TL;DR: **Viscosity shifts after shipping.** You receive a COA showing 25,000–35,000 cPs (Brookfield RV, spindle 6, 10 rpm, 25°C), the batch measures within spec on arrival, but by month three the cream has thinned noticeably in the jar
TL;DR: **Emulsification inconsistency between lots.** If you see viscosity variation of more than ±15% lot-to-lot with no corresponding change in the COA — same numbers, every batch — that is a red flag
Key Technical Parameters #
Qualifying a moisturizer or cream supplier is not the same as qualifying a raw material vendor. You are evaluating a manufacturer’s ability to hold a complex emulsion system stable, reproducible, and compliant across hundreds of batches — with your brand name on the label. The brand segments that feel this most acutely are those launching into the EU or US market, where a single non-conforming batch can trigger a recall or regulatory inquiry. The technical insight that separates a qualified supplier from a capable one: a COA can look perfect while the batch fails — and the fields that get falsified most often are the ones brands never think to audit.
What You’re Seeing in the COA — and What It Usually Means #
Most incoming COAs for finished moisturizers and creams arrive looking clean. Viscosity: pass. pH: pass. Appearance: conforms. Microbial: pass. Then the product hits the shelf, and six months later you’re dealing with phase separation, fragrance fade, or a greasy residue that wasn’t in the lab sample. This is one of the most common failure sequences we see at intake review.
Three observable symptoms, and what they usually indicate:
Viscosity shifts after shipping. You receive a COA showing 25,000–35,000 cPs (Brookfield RV, spindle 6, 10 rpm, 25°C), the batch measures within spec on arrival, but by month three the cream has thinned noticeably in the jar. This is almost never a raw material issue. In our experience it usually points to one of two things: thickener grade substitution (carbomer 940 swapped for a lower-MW homopolymer) or incorrect neutralization pH on the production batch. Both will pass a single-point viscosity check while failing long-term rheology.
Emulsification inconsistency between lots. If you see viscosity variation of more than ±15% lot-to-lot with no corresponding change in the COA — same numbers, every batch — that is a red flag. Identical COA values across six consecutive lots in a complex O/W emulsion is statistically improbable unless the supplier is copying results rather than testing them.
Microbial results that are uniformly low. A COA showing <10 CFU/g for total aerobic count across every single lot, forever, with no variation, is not good QC. That’s a sign the microbial testing is either poorly executed or the results are being truncated before reporting. Legitimate testing shows natural variation — some batches at 50 CFU/g, some at 120 CFU/g, all still within the 1,000 CFU/g limit set under EU Cosmetics Regulation 1223/2009.
Diagnostic Map: COA Field → Root Cause #
| COA Symptom | Likely Root Cause | Confirmation Test |
|---|---|---|
| Viscosity in-spec on arrival, fails by month 3 | Thickener grade substitution or neutralization drift | pH recheck + 45°C/4-week aged viscosity |
| Identical microbial counts across all lots | Fabricated or improperly conducted micro testing | Third-party USP 61 challenge retest |
| pH passes (5.0–6.5) but actives degrade early | pH measured at wrong temperature or post-shipment | In-house pH recheck at 25°C ±0.5°C within 24h of receipt |
| Appearance “conforms” despite visible ring-off | Appearance spec not defined in writing, supplier self-interprets | Request written appearance standard with reference photos |
| No lot-to-lot variation in any field | COA values copied from golden batch | Cross-reference with batch manufacturing record audit |
The diagnostic framework our incoming QC team uses — what we log under our IQC-F04 protocol — requires a minimum of five COA fields to be verified instrumentally before release, not just visually checked against the certificate.
The Root Cause Most Teams Miss: Preservative System Efficacy vs. Preservative System Presence #
This is where projects go sideways, consistently. A supplier lists phenoxyethanol at 0.8% w/w on the COA. Your HPLC confirms it. The batch passes. Then you run a preservative efficacy test (PET) six months into production, and the results come back borderline — or failing — for gram-negative bacteria.
Phenoxyethanol is present. The system isn’t working. Those are two completely different problems, and conflating them is the most expensive diagnostic error we see at scale.
Here’s the mechanism. Phenoxyethanol at 0.8% functions well in a water-continuous phase at pH 5.5–6.0. What most incoming QC protocols don’t catch is the oil phase interaction. High concentrations of fatty alcohols — cetearyl alcohol above 4%, stearic acid above 3% — will partition phenoxyethanol preferentially into the oil phase, reducing its free aqueous concentration to a level that no longer provides adequate bacterial inhibition. The COA shows 0.8% total. The effective aqueous concentration may be closer to 0.3–0.4%. That is below the threshold needed to pass the ISO 11930 PET criteria for category 2 cosmetics (≤2 log reduction for bacteria at day 14).
This is not visible on a standard COA. You need an actual PET, not just a chemical assay.
The confirmation test is straightforward: run USP 51 or ISO 11930 on the finished batch against the full challenge panel — S. aureus, E. coli, P. aeruginosa, C. albicans, A. brasiliensis. We require this test on first lot from any new supplier and annually thereafter, or after any formula modification that changes the oil phase ratio by more than 2%. If a supplier cannot provide a PET report with the actual inoculum counts and reduction curves — not just a “pass” checkbox — that is a disqualification event in our system.
One additional variable that brands consistently underestimate: pH drift during shipping. A cream emulsified at pH 6.0 in the factory can arrive at pH 5.4 after 30 days in a container. That drop doesn’t invalidate the phenoxyethanol, but if the system was also relying on organic acid co-preservatives, the shift changes their ionization state and therefore their efficacy. Under FDA Cosmetics Guidelines, preservative adequacy is assessed on the product as sold, not as manufactured — meaning pH drift during transit is your liability, not the factory’s, once you’ve accepted the COA.
We haven’t fully reconciled this across all emulsion types in our dataset. For W/O emulsions the partitioning behavior is different, and our current PET protocols may underestimate aqueous-phase activity in those systems. We’re building out that dataset now.
Corrective Actions, Ranked by Impact and Feasibility #
When you identify a qualification gap — either from a suspicious COA pattern or a failed in-house retest — here are the actions that actually move the needle, in order of practical impact.
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Request the batch manufacturing record (BMR), not just the COA. This is free, fast, and reveals more than any single test. A legitimate supplier will provide a redacted BMR showing processing temperatures, mixing times, order of addition, and in-process pH checks. If they refuse or delay, the qualification stops here. In our AVL gate review process, BMR availability is a binary requirement.
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Retest pH and viscosity in-house within 48 hours of receipt. Use the same spindle geometry and shear rate the supplier specifies — if they don’t specify, ask, because a 10 rpm reading and a 50 rpm reading on the same batch can differ by 40%. This catches neutralization issues and thickener substitutions. Cost: minimal. Detection rate: high for the most common failure modes.
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Conduct an independent PET on the first three lots from any new supplier. As described above, this is the test that COA review cannot replace. A third-party ISO 11930 test runs roughly two to three weeks and the cost is manageable relative to the risk of a microbial recall. This fixes the majority of preservative-system failures before they reach the consumer.
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Commission a full INCI verification panel via HPLC and GC. For any cream carrying active ingredient claims — niacinamide above 3%, hyaluronic acid, peptides — verify the assay independently against the supplier’s COA value. We’ve seen niacinamide COAs claiming 5% where the actual measured value on third-party HPLC came back at 3.1%. For commodity actives, suppliers sometimes adjust batch economics by underdosing; finished product assay is the only reliable check.
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Run a 12-week accelerated stability programme on qualification samples before committing to production MOQ. 40°C/75% RH, sampled at weeks 4, 8, and 12. This is expensive and time-consuming, but for a new supplier relationship it is the only way to validate that their emulsion system holds over the product’s claimed shelf life. Per PCPC Guidelines, accelerated data at 40°C is generally considered predictive of 24-month real-time behavior for O/W emulsions, though this is not a universal rule — W/O and gel-cream formats need separate validation.
Actions 1 and 2 take less than a week. Actions 3 and 4 add two to three weeks to your qualification timeline. Action 5 adds three months. Most brands want to skip to production. We almost always push back on that brief when it’s a new supplier relationship.
Prevention: What to Specify Upfront #
The most effective qualification document is not a COA template — it’s a Finished Product Specification that the supplier signs before sampling begins. At minimum, this spec sheet must include: viscosity method (spindle, speed, temperature, equilibration time), pH method (instrument calibration standard, measurement temperature), appearance standard with a reference photograph, microbial acceptance criteria aligned with EU Cosmetics Regulation 1223/2009 Annex I, and a PET frequency commitment (lot 1, then annually).
Attach a PET report requirement directly to your purchase order terms — not as a separate request, but as a release condition. If it’s not in the PO, it’s optional from the supplier’s perspective.
The document to request at qualification stage: a filled, redacted batch manufacturing record from a previous commercial production run (not a lab batch). What you’re looking for is evidence that the formula has been scaled, that in-process controls exist, and that the supplier understands the difference between a development batch and a 500 kg production run. That gap is where most moisturizer & cream failures originate.
For brands positioning in the barrier repair or sensitive skin segment specifically, add a skin compatibility test requirement — repeated insult patch test (RIPT) or HRIPT with n ≥ 100 subjects — to the spec. A 2019 controlled clinical study (n=54, 8 weeks, split-face RCT design) comparing two ceramide-containing cream formulations showed that the batch with verified emulsifier purity had a 28% lower transepidermal water loss (TEWL) reading at week 8 versus the batch where emulsifier grade was unverified. The formulas were nominally identical. The difference traced back to a polysorbate 60 grade substitution that passed the COA but altered the lipid membrane interaction profile.
That is not a formulation story. It’s a supplier qualification story.
Formulation Notes for Brand Partners #
When you brief us on a moisturizer or cream project, the first questions we ask are not about texture or fragrance. What market is this for? EU, US, or NMPA China registration? What’s the on-pack efficacy claim — moisturizing, anti-aging, barrier repair? And what packaging format have you committed to, because the packaging choice changes almost everything about how we qualify the fill.
The brief mistake we see most often: brands come in with a competitor product they want to match, a nicely formatted COA from a previous supplier, and a request to “use this as the starting point.” A COA from another factory is not a formulation brief. It tells us what the product was, not how it was made, and it tells us nothing about whether it was stable, efficacious, or compliant in your target market. We always redirect this conversation toward a target product profile with specific performance thresholds — TEWL reduction, viscosity range, sensory descriptor set — rather than reverse-engineering someone else’s certificate.
Timeline: lab samples in 2–3 weeks from approved brief, accelerated stability at 40°C/75% RH over 4–8 weeks, with 24-month real-time stability initiated concurrently. For new supplier qualifications, add 3–4 weeks for independent PET and HPLC verification before we recommend a production commitment.
Frequently Asked Questions #
Can I accept a supplier’s own COA without running independent tests?
A: For the first three lots from any new supplier, independent retesting of pH, viscosity, and microbial count is non-negotiable from our standpoint. After a track record of 10+ conforming lots, you can reasonably reduce the frequency — but never eliminate the PET requirement entirely.
We’re launching into the EU — what specific micro limits apply to our cream?
A: Under EU Cosmetics Regulation 1223/2009, finished cream must meet ≤1,000 CFU/g total aerobic count, ≤100 CFU/g for combined yeast and mould, and absence of S. aureus, P. aeruginosa, and C. albicans in 1g or 1ml. These are the release limits — but the PET under ISO 11930 is what proves the preservative system will maintain those levels through shelf life, which is what EU authorities actually audit when a product is challenged.
We had phase separation at month four of a previously stable sample. What happened?
A: This almost always comes back to one of three things: emulsifier grade or ratio changed in a production lot, a thickener substitution happened silently, or packaging barrier failed and allowed moisture ingress that disrupted the aqueous phase. Pull the BMR from that production lot and compare it against the qualification batch — specifically processing temperature during emulsification, because a 5°C drop in homogenization temperature is enough to produce an ostensibly normal batch that fails rheologically within 12 weeks at ambient storage.
What’s your MOQ for a qualification run, and how long does it take?
A: Qualification pilot batches typically run at 30–50 kg to produce sufficient material for stability, PET, and third-party assay verification. From brief sign-off to qualification sample delivery: 2–3 weeks. Full qualification including accelerated stability: 10–14 weeks. Production MOQ for a standard cream SKU is generally 500 kg, though this varies by formula complexity and fill format.
Should we require a RIPT or HRIPT before launch, or is the supplier’s safety assessment enough?
A: It depends on your claim and your channel. A plain moisturizer going into a mid-market online channel might clear on a supplier safety dossier alone. A “sensitive skin” or “dermatologist-tested” positioning — or anything going into a pharmacy retail channel in Germany or France — will need an HRIPT with a minimum of 100 subjects to support the claim credibly and to satisfy retailer due diligence. The SCCS Scientific Opinion framework increasingly informs what retailers in those markets consider adequate substantiation, even when it’s not legally mandated. We flag this early in every brief because it affects both timeline and budget significantly.
Have a product concept in mind? Contact our formulation team to request a complimentary brief review.
