversible loss of fecundity. Herein, we transcervically injected LL-37 (36 µM-10× spermicidal dose) into female mice in estrus in three consecutive estrous cycles. A set of mice were sacrificed for histological assessment of the vagina/cervix/uterus 24 h after the last injection, while the second set were artificially inseminated with sperm from fertile males 1 week afterwards, and then monitored for pregnancy. Mice injected with PBS in parallel were regarded as negative controls, whereas those injected with vaginal contraceptive foam (VCF, available over the counter), containing 12.5% nonoxynol-9, served as positive controls for vaginal epithelium disruption. We demonstrated that the vagina/cervix/uterus remained normal in both LL-37-injected and PBS-injected mice, which also showed 100% resumption of fecundity. In contrast, VCF-injected mice showed histological abnormalities in the vagina/cervix/uterus and only 50% of them resumed fecundity. Similarly, LL-37 multiply administered intravaginally caused no damage to FRT tissues. While our results indicate the safety of multiple treatments of LL-37 in the mouse model, similar studies have to be conducted in non-human primates and then humans. Regardless, our study provides an experimental model for studying in vivo safety of other vaginal MPT/spermicide candidates.

Study Information

Provider

pubmed

Year

2023

Date

2023-06-30T00:00:00.000Z

DOI

10.1093/molehr/gaad023

Citations

2

References

32