PDRN — the salmon ingredient that started in surgery, not serums · K Brand
K Brand The K Lab Ingredient Lab

PDRN —
the ingredient that started in surgery,
not serums.

It’s the most clinically credible ingredient to enter K-beauty in a decade. It’s also the most misrepresented. Here’s what the evidence actually says about the “salmon DNA” molecule.

37.3%
Wound closure in PDRN group
vs. 18.9% placebo (p=0.003)
Diabetic foot ulcer RCT · PMC clinical trial
1994
Year PDRN was approved
as a pharmaceutical in Italy
AIFA approval · Regentec clinical documentation
8–12 wks
Minimum timeline for anti-aging
results in topical clinical studies
Journal of Cosmetic Dermatology, 2023

What PDRN actually is — and why it matters that you know

PDRN stands for polydeoxyribonucleotide. Strip away the acronym and you have a purified, highly processed fragment of DNA — a biopolymer made from chains of deoxyribonucleotides with molecular weights ranging from 50 to 1,500 kDa. It is extracted from salmon milt (the tissue with the highest DNA concentration in the fish), then subjected to a rigorous purification process that removes all proteins, reproductive material, and biological debris. What remains is a sterile, cell-free nucleotide polymer.

PDRN is not a new discovery dressed in K-beauty packaging. It was approved by Italy’s AIFA — the Italian equivalent of the FDA — as a pharmaceutical drug for wound healing in 1994. That’s over three decades of clinical use before it became a serum ingredient. In South Korea, the injectable form (Rejuran Healer) became one of the most in-demand aesthetic procedures in the country. The topical serums followed on the back of that clinical reputation.

This origin story is the reason PDRN is worth taking seriously — and also the reason it needs to be scrutinized carefully. Ingredients with strong injectable or pharmaceutical evidence don’t automatically translate into equivalent topical efficacy. The skin is a barrier. Molecule size and delivery method change everything. Understanding what the evidence actually says for topical PDRN, versus what carries over from injectables, is the only way to evaluate it honestly.

🐟 Myth vs. Reality — The “Salmon Sperm” Story

The claim: You’re putting salmon sperm on your face.

The reality: The final PDRN compound contains zero reproductive cells, zero proteins, and zero biological material from salmon beyond the nucleotide chain itself. “Salmon milt” refers to the source tissue — chosen because it has the highest DNA concentration — not the product. The purification process is pharmaceutical-grade. Calling it “salmon sperm” in a skincare context is technically traceable but functionally misleading. What ends up in your serum is a sterile DNA polymer that is highly compatible with human skin biology, precisely because DNA is structurally universal across species.

How it works — the mechanism is the story

PDRN has two primary mechanisms that make it genuinely interesting to dermatologists — not because of the “salmon” angle, but because of the receptor pathway it activates.

A2A Adenosine Receptor Activation. This is PDRN’s main pharmacological mechanism. PDRN binds to adenosine A2A receptors on skin cells, triggering a cascade of downstream effects: reduced pro-inflammatory cytokines (TNF-α, IL-6), upregulation of VEGF (which promotes new blood vessel formation — angiogenesis), and stimulation of fibroblast proliferation. Fibroblasts are the cells responsible for producing collagen, elastin, and other structural ECM proteins. Activating them through a receptor pathway — rather than causing controlled damage like retinol or acids do — is a gentler and more targeted approach to collagen stimulation.

Nucleotide Salvage — DNA Building Blocks. Rapidly dividing and repairing cells need raw materials for DNA synthesis. Rather than building from scratch (de-novo synthesis), cells can take up pre-formed nucleotide fragments and incorporate them directly — a process called nucleotide salvage. PDRN provides exactly this: a supply of deoxyribonucleotide building blocks that stressed or damaged cells can use to accelerate repair. In wound healing contexts, this mechanism is well-documented. For everyday skincare, it translates to supporting turnover in UV-damaged, post-procedure, or chronologically aged skin.

Barrier restoration. Studies in 3D skin models show PDRN improves expression of filaggrin, E-cadherin, and tight junction proteins — the structural proteins that hold the skin barrier together. This isn’t just theoretical. A plant-derived PDRN study (with the caveat that plant PDRN differs from salmon PDRN) showed a 92% re-epithelialization rate at 50% PDRN concentration versus 17% untreated at day 5.

“PDRN demonstrated significant therapeutic potential in promoting cellular proliferation, migration, and differentiation — with in vivo studies showing accelerated wound closure, improved epithelialization, increased vascularization, and modulated inflammatory markers.”

— Systematic Review & Meta-Analysis (7 studies), International Surgery Journal, 2025. Verify on PubMed →

The evidence, benefit by benefit

Mechanism / Benefit
Evidence Rating
What the research actually shows
Wound Healing & Skin Recovery
PDRN’s best-proven application
Strong
Multiple RCTs including a diabetic foot ulcer trial (PDRN: 37.3% wound closure vs. 18.9% placebo, p=0.003), a 2025 meta-analysis of 7 studies, and validated post-procedure protocols in Korean clinical aesthetics — wound healing is where PDRN’s evidence base is unambiguous and independently confirmed.
Post-Procedure Recovery
Post-laser, microneedling, peels
Strong
PDRN is specifically used and clinically validated in Korean aesthetic medicine as a post-procedure recovery agent. A 2025 systematic review found topical PDRN offered synergistic oxidative stress reduction and skin tone improvement when combined with microneedling — its A2A receptor mechanism actively reduces post-treatment inflammation while nucleotide salvage supports accelerated repair.
Fine Lines & Elasticity (Injectable)
Rejuran Healer / PN injectable form
Strong
Injectable PDRN/PN has robust clinical support — including a split-face RCT where PN outperformed HA fillers for skin roughness, pore size, and periorbital hydration. The anti-aging reputation that drove consumer demand for topical PDRN is built almost entirely on injectable evidence. This distinction is critical to understand.
Fine Lines & Elasticity (Topical)
OTC serums and ampoules
Moderate
Industry-associated studies (including one split-face study reporting 47% fine line reduction and 39% elasticity improvement at 8 weeks) show promising topical results — but independent peer-reviewed confirmation of topical-specific RCTs is limited. Treat as promising, not proven. The mechanism supports the benefit; the independent evidence trail is still thin.
Hydration & Barrier Function
Filaggrin, tight junction restoration
Moderate
3D skin model and combination studies (PDRN + HA) show meaningful hydration improvement and barrier marker restoration — including filaggrin and E-cadherin expression. Strong mechanistic rationale, but most supporting data comes from in-vitro and combination studies rather than standalone topical RCTs in human subjects.
Anti-Inflammatory Effect
TNF-α, IL-6 reduction via A2A
Moderate
A2A adenosine receptor activation and subsequent reduction in TNF-α and IL-6 is well-established in pharmaceutical/injectable research. Translation of this mechanism to topical application depends on how much PDRN actually penetrates — which is limited by molecular size. The anti-inflammatory benefit is real; the magnitude in consumer serums is still being quantified.
Hair Regeneration / Acne Scarring
Emerging applications
Limited
The 2025 Brieflands systematic review notes PDRN’s potential for hair regeneration, acne scar treatment, and melanogenesis modulation — but these applications are newer, less independently replicated, and mostly supported by preliminary studies or injectable contexts. Interesting, not ready for strong claims.

The delivery gap — injectable vs. topical, clearly separated

The single most important thing to understand about PDRN in consumer skincare is that the ingredient is the same, but the delivery is not. PDRN is a relatively large molecule — 50 to 1,500 kDa — which means it faces the same fundamental barrier problem as any large biopolymer attempting to penetrate intact skin. Most topical PDRN remains in the epidermis. Only smaller molecular weight fragments reach the upper dermis. Injectable PDRN bypasses this entirely, depositing directly into the dermis where fibroblasts and the ECM live.

This is not a reason to dismiss topical PDRN — the epidermis and skin surface are legitimate targets, the A2A receptor mechanism operates even at the surface level, and post-procedure application (when the barrier is temporarily compromised by microneedling channels) dramatically improves penetration. But it is a reason to calibrate expectations. Topical results are more gradual, more surface-focused, and require consistent long-term use. They are not a substitute for an injectable Rejuran procedure.

Injectable PDRN — Medical Grade
Form Prescription pharmaceutical
Concentration 3–5% (medical grade)
Delivery Direct to dermis; bypasses barrier entirely
Evidence Strong RCT evidence for anti-aging and skin quality
Side effects Bruising, swelling, pain, nodules (injection-site only)
USA status Not FDA-approved for injection; used topically post-procedure by US practitioners
Topical PDRN — Consumer Skincare
Form OTC serum, ampoule, mask
Concentration 0.001–2% depending on product tier
Delivery Epidermis; limited dermal penetration (size-dependent)
Evidence Moderate — promising but mostly industry-funded topical trials
Side effects Rare mild redness (<2%); well-tolerated in all clinical studies
USA status Unrestricted OTC; sold freely in US, Korea, and most markets

The PPM game — concentration numbers explained

K-beauty PDRN brands have turned concentration into a marketing battleground. You’ll see products shouting 2,000 ppm, 5,000 ppm, 10,000 ppm. The number sounds impressive. The science behind it is more complicated.

Independent formulation experts note there’s no established evidence of additional benefit above the skin’s absorption capacity — and that very high concentrations may increase irritation risk without any additional efficacy payoff. One clinical-grade brand claims 1,200 ppm (~0.12%) as an optimal concentration, but this figure comes from a proprietary study and hasn’t been independently verified. What the research does confirm: the mass-market tier (0.001–0.01%) is likely too low to deliver meaningful clinical results. Mid-range products (~0.1%) are more formulation-credible.

PDRN Concentration Reference Guide What the tiers actually mean for efficacy
Product Tier Typical Concentration In PPM Evidence Context Rating
Mass-market OTC 0.001–0.01% 10–100 ppm Below concentrations used in clinical studies; minimal validation at these levels Low credibility
Mid-range K-beauty serums ~0.1% ~1,000 ppm More formulation-credible; aligns closer to studied concentrations Reasonable
Clinical-grade topical ~0.12–0.5% 1,200–5,000 ppm Range referenced in professional post-procedure protocols; one brand-cited optimal concentration Best-supported
Professional / post-procedure 0.5–2% 5,000–20,000 ppm Used under practitioner guidance; significantly enhanced penetration via microneedling channels Professional use
Injectable (Rx only) 3–5% 30,000–50,000 ppm Pharmaceutical grade; not a cosmetic product; direct dermal delivery; strongest evidence base Prescription only

Plant-derived vs. Salmon PDRN — not the same thing

Some brands sell “plant-derived PDRN” sourced from ginseng or green tea and label it PDRN. These are polysaccharide-based compounds — structurally different from salmon-derived nucleotide polymers. They do not share the same A2A receptor mechanism, and the clinical evidence for salmon PDRN does not apply to plant-derived versions. When shopping, look for “polydeoxyribonucleotide from salmon” or “salmon PDRN” explicitly on the label. If the brand only lists “plant-derived PDRN” or doesn’t specify source, that’s a different ingredient wearing the same name.

Safety, fish allergies, pregnancy, and the EU “ban” myth

Topical PDRN has an excellent safety profile in clinical literature. Multiple studies report no significant adverse events. The rate of mild, transient redness or tingling is below 2% in controlled trials. PDRN is non-immunogenic in the conventional sense — it’s not a protein, so it doesn’t trigger the standard allergen pathway.

⚠ Fish Allergy Note

PDRN is derived from salmon, but the purification process removes all proteins — the components that actually cause fish allergies. Clinical studies have not confirmed allergic reactions in fish-allergic participants using high-purity PDRN. That said, if you have a severe fish allergy, patch testing and dermatologist consultation before use is the sensible precaution. It’s a real edge case, not a widespread concern — but worth flagging for your specific situation.

⚠ Pregnancy & Breastfeeding — Insufficient Data

There are no formal safety studies for topical PDRN use during pregnancy or breastfeeding. Systemic absorption from topical application is expected to be very low, but the absence of data is itself reason for caution. Most dermatologists recommend avoiding PDRN during pregnancy — not because there’s evidence of harm, but because there’s no evidence of safety either. Hyaluronic acid, Centella asiatica, and niacinamide are well-documented pregnancy-safe alternatives with equivalent or stronger topical hydration and barrier-support evidence.

On the regulatory front: PDRN is not banned in the EU. This claim circulates online and is incorrect. PDRN is not on the EU Cosmetics Regulation’s restricted or prohibited ingredient list, and the EU’s 2025 Omnibus Act VII (which bans newly classified CMR substances) does not include PDRN. The EU regulatory complexity around PDRN is about documentation — products containing animal-derived biological material require an individual Cosmetic Product Safety Report and source traceability. That’s a compliance barrier, not a prohibition.

How to actually use it

Step in the routine: Apply after cleansing and toning, before heavier moisturizers and occlusives. If using alongside HA, apply PDRN first — it handles repair and signaling, HA handles moisture-binding and surface hydration. They’re complementary, not competing.

Best application window: Post-procedure — after laser, microneedling, or professional peels — is when topical PDRN earns its strongest argument. The skin barrier is temporarily disrupted, penetration improves substantially, and PDRN’s anti-inflammatory and repair mechanisms have maximum relevance. This is the window where the clinical evidence for topical use is most directly supported.

What to pair with: HA (for complementary hydration), niacinamide (anti-inflammatory synergy, brightening), and peptides (collagen support from a different mechanism). Avoid pairing with high-strength AHAs or BHAs in the same application pass. PDRN is a recovery ingredient — use it when your skin is in repair mode, not while actively exfoliating.

Frequency and timeline: Twice daily application matches most studied protocols. Anti-aging results in topical clinical studies were measured at 8–12 weeks. Post-procedure recovery benefits are visible in 1–2 weeks. The 28-day cell cycle means you need at least a full month before making any judgment on efficacy — most brands sensibly recommend a 4-week minimum.

Storage matters more than most ingredients: PDRN is a biological molecule sensitive to heat, light, and air exposure. Opaque, airtight packaging is not just a premium aesthetic choice — it protects molecular integrity. Pump or dropper tubes outperform open-jar formats for this ingredient specifically.

The K Lab Proof Score

Rated on published clinical evidence, not marketing claims
Worth the Spend — with informed expectations
Ingredient Quality
8.5/10

A legitimate pharmaceutical-grade ingredient with 30+ years of clinical use. Non-immunogenic, sterile, well-characterized. Source and purity transparency vary by brand — this is where quality diverges in consumer products.

Clinical Evidence (Topical)
6.8/10

Strong evidence for wound healing and post-procedure recovery. Moderate and emerging for topical anti-aging specifically — most anti-aging RCT strength belongs to injectable PDRN. Independent topical trials are growing but not yet at niacinamide or HA levels of replication.

Value for Money
7.2/10

Mid-range and clinical-tier K-beauty PDRN serums offer genuine value — particularly for post-procedure use. Mass-market products shouting ppm numbers at low concentrations are selling branding, not bioactivity. The ppm race is mostly noise above the absorption threshold.

Skin Type Versatility
7.5/10

Suitable for most skin types — particularly aging, dull, post-procedure, and acne-scarred skin. Not suitable during pregnancy (insufficient data). Not suitable for vegans. Fish-allergic individuals should patch test. Otherwise, tolerability is excellent.

Who this ingredient works for — and who should look elsewhere

Works well for

  • Post-procedure recovery — this is PDRN’s strongest topical use case, full stop
  • Aging skin looking for a repair-focused collagen-support ingredient
  • Dull or damaged skin where barrier restoration is the priority
  • Acne-prone or acne-scarred skin — anti-inflammatory mechanism is relevant here
  • Anyone who has tried injectables and wants a topical maintenance option
  • Sensitive skin — well-tolerated, low irritation profile in all clinical studies
  • K-beauty enthusiasts wanting the ingredient behind Rejuran in topical form

Look elsewhere if…

  • You are pregnant or breastfeeding — insufficient safety data; switch to HA or Cica
  • You follow a vegan lifestyle — salmon PDRN is an animal-derived ingredient
  • You have a severe fish allergy — patch test first, consult your dermatologist
  • You want injectable-equivalent results from a serum — adjust expectations; the delivery gap is real
  • You are evaluating mass-market “PDRN” products at 10–100 ppm — the concentration is below clinically relevant levels
  • You see “plant-derived PDRN” on the label without specification — it’s a different molecule

The K Lab Final Verdict

PDRN is the most clinically credible new ingredient in K-beauty. That’s also exactly why it requires the most careful reading.

The clinical foundation is real. Three decades of pharmaceutical use, a 2025 meta-analysis, RCTs with statistically significant wound healing outcomes, and a well-characterized receptor mechanism that dermatologists take seriously. This is not a botanical extract riding a trend. PDRN earned its place in Korean clinical aesthetics through surgical and pharmaceutical evidence before it ever entered a serum bottle.

But the translation from injectable to topical is partial, not complete. The penetration barrier is real. The strongest topical evidence is for post-procedure recovery — when that barrier is temporarily open. For everyday anti-aging in intact skin, the topical evidence is promising but still industry-heavy and less independently replicated than established ingredients like niacinamide or HA. “Promising and mechanistically sound” is not the same as “proven at the same level.”

Shop at the right concentration tier, demand source transparency (salmon, not plant-derived), and use it where it performs best — post-procedure, consistently, over at least 8 weeks. That’s the protocol where the evidence is behind you. Everything else is managing the gap between pharmaceutical reality and consumer marketing.

K Brand Proof Summary

Worth the Spend — strongest for post-procedure; promising for everyday anti-aging.

Injectable evidence ≠ topical evidence — know the gap Post-procedure is PDRN’s strongest topical use case Demand salmon-derived, not plant-based PPM race is noise — check the tier, not the number Avoid in pregnancy · not vegan · patch test for fish allergy

Research citations

1
Veronesi, F. et al. (2022). “Polydeoxyribonucleotides as Emerging Therapeutics for Skin Conditions.” Pharmaceutics. Overview of PDRN mechanisms including A2A receptor activation, wound healing, and collagen stimulation. Verify on PubMed →
2
Systematic Review & Meta-Analysis (7 studies). (2025). “The impact of polydeoxyribonucleotide on wound healing.” International Surgery Journal. Confirmed significant therapeutic potential — cellular proliferation, migration, differentiation, vascularization, and inflammatory modulation in in vivo models. Verify on PubMed →
3
Lee, J.H. et al. (PMC). “Pharmacological Activity and Clinical Use of PDRN.” PMC / National Library of Medicine. Details PDRN’s tissue-repairing, anti-inflammatory, and angiogenic activities with clinical trial context. View on PMC →
4
Comparison study (split-face RCT). “Comparison of Polynucleotide and Polydeoxyribonucleotide for periorbital skin quality.” PMC. PN demonstrated superior outcomes to HA fillers for roughness, pore size, and hydration in the periorbital region. View on PMC →
5
Kim, Y. et al. (2023). “Analysis of Skin Regeneration and Barrier-Improvement Efficacy of Polydeoxyribonucleotide in 3D Skin Models.” PMC. Confirmed filaggrin, E-cadherin, and tight junction protein restoration; re-epithelialization rate of 92% vs. 17% untreated at day 5. View on PMC →
6
Systematic Review (2025). “Polydeoxyribonucleotide in Skincare and Cosmetics.” Brieflands / Journal of Skin Science and Cosmetic Technology. Review of PDRN benefits across anti-aging, wound healing, hair regeneration, acne scars, and melanogenesis. View on Brieflands →

K Brand Ingredient Lab ratings are based on published peer-reviewed literature, regulatory documentation, and NCBI-indexed clinical trials — not personal product testing or brand sponsorship. All citations are provided for verification; readers are encouraged to review original sources. This article is for educational purposes only and does not constitute medical advice. Topical PDRN is not recommended during pregnancy due to insufficient safety data — consult your doctor or dermatologist. PDRN is an animal-derived ingredient and is not suitable for vegans. This article may contain affiliate links. Full disclosure →

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