Informational only. Not medical advice.INFORMATIONAL PLATFORM ONLY — NOT MEDICAL ADVICE, DIAGNOSIS, OR TREATMENT
Head-to-head comparison of Bronchogen and LL-37 — mechanism, dosing, side effects, legal status, and pricing.
A short synthetic peptide bioregulator (Ala-Asp-Glu-Leu) from the Khavinson family, marketed for bronchial/respiratory tissue support. Evidence is largely Russian-language and preclinical.
LL-37 is the only human cathelicidin antimicrobial peptide — a 37-amino-acid peptide (starting with two leucines) cleaved from the hCAP-18 precursor. It has broad-spectrum antimicrobial activity and immunomodulatory roles, but is also implicated in the pathogenesis of autoimmune and inflammatory skin diseases including psoriasis, rosacea, and lupus. Not FDA-approved; research-use only.
Bronchogen
LL-37
Category
Legal Status
Mechanism
Dose Range
Route
Frequency
Dosing Notes
COA-verified vendors · trust score ≥70 required · single-vial price — bulk/bundle deals may be lower
Bronchogen
LL-37
COA corpus from Disclosed Labs — independently tested batches only.
Bronchogen
9
COAs
99.5%
Avg purity
4
Labs
LL-37
31
COAs
99.2%
Avg purity
8
Labs
Primarily Russian institutional studies; no large independent controlled human trials.
LL-37 was characterized in the mid-1990s as the processed antimicrobial product of hCAP-18 (Gudmundsson et al., 1996). Dürr et al. (2006, Biochim Biophys Acta, PMID 16716248) provided a foundational review of its structure and activity as the sole human cathelicidin. Overhage et al. (2008, Infection and Immunity, PMID 18591225) showed LL-37 prevents Pseudomonas aeruginosa biofilm formation at 0.5 µg/mL — far below its MIC. A randomized, placebo-controlled Phase 1/2 trial (Grönberg et al., 2014, Wound Repair and Regeneration, PMID 25041740) found topical LL-37 safely accelerated healing of hard-to-heal venous leg ulcers at low doses. Its dual role in autoimmunity is well established: Lande et al. (2014, Nature Communications, PMID 25470744) identified LL-37 as a T-cell autoantigen in two-thirds of moderate-to-severe plaque psoriasis patients. No FDA approval exists for any indication. Injectable grey-market protocols for Lyme, biofilm, or mold illness lack controlled clinical evidence and carry theoretical autoimmune risk given LL-37's role in psoriasis, lupus, and rosacea pathogenesis.
Key references
Bronchogen and LL-37 are both in the Immune category and may have overlapping mechanisms. Researchers should review both profiles carefully, understand the mechanisms of action, and monitor the relevant biomarkers when combining compounds in the same class. As always, consult a licensed healthcare provider before making any decisions about combining research compounds.
This platform provides informational tools only, not medical advice. This comparison is for educational purposes only. Consult a licensed provider.
Half-life
Side Effects
Contraindications
Lab Testing