TL;DR: The problem is choosing the right active in the wrong vehicle, at the wrong pH, with incompatible excipients — and only discovering this at week 8 of stability
TL;DR: Salicylic acid requires a formulation pH between 3.0 and 4.0 to maintain meaningful free acid activity
Key Technical Parameters #
Choosing the wrong active isn’t usually the problem. The problem is choosing the right active in the wrong vehicle, at the wrong pH, with incompatible excipients — and only discovering this at week 8 of stability. This guide walks through the six material selection criteria we apply before committing to a formulation direction for acne and blemish control products. It’s aimed at brand teams who’ve already decided on a general concept and now need to make concrete ingredient decisions that will survive both stability qualification and regulatory review. The criteria here apply most directly to leave-on serums, moisturizers, and targeted treatments — not rinse-off formats, which have a different tolerance window for actives.
Six Selection Criteria With Numeric Thresholds #
Criterion 1: Active-to-Vehicle pH Compatibility #
This is where most acne formulation briefs start to break down. Salicylic acid requires a formulation pH between 3.0 and 4.0 to maintain meaningful free acid activity. Niacinamide, on the other hand, converts to nicotinic acid and generates flushing risk at pH below 4.5 or above 7.0 under thermal stress. Combine them without buffering strategy and you have a formulation that either underperforms the active or fails consumer experience testing.
Benzoyl peroxide is a different case entirely. It’s inherently pH-insensitive in terms of efficacy, but the oxidative environment it creates degrades almost every co-active you’d want alongside it — retinoids, vitamin C derivatives, and most botanical polyphenols included. We run what we call our AC-04 compatibility screen on any formulation pairing benzoyl peroxide with a secondary active before committing to a prototype direction.
Azelaic acid sits at pH 4.0–5.5 in most effective formulations and is one of the more forgiving actives in this category from a vehicle compatibility standpoint. That said, solubility is the constraint — above roughly 15% in aqueous emulsions you start seeing crystal formation, especially in cold-chain stress cycles.
Criterion 2: Skin Barrier Impact Score #
Acne actives are inherently disruptive to varying degrees. The selection question isn’t “which active is mildest” but “what is the acceptable TEWL (transepidermal water loss) increase at the intended use concentration, given the target consumer’s baseline skin condition?”
We use a four-tier internal classification:
| Active | Effective Concentration Range | Expected TEWL Change at Upper End | Barrier Recovery Estimate |
|---|---|---|---|
| Salicylic acid | 0.5–2.0% | +18–25% over 4 weeks | 3–5 weeks off-cycle |
| Benzoyl peroxide | 2.5–5.0% | +30–40% in sensitized skin | Requires concurrent emollient |
| Azelaic acid | 10–15% | +6–10% | Self-limiting, low concern |
| Niacinamide | 4–10% | Neutral to slightly positive | Barrier-supportive at ≥5% |
The TEWL figures above come from our internal test panel data (n=28, mixed acne-prone skin types, measured at week 4 of twice-daily application). They’re directional, not regulatory-grade clinical data. For claims substantiation you’d need a formal study, and we’d set that up separately.
Benzoyl peroxide at 5% is the one that surprises brand partners most. The barrier disruption is real, and at 5% you almost always need a concurrent ceramide or glycolipid repair component to prevent the product from worsening sensitivity over time, particularly in Asian markets where consumer tolerance for initial skin reaction is lower than in Western markets.
Criterion 3: Regulatory Classification Threshold #
This is non-negotiable and has to be resolved before any other decision. In the US, salicylic acid above 0.5% in leave-on products and benzoyl peroxide at any concentration in leave-on products are regulated under the FDA Cosmetics Guidelines OTC monograph framework — which means drug registration, specific labeling, and manufacturing site registration. In the EU, salicylic acid in face products is limited to 0.5% under EU Cosmetics Regulation 1223/2009, and benzoyl peroxide is not permitted as a leave-on cosmetic ingredient at all.
For brands developing a global SKU, this often means the EU version is a genuinely different formulation — not just a label change. We flag this at every kickoff call because the default assumption from brand teams is that one formula with market-specific labeling will cover everything. It won’t, not in this category.
For NMPA Cosmetic Regulation in China, salicylic acid above 0.3% in leave-on products requires special cosmetic registration, which adds 6–12 months to the timeline. Most brands developing for the China market have to decide early whether to file at the higher concentration or reformulate.
Criterion 4: Interaction With Emollient and Humectant Selection #
This section gets skipped in most briefs. The emollient and humectant choices determine whether an acne active reaches the target site at effective concentration, or whether it gets sequestered in the oil phase or complexed by a high-molecular-weight humectant before it penetrates.
In practice, high-viscosity hyaluronic acid at concentrations above 0.5% creates a physical barrier that measurably slows salicylic acid flux across the stratum corneum in our in-vitro Franz cell models. Low-molecular-weight HA (below 5 kDa) has a much smaller effect. We see this come up constantly — a brand specifies both “HA complex” and “2% salicylic acid” without specifying molecular weight fractions, and the formulation then underperforms on comedolytic efficacy even though the label concentration is correct.
Our acid exfoliation technology pages cover the penetration enhancement strategies in more detail, but the short version is: keep your emollient phase lean in acne leave-on treatments, and prioritise low-MW penetration enhancers over film-forming moisturisers.
Criterion 5: Antimicrobial Preservation Adequacy Under Active Load #
Acne formulations create a hostile environment for your preservation system. Benzoyl peroxide is itself an oxidising antimicrobial, but it also degrades most parabens rapidly — within 4 weeks at 40°C in our stress tests. Phenoxyethanol stability is better but still compromised above 3% BPO. We’ve had batches come through challenge testing at week 0 and fail at week 6 because the preservative was depleted by the active, not by microbial load.
The PCPC Guidelines recommend challenge testing per ISO 11930, and the ISO Standards specification requires category A criteria for leave-on facial products. We run this at 0, 4, 8, and 12 weeks during accelerated stability — not just at start and end. The failure mode with BPO-heavy formulas is mid-cycle, and a start/end-only protocol will miss it.
For formulas using salicylic acid at ≥1.5%, the low pH itself provides some antimicrobial support, but it’s not a replacement for a qualified preservation system. We’ve tried to use the self-preserving argument with a few briefs. The challenge data has not been consistent enough to rely on it.
Criterion 6: Consumer-Visible Stability (Colour, Odour, Phase) #
Brands consistently underestimate this one. The active might be stable at clinically relevant concentration while the product looks and smells oxidised to the consumer. Benzoyl peroxide formulas yellowing in HDPE bottles. Salicylic acid serums developing a faint vinegary note after 6 months in PET packaging. Niacinamide formulas going faintly pink due to niacin conversion under UV exposure through clear glass.
For packaging selection in this category, our internal protocol (logged under MPC-12 in our packaging compatibility tracker) tests colour delta-E and odour panel scores at 3-month intervals up to 24 months. A delta-E above 2.0 is considered consumer-perceptible. We’ve had BPO formulas that were chemically within spec but hit delta-E of 3.8 by month 9. The brand had to switch to opaque white PP, which they hadn’t budgeted for.
Why the Clinical Evidence Matters More Than Concentration for This Category #
The actives in acne-blemish control are among the best-studied in cosmetics and OTC dermatology. But the clinical picture is more nuanced than most ingredient datasheets suggest.
A 2022 split-face RCT (n=44, 12 weeks, published in the Journal of Clinical and Aesthetic Dermatology) compared 1% salicylic acid versus 20% azelaic acid in subjects with mild-to-moderate comedonal and inflammatory acne. Azelaic acid at 20% showed a 58% reduction in inflammatory lesion count versus 41% for salicylic acid at 1%. Non-inflammatory lesions responded more similarly: 49% reduction for azelaic acid versus 44% for salicylic acid. The takeaway for formulation teams is that if a brand wants to emphasise anti-inflammatory positioning alongside anti-comedogenic, azelaic acid at 15–20% has a stronger evidence base than salicylic acid for that specific claim vector — but the EU regulatory path for that concentration requires the formula to be positioned as a medical device or OTC drug in most markets, which changes the whole commercialisation model.
We’re genuinely uncertain about some of the newer actives in this space. Bakuchiol as an acne active, for example — the retinol-like positioning is well-supported for anti-aging, but the published evidence specifically for acne is thin. One randomised study (n=61, 12 weeks) showed a modest 32% reduction in lesion count, but the control arm wasn’t matched for concurrent skincare use, which weakens the result. We still formulate with bakuchiol in our acne-blemish-control category, but we’re careful about what claims we’d support.
The supplier data and our own stability results also don’t always agree on azelaic acid solubility at elevated temperatures. One raw material supplier specifies stable emulsification up to 50°C during manufacturing. Our process data suggests you need to work below 45°C if you want to avoid particle size drift post-cooling. We apply the more conservative threshold.
What to Specify in Your Purchase Order #
A brief that says “salicylic acid serum, 1.5%, targeting acne-prone skin” is not a formulation specification. Before a PO makes sense in this category, the following need to be defined:
Active identity and grade. Not all salicylic acid grades are equivalent in particle size distribution and impurity profile. Specify USP or EP grade where regulatory status requires it. Same for benzoyl peroxide — cosmetic and pharmaceutical grades differ in ways that matter for both stability and compliance.
Target pH with tolerance window. Don’t leave this open. Specify the pH range (e.g., 3.5 ± 0.3 for a salicylic acid serum) and require it documented on every batch record. Drift outside this window mid-shelf-life is a stability failure, not a cosmetic variation.
Packaging material, closure type, and airless vs. non-airless. For any BPO or oxidation-sensitive formula, the oxygen ingress rate of the packaging is a material spec, not a procurement afterthought.
Preservation system with minimum acceptance criteria. Reference ISO 11930 Category A or B explicitly. Don’t allow “equivalent system” without pre-agreed testing.
Regulatory market scope. State the filing markets on the PO. This determines which restricted substances list applies and whether drug registration is required before production release.
Stability acceptance criteria. Define what pass/fail looks like at 4 and 8 weeks accelerated. Don’t leave the judgment call to the manufacturer.
Formulation Notes for Brand Partners #
When you brief us on an acne or blemish-control product, the first questions we ask aren’t about the active — they’re about the market, the format, and what the pack is going to say on front-of-pack. Those three things determine the qualification burden before we’ve looked at a single ingredient.
The brief mistake we see most often is specifying both the active and the texture in the same document as fixed requirements, when actually one of them has to flex to make the other work. A brand will brief us on “lightweight watery serum, 2% salicylic acid, EU and US launch.” At 2% salicylic acid in an aqueous serum at EU-compliant pH, the formula has a sharp acidic character that is difficult to mask in a thin fluid vehicle — and the EU 0.5% cosmetic limit means this product needs OTC drug status in Europe regardless of texture. Picking the active concentration first, then letting us recommend the vehicle, avoids this kind of constraint-stacking.
Lab samples take 2–3 weeks from confirmed brief. Accelerated stability runs 4–8 weeks at 40°C/75% RH. 24-month real-time stability is initiated concurrently and runs through production scale-up. For actives requiring regulatory filing, we typically add 4–6 weeks upfront for regulatory pre-assessment before the formulation stage begins.
Frequently Asked Questions #
Can we run salicylic acid and niacinamide in the same formula?
A: Yes, but you have to commit to a pH range that serves both, which in practice means 4.5–5.0 — and at that pH, the free acid fraction of salicylic acid is reduced enough that you’re relying more on its lipophilic penetration than its keratolytic activity. For a product where salicylic acid is the hero active, we’d almost always put niacinamide in a separate step or a second SKU. For a formula where niacinamide is the hero and salicylic acid is supporting, the pairing works fine at 0.5–1%.
What happens if we want benzoyl peroxide in a leave-on product for EU launch?
A: BPO in leave-on cosmetics isn’t permitted under EU Cosmetics Regulation 1223/2009. It’s not a concentration question — it’s categorically excluded. If EU is in scope, the product either routes through medical device or dermatology prescription channels, or you swap to a permitted alternative like azelaic acid or piroctone olamine.
We’ve had a product pass stability at 3 months and then fail consumer testing at month 9 — what usually causes this?
A: Preservation depletion under oxidative active load is the most common mechanism we identify. A benzoyl peroxide formula can show clean microbial challenge results at week 12 during accelerated testing, then fail at month 9 in real-time because the preservative is exhausted by the active before the microbial challenge occurs under real storage conditions. Running challenge tests at intermediate time points — not just start and end — catches this. We mandate 0, 4, 8, and 12 weeks for any BPO-containing formula under our MPC-12 protocol.
What’s the MOQ for a salicylic acid serum in this category?
A: Minimum order quantity starts at 3,000 units for a standard formula in a stock component. For a customised formula in a custom-mould packaging, 10,000 units is a more realistic floor when you account for minimum fill runs and packaging tooling amortisation. Lab sample stage to production release typically runs 14–20 weeks for a new formula, assuming no regulatory filing delays.
Is there an active combination that addresses both active acne and post-acne marks in a single product?
A: Azelaic acid at 10–15% is the closest single-active answer — it has both anti-C. acnes activity and melanogenesis inhibition that’s relevant for post-inflammatory hyperpigmentation. The challenge is that the concentration needed for meaningful PIH impact (≥15%) sits above the EU cosmetic limit threshold for some product formats. For a single global SKU, we’d often pair niacinamide at 5–8% with salicylic acid at the market-maximum concentration, and position azelaic acid as the hero in market-specific SKUs where the regulatory path allows it. It depends on how many SKUs the brand is prepared to manage.
Have a product concept in mind? Contact our formulation team to request a complimentary brief review.
