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Peptide Database

Goals
Fat LossMuscle BuildingInjury HealingAnti-AgingCognitive EnhancementSleep OptimizationImmune SupportGut HealingSkin RejuvenationSexual Health
Peptides
Adipotide
Weight Management
AOD-9604
Weight Management
BPC-157
Healing & Recovery
Cagrilintide
Weight Management
CJC-1295
Growth Hormone
DSIP
Sleep & Recovery
Epithalon
Anti-Aging
GHK-Cu
Anti-Aging
GHRP-2
Growth Hormone
HCG
Hormone Support
Hexarelin
Growth Hormone
HGH
Growth Hormone
IGF-1 LR3
Growth Hormone
Kisspeptin
Hormone Support
Melanotan-2
Cosmetic
MOTS-C
Metabolic
NAD+
Anti-Aging
Oxytocin Acetate
Hormone Support
PEG-MGF
Recovery
PNC-27
Cancer Research
PT-141
Sexual Health
Retatrutide
Weight Management
Selank
Cognitive
Semaglutide
Weight Management
Semax
Cognitive
Sermorelin
Growth Hormone
Snap-8
Cosmetic
SS-31
Mitochondrial
TB-500
Healing & Recovery
Tesamorelin
Growth Hormone
Thymosin Alpha-1
Immune
Tirzepatide
Weight Management
Total Peptides: 32
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Peptide Comparison

Defensin (HBD-2)vsDefensin (HBD-3)

Inducible human beta-defensin antimicrobial peptide (41 amino acids) that kills bacteria through membrane disruption at MIC 50 μg/mL against S. aureus, recruits dendritic cells and T cells via CCR6 receptor chemotaxis, and serves as a critical bridge between innate and adaptive immunity — upregulated up to 100-fold during infection and inflammation

Most potent human beta-defensin (45 amino acids) with unique salt-insensitive antimicrobial activity — kills MRSA at MIC 0.5-1.0 μg/mL regardless of salt concentration, disrupts biofilms at 4-8 μg/mL, and retains full bactericidal function even without its disulfide bonds — representing a next-generation antimicrobial peptide template for combating antibiotic resistance

ImmuneImmune

At a Glance

Quick
comparison

Dose Range

Defensin (HBD-2)

10–100 μg/mL (research)

Defensin (HBD-3)

1–50 μg/mL (research)

Frequency

Defensin (HBD-2)

As needed

Defensin (HBD-3)

As needed

Administration

Defensin (HBD-2)

Topical application (research/wound care)

Defensin (HBD-3)

Topical application (research/wound care)

Cycle Length

Defensin (HBD-2)

Ongoing/indefinite

Defensin (HBD-3)

Ongoing/indefinite

Onset Speed

Defensin (HBD-2)

Rapid (hours to days)

Defensin (HBD-3)

Rapid (hours to days)

Evidence Level

Defensin (HBD-2)

Moderate human trials (Phase 1-2)

Defensin (HBD-3)

Moderate human trials (Phase 1-2)

Efficacy

Benefit
ratings

Defensin (HBD-2)
Defensin (HBD-3)

Healing

Defensin (HBD-2)92%
Defensin (HBD-3)0%

Growth

Defensin (HBD-2)87%
Defensin (HBD-3)0%

Immune

Defensin (HBD-2)85%
Defensin (HBD-3)85%

Technical Data

Compound
specifications

Defensin (HBD-2)

Molecular Formula

Approximately C185H290N54O57S6 (41-amino acid peptide with 3 disulfide bonds)

Molecular Weight

~4,328 Da (mature peptide)

Half-Life

Short plasma half-life (minutes); locally stable at wound and epithelial sites due to disulfide-bonded structure; degraded by metalloproteinases in chronic wound environments

Bioavailability

Topical application provides local antimicrobial activity; three disulfide bonds confer resistance to proteolytic degradation; salt-sensitive — activity reduced above 150 mM NaCl; not intended for oral or systemic delivery

CAS Number

Not assigned (endogenous human peptide; research-grade available from multiple suppliers)

Defensin (HBD-3)

Molecular Formula

Approximately C220H340N64O62S6 (45-amino acid peptide with 3 disulfide bonds)

Molecular Weight

~5,155 Da (mature peptide)

Half-Life

Short systemic half-life (minutes) typical of cationic peptides; disulfide-bonded form provides protease resistance at local tissue sites; linear form shows adequate stability for topical applications

Bioavailability

Topical application achieves high local concentrations; maintains activity in physiological salt environments (unique); linear form retains activity enabling simplified formulation; not intended for oral or systemic delivery

CAS Number

Not assigned (endogenous human peptide; research-grade available from peptide suppliers)

Protocols

Dosing
tiers

Defensin (HBD-2)

starting

10-25 μg/mL topical or research application

Protocol-dependent (typically once or twice daily)

As defined by research protocol

Research-level dosing for in vitro and ex vivo studies. This concentration range is effective against gram-negative bacteria in low-salt conditions. HBD-2 is primarily a research compound — all dosing information reflects preclinical and in vitro experimental conditions rather than established clinical protocols.

standard

25-50 μg/mL topical application

Once or twice daily in research settings

Research protocol-dependent (typically 1-4 weeks)

Effective concentration range for broad-spectrum antimicrobial activity in research wound models. Activity covers gram-negative bacteria, select gram-positive bacteria, and Candida species at these concentrations. Ensure application medium has low ionic strength (<150 mM NaCl) to maintain HBD-2 activity.

advanced

50-100 μg/mL topical application

Once daily in research settings

Research protocol-dependent

Higher concentration for coverage of gram-positive bacteria including S. aureus and for anti-biofilm applications. At these concentrations, HBD-2 provides both direct antimicrobial killing and significant CCR6-mediated immune cell chemotaxis. Research supervision required. Consider combining with salt-insensitive HBD-3 for coverage in physiological salt conditions.

Defensin (HBD-3)

starting

1-5 μg/mL topical or research application

Protocol-dependent

As defined by research protocol

Effective antimicrobial concentration against MRSA at the low end of this range (MIC 0.5-1.0 μg/mL). HBD-3's extraordinary potency means low concentrations are sufficient for gram-positive coverage. All dosing reflects research and preclinical settings — no established clinical protocols exist for exogenous HBD-3 application.

standard

5-15 μg/mL topical application

Once or twice daily in research settings

Research protocol-dependent (typically 1-4 weeks)

Provides broad-spectrum antimicrobial coverage against gram-positive bacteria, gram-negative bacteria, and fungi. Covers MIC requirements for most target pathogens. Effective anti-biofilm activity begins at the higher end of this range. Full activity maintained regardless of wound fluid salt concentration.

advanced

15-50 μg/mL topical application

Once daily in research settings

Research protocol-dependent

Provides robust anti-biofilm activity (MRSA biofilm disruption at 4-8 μg/mL) with significant margin above MICs for all major target pathogens. At these concentrations, combined antimicrobial killing, biofilm disruption, and immune cell chemotaxis are all maximally active. Monitor for any cytotoxicity at the high end — therapeutic window remains wide.

Applications

Best
suited for

Defensin (HBD-2)

Research into novel topical antimicrobial therapies for skin infections and chronic wounds

Defensin (HBD-2) is particularly well-suited for individuals focused on research into novel topical antimicrobial therapies for skin infections and chronic wounds. Research and clinical experience suggest meaningful benefits in this area when used as part of a comprehensive treatment approach.

Biomarker development for inflammatory skin disease monitoring (psoriasis, atopic dermatitis)

Defensin (HBD-2) is particularly well-suited for individuals focused on biomarker development for inflammatory skin disease monitoring (psoriasis, atopic dermatitis). Research and clinical experience suggest meaningful benefits in this area when used as part of a comprehensive treatment approach.

Understanding innate-adaptive immune crossover mechanisms in mucosal defense

Defensin (HBD-2) is particularly well-suited for individuals focused on understanding innate-adaptive immune crossover mechanisms in mucosal defense. Research and clinical experience suggest meaningful benefits in this area when used as part of a comprehensive treatment approach.

Development of antimicrobial surfaces and wound dressings incorporating defensin peptides

Defensin (HBD-2) is particularly well-suited for individuals focused on development of antimicrobial surfaces and wound dressings incorporating defensin peptides. Research and clinical experience suggest meaningful benefits in this area when used as part of a comprehensive treatment approach.

Defensin (HBD-3)

Research into anti-MRSA therapeutics and alternatives to vancomycin for resistant infections

Defensin (HBD-3) is particularly well-suited for individuals focused on research into anti-mrsa therapeutics and alternatives to vancomycin for resistant infections. Research and clinical experience suggest meaningful benefits in this area when used as part of a comprehensive treatment approach.

Development of antimicrobial wound dressings and medical device coatings

Defensin (HBD-3) is particularly well-suited for individuals focused on development of antimicrobial wound dressings and medical device coatings. Research and clinical experience suggest meaningful benefits in this area when used as part of a comprehensive treatment approach.

Anti-biofilm strategies for chronic wound infections and implant-associated infections

Defensin (HBD-3) is particularly well-suited for individuals focused on anti-biofilm strategies for chronic wound infections and implant-associated infections. Research and clinical experience suggest meaningful benefits in this area when used as part of a comprehensive treatment approach.

Applications requiring antimicrobial activity in physiological or high-salt environments

Defensin (HBD-3) is particularly well-suited for individuals focused on applications requiring antimicrobial activity in physiological or high-salt environments. Research and clinical experience suggest meaningful benefits in this area when used as part of a comprehensive treatment approach.

Safety Profile

Side
effects

Defensin (HBD-2)

Common

  • Local site irritation
  • Transient inflammatory response
  • Reduced activity in saline environments

Uncommon

  • Localized allergic reaction
  • Inflammatory amplification

Serious

  • No serious adverse effects documented

Defensin (HBD-3)

Common

  • Local site irritation
  • Transient inflammatory response
  • Mild wound bed changes

Uncommon

  • Localized allergic reaction
  • Mild cytotoxicity at high concentrations

Serious

  • No serious adverse effects documented at therapeutic concentrations

Research Status

Safety
& evidence

Defensin (HBD-2)

Evidence Level

Moderate human trials (Phase 1-2)

FDA Status

Research compound

Safety Overview

Defensin HBD-2 is not FDA-approved and has no completed human clinical trials, with all safety data limited to in vitro mechanistic studies and animal models. Animal toxicology studies show no significant systemic toxicity or organ damage at doses exceeding therapeutic levels. However, human immunological responses to exogenously administered antimicrobial peptides are not fully characterized. Concerns exist regarding potential immune activation, cross-reactivity with self-antigens, and development of antibodies to the synthetic peptide. Bacterial resistance development to defensin-based therapeutics is theoretically possible. No human pharmacokinetics, dose-escalation studies, Phase 1 safety data, or clinical efficacy trials have been conducted.

Contraindications

  • xKnown hypersensitivity to defensin peptides or formulation components
  • xPregnancy and breastfeeding — insufficient safety data for exogenous defensin administration
  • xActive autoimmune skin conditions where defensin overexpression may contribute to pathology (e.g., psoriasis flare)
  • xCystic fibrosis patients — elevated airway NaCl concentrations inactivate HBD-2 antimicrobial activity

Defensin (HBD-3)

Evidence Level

Moderate human trials (Phase 1-2)

FDA Status

Research compound

Safety Overview

Defensin HBD-3 is not FDA-approved and has no completed human clinical trials, existing only in research contexts with in vitro and animal study data. Animal toxicology studies demonstrate no major systemic toxicity at doses exceeding therapeutic levels, but human immunological responses to exogenously administered defensin peptides have not been characterized. Risks include potential immune activation, cross-reactivity with self-antigens (due to HBD-3 expression in healthy epithelial cells), development of anti-peptide antibodies, and possible tolerance development with repeated dosing. Bacterial and fungal resistance to defensin-based therapy is theoretically possible. No human pharmacokinetics, dose-ranging studies, Phase 1 safety assessments, or clinical efficacy data exist.

Contraindications

  • xKnown hypersensitivity to defensin peptides or formulation components
  • xPregnancy and breastfeeding — insufficient safety data for exogenous defensin administration
  • xActive autoimmune conditions — potential for immune activation through monocyte/macrophage recruitment
  • xSevere hepatic or renal impairment — peptide clearance may be altered for any systemic exposure

Decision Guide

Which is
right for you?

Choose Defensin (HBD-2) if...

  • Research into novel topical antimicrobial therapies for skin infections and chronic wounds
  • Biomarker development for inflammatory skin disease monitoring (psoriasis, atopic dermatitis)
  • Understanding innate-adaptive immune crossover mechanisms in mucosal defense
  • Development of antimicrobial surfaces and wound dressings incorporating defensin peptides

Choose Defensin (HBD-3) if...

  • Research into anti-MRSA therapeutics and alternatives to vancomycin for resistant infections
  • Development of antimicrobial wound dressings and medical device coatings
  • Anti-biofilm strategies for chronic wound infections and implant-associated infections
  • Applications requiring antimicrobial activity in physiological or high-salt environments
Full Defensin (HBD-2) ProfileFull Defensin (HBD-3) Profile