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LL-37

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

Quick Stats
Studies 2230
Trials 95
Score 2
2018 pubmed 17 citations

Dermatologic toxicity from novel therapy using antimicrobial peptide LL-37 in melanoma: A detailed examination of the clinicopathologic features.

Dolkar. Tsetan T; Trinidad. Celestine M CM; Nelson. Kelly C KC; Amaria. Rodabe N RN; Nagarajan. Priyadharsini P; Torres-Cabala. Carlos A CA; Ivan. Doina D; Prieto. Victor G VG; Tetzlaff. Michael T MT; Curry. Jonathan L JL; Aung. Phyu P PP

Key Findings

  • LL‑37 intra‑tumoral injections reduced melanoma lesion size in a patient
  • After ~45 days, the patient developed multiple verrucous papules and vesiculo‑bullous lesions
  • Skin lesions resolved within two months after stopping LL‑37 therapy

Practical Outcomes

  • If you’re considering LL‑37 for any off‑label use, watch your skin closely and stop the peptide if any unusual bumps or blisters appear. The potential skin toxicity outweighs the modest tumor‑shrinking benefit for non‑clinical applications.

Summary

A case report shows that injecting the immune‑boosting peptide LL‑37 into melanoma tumors can shrink the cancer but may cause serious skin problems like wart‑like bumps and blistering after about a month and a half. The skin issues went away once the injections stopped.

Abstract

LL-37 is a naturally occurring 37-amino-acid peptide that is part of the innate immune system in human skin. Preclinical studies have showed that intra-tumoral injections of LL-37 stimulate the innate immune system by activation of plasmacytoid dendritic cells, which mediate tumor destruction. LL-37 intra-tumoral injections have been utilized in a phase 1 clinical trial for melanoma patients with cutaneous metastases. We report dermatologic toxicity in a 63-year-old woman with stage IIIC melanoma of the right calf and inguinal lymph nodes. She was previously treated with nivolumab and combination chemotherapy (cisplatin, vinblastine and dacarbazine) and subsequently treated with LL-37 injections upon progression of both prior regimens. She received a total of 8 weekly LL-37 injections, with interval clinical shrinkage of injected lesions. However, approximately 45 days after initiation of this therapy, she presented with multiple verrucous papules and a vesiculo-bullous lesion on the trunk and extremities. Clinically, most of these lesions were thought to be either squamous cell carcinoma or inflamed seborrheic keratosis. Histologically, 11 of the total 12 skin biopsies showed similar histopathologic features, with a prominent lichenoid inflammatory infiltrate admixed with eosinophils and an overlying atypical squamous epithelial proliferation with verrucous and keratoacanthoma-like features and varying degrees of keratinocytic atypia. Interestingly, a majority of the lesions did not show spongiosis (11/12). All lesions resolved within 2 months of cessation of LL-37 injection therapy. This case highlights adverse dermatological manifestations of LL-37 therapy, similar to the consequences of other novel therapies.

Study Information

Provider

pubmed

Year

2018

Date

2018-05-16T00:00:00.000Z

DOI

10.1111/cup.13262

Citations

17

References

18