The quick answer

What this symptom may mean

Persistent adult acne in U.S. women — particularly along the jawline, chin, and lower face — is more often hormonally driven than skin-care driven. The dominant pattern is androgens (testosterone in particular) acting on sebum-producing glands, frequently with insulin and IGF-1 amplifying the signal. Cycle-tied flares are common; a baseline that doesn't clear with topical care is the louder signal.

Common biomarker patterns

Elevated free testosterone with a low or normal SHBG; elevated DHEA-S indicating adrenal contribution; fasting insulin creeping up before HbA1c; a thyroid panel worth checking on the same draw; and vitamin D often low. PCOS sits underneath a meaningful share of persistent adult acne in women.

What to ask your provider

Ask for total and free testosterone, SHBG, DHEA-S, fasting insulin and HbA1c, a thyroid panel, and vitamin D. If a PCOS picture is on the table, mid-luteal progesterone and an ultrasound conversation belong with a clinician. Borderline values are worth a conversation, not a dismissal.

What's typically going on.

Acne is, at its core, a sebaceous gland story. The glands that produce skin oil are studded with androgen receptors. When androgens — testosterone in particular — bind those receptors more strongly, the glands produce more oil, the lining of the pore turns over faster and stickier, and the bacterial layer that lives in every pore (Cutibacterium acnes) gets more of what it likes to feed on. Inflammation follows. That whole cascade is downstream of androgen signalling, and androgen signalling is downstream of measurable inputs.

The most useful number in adult female acne is rarely total testosterone. It is free testosterone — the unbound, biologically active fraction — read alongside SHBG, the protein that binds it. A normal-looking total can hide a high free if SHBG is low. SHBG falls with insulin resistance and certain endocrine conditions, and rises with combined oral contraceptives and oral estrogen. The same lab pattern that drives weight gain and energy crashes — high insulin, low SHBG — also tends to drive acne. They are not separate problems.

Insulin and the insulin-like growth factor IGF-1 sit one layer above. Higher circulating insulin tends to lower SHBG (raising free testosterone) and tends to amplify the proliferation of cells lining the pore. This is part of why high-glycemic diets and, in some women, dairy intake correlate with acne severity in observational studies. It is also part of why women with PCOS — a condition defined by insulin resistance and hyperandrogenism — have such a strong overlap with persistent adult acne.

The adrenals contribute too. DHEA-S is the adrenal androgen marker most worth knowing, and elevated DHEA-S can drive acne even when ovarian androgens look normal. Chronic stress and chronic sleep loss both push adrenal output in unhelpful directions. Thyroid dysfunction can sit in the picture too, often through skin barrier and hormonal-axis effects rather than directly.

The cycle matters. Most adult women with hormonal acne notice a luteal-phase flare — the second half of the cycle, when progesterone rises and estrogen falls relative to the first half. This is normal cyclical variation amplifying baseline susceptibility. If the baseline is acne-prone, the luteal flare is louder. If the baseline is calmer, the luteal flare is barely there. Bloodwork is most useful when it helps separate the cyclical flare layer (manageable) from the baseline susceptibility layer (the one that actually needs measurement).

"Persistent adult acne in women is rarely a skincare problem. It's an androgen problem that hasn't been measured."

The biomarkers most worth knowing.

You do not need every marker on this list to start. You need enough to see the androgen-and-insulin story underneath. Read together by a qualified healthcare provider — ideally an OB-GYN, women's-health NP or endocrinologist who treats PCOS — the following panel catches most of the measurable drivers of persistent adult acne.

Total & free testosterone
The androgen most closely tied to acne. Free testosterone — unbound, biologically active — is the more informative number. A normal total can hide a functionally high free if SHBG is low.
SHBG
Sex hormone-binding globulin. Falls with insulin resistance and PCOS; rises on combined oral contraceptives. Low SHBG mechanically raises free testosterone — worth measuring rather than guessing.
DHEA-S
Adrenal androgen precursor. Elevated DHEA-S can drive acne even when ovarian androgens are normal. Worth running alongside testosterone to localise the source.
Fasting insulin & HbA1c
Fasting insulin moves before glucose or HbA1c when insulin resistance is developing. Higher insulin tends to lower SHBG and raise free testosterone — a key mechanism in PCOS-associated acne.
TSH & full thyroid panel
Thyroid dysfunction can affect skin barrier, healing and the hormonal axis. Worth on the same draw rather than chased separately later.
Vitamin D (25-OH)
Influences immune signalling and inflammation. Often low in U.S. women, and worth replacing to within an optimal range rather than just "above deficiency."
Mid-luteal progesterone
A mid-luteal sample (roughly day 21 of a 28-day cycle) confirms whether a cycle ovulated. Anovulatory cycles raise PCOS suspicion when combined with elevated androgens.

None of these is useful as a single isolated number. A clinician who reads an elevated free testosterone with low SHBG, raised fasting insulin and persistent jawline acne is in a very different conversation from one who reads only "total testosterone normal."

Common patterns.

The PCOS pattern

Persistent jawline and chin acne in a woman in her 20s or 30s, alongside irregular cycles (or apparently regular cycles in lean-phenotype PCOS), thicker hair on the face, thinning on the scalp, and a tendency toward weight that's hard to shift. Free testosterone elevated, SHBG low, fasting insulin elevated, DHEA-S sometimes elevated. This is the highest-volume pattern behind persistent adult acne in women, and it is worth raising explicitly with a qualified clinician — the diagnosis matters because the treatment shifts.

The adrenal-androgen pattern

Acne that flares with stress, alongside otherwise unremarkable ovarian androgens but elevated DHEA-S. Sometimes seen in women on long-term oral contraception when they stop (the so-called post-pill picture) and in women under chronic stress with poor sleep. The treatable layer here is the adrenal-stress axis as much as the skin itself.

The cycle-tied flare pattern

A relatively calm baseline with a reliable luteal-phase flare — chin breakouts the week before the period, calmer once the period starts. Bloodwork may look unremarkable. This is normal cyclical variation; the conversation is more about topical and hormonal options than about a missing biomarker.

The perimenopausal pattern

Acne arriving (or returning) in the late 30s or 40s, often alongside other perimenopausal signals. Falling estradiol shifts the androgen-to-estrogen ratio toward androgen-dominant skin behaviour, even when absolute androgens haven't changed. Worth reading alongside the perimenopause hub.

What to ask your provider.

Eight questions worth bringing to the appointment.

  • Can we run total and free testosterone with SHBG and DHEA-S — the full androgen panel?
  • Can we measure fasting insulin alongside glucose and HbA1c?
  • Given my cycle and skin pattern, is PCOS on the table as a diagnosis?
  • If I'm on combined oral contraception, what would happen to my labs and skin if I stopped?
  • Can we add a full thyroid panel and vitamin D to the same draw?
  • Is mid-luteal progesterone worth measuring to confirm ovulation?
  • What's your view on dietary and lifestyle levers for insulin sensitivity in my picture?
  • When should we re-test, and what would prompt earlier follow-up?

These are not a script. Your clinician will steer the conversation where it is most useful. They are a starting point that tends to widen the panel and sharpen the interpretation.

When to escalate vs when to track over time.

Most adult acne in women is worth a planned dermatology and/or women's-health conversation rather than an urgent visit. A few exceptions warrant a faster timeline.

Worth a planned conversation. Persistent acne over six months that doesn't respond to first-line topical care; cycle-tied flares with a calm baseline; perimenopausal acne arriving alongside other transition signals. Bloodwork on a calm timeline; re-test in three to six months after any intervention.

Worth sooner. Sudden, severe acne that is new in adulthood — particularly alongside rapid hair growth on the face, deepening voice, or rapid weight changes — warrants prompt endocrine evaluation. Same with scarring nodular or cystic acne that is causing significant distress; that belongs with a dermatologist on a shorter timeline.

Worth tracking, not panicking. A borderline lab in someone with otherwise mild, manageable acne is rarely the whole story. Trending the same markers six to twelve months apart gives a more honest picture than a single snapshot.

Frequently asked.

Is adult acne always hormonal?
Most persistent adult acne in women has a hormonal component, but the upstream drivers differ. Elevated free testosterone, low SHBG, insulin resistance, PCOS, and the perimenopausal androgen-to-estrogen ratio shift are all measurable. Skin care alone often does not move acne that is hormonally driven; the relevant labs do.
Which biomarker should I ask for first?
Total and free testosterone with SHBG is the most informative starting point. Adding DHEA-S, fasting insulin and HbA1c on the same draw catches the PCOS and insulin-resistance picture that often sits underneath persistent jawline and chin acne in adult women.
Could this be PCOS even if my cycles seem regular?
Yes. Cycles can be ovulatory and apparently regular in some women with PCOS, particularly those with the lean PCOS phenotype. Persistent jawline and chin acne, hair changes (more on the face, thinning on the scalp), and elevated free testosterone or DHEA-S are worth raising with a qualified healthcare provider — diagnosis criteria allow for variation in cycle pattern.
Why does my acne flare in the second half of the cycle?
In the luteal phase, progesterone rises and estrogen falls relative to the first half of the cycle, which can shift the androgen-to-estrogen balance toward acne-prone settings. This is normal cyclical variation, but if it overlaps with persistent baseline acne, both layers may be worth measuring rather than only treating the flare.
Does diet really affect acne?
Insulin and IGF-1 are part of the acne pathway. High glycemic loads and, in some women, dairy can raise insulin and IGF-1 enough to influence acne. Diet is rarely the only lever, but if fasting insulin is elevated, addressing it through a clinician-guided plan may matter for skin alongside everything else.
Will going off the pill make my acne worse?
Often, yes — temporarily. Combined oral contraceptives raise SHBG, lowering free testosterone for the duration of use. Stopping can produce a rebound flare as SHBG falls and free testosterone rises. The flare typically settles over 6–12 months, but worth raising with a clinician before stopping rather than after.

Selected references

  1. American Academy of Dermatology — Adult acne in women: clinical guidelines. [Source required: AAD guideline document.]
  2. The Endocrine Society — PCOS clinical practice guideline. [Source required: Endocrine Society 2023 update.]
  3. American College of Obstetricians and Gynecologists — Hyperandrogenism in adolescents and women. [Source required: ACOG Practice Bulletin.]
  4. Journal of the American Academy of Dermatology — Hormonal therapy in adult female acne. [Source required: peer-reviewed review article.]
  5. Office on Women's Health, U.S. Department of Health and Human Services — Skin and hormones. [Source required: OWH fact sheet.]

Educational only. Not medical advice. This hub is general health education and is not a substitute for personal medical advice, diagnosis or treatment. Always speak with a qualified healthcare provider about symptoms, lab results, supplement choices or treatment decisions — particularly if you are pregnant, breastfeeding, take medication, or have an existing medical condition. See our methodology for how we research and review.