HORMONES & SKIN AGEING – Aeternitas Cosmetics

The Biology of Hormonal Skin Behaviour

THE BIOLOGY OF HORMONAL SKIN AGEING

(How each hormone influences collagen, elasticity, inflammation, pigment, oil, and skin behaviour)

THE SKIN IS A HORMONE-DEPENDENT ORGAN

Hormones control nearly every visible change in the skin:

firmness
thickness
elasticity
inflammation
redness
oil activity
hydration
pigment
healing
sensitivity
texture
collagen and elastin production

When hormones shift, skin behaviour shifts immediately.

Page 5B explains each major hormone and its effect on the skin.

OESTROGEN — THE COLLAGEN-PROTECTOR

Oestrogen is the hormone most responsible for youthful skin.

It increases:

collagen production
elastin density
fibroblast activity
ECM hydration
hyaluronic acid
vascular health
wound healing
barrier strength
antioxidant protection

Oestrogen declines begin as early as age 32–35, accelerating from 40–55.

The consequences are dramatic:

30% collagen lost in the first 5 years of menopause
increased laxity
thinning dermis
crepey texture
slower healing
increased redness
deeper lines
under-eye collapse
neck ageing
mouth-area ageing

This is one of the biggest drivers of female structural ageing.

PROGESTERONE — THE SENSITIVITY HORMONE

Progesterone influences:

water retention
barrier function
oil activity
inflammation

Low progesterone (common from mid-30s onward):

increases sensitivity
increases inflammation
increases redness
weakens the barrier
increases dryness
increases irritation
worsens rosacea-type reactions

In perimenopause, progesterone fluctuations cause skin to feel “all over the place.”

TESTOSTERONE — THE STRUCTURAL & OIL HORMONE

Testosterone increases:

dermal thickness
collagen density
structural strength
jawline definition
muscle support under the skin
oil activity (sebum)

In women:

Low testosterone →

thinning skin
low glow
decreased firmness
reduced oil (dryness)
accelerated ageing

In men:

Testosterone decline (andropause) →

heavy sagging
deeper folds
sudden jawline loss

In transgender clients:

MTF (oestrogen therapy) →

testosterone falls
skin becomes more feminine, thinner, sensitive

FTM (testosterone therapy) →

oil increases
acne and inflammation may increase
increased collagen density over time

DHT (DIHYDROTESTOSTERONE) — THE JAWLINE BREAKOUT HORMONE

DHT is a derivative of testosterone and drives:

jawline acne
cystic breakouts
inflammation
scarring
oil overproduction

High DHT is common in:

men
women with hormonal imbalance
PCOS
FTM testosterone therapy
stress-driven androgen surges

It also causes:

deeper pores
thicker texture
stronger sebaceous glands
more stubborn inflammation

CORTISOL — THE STRESS HORMONE THAT ACCELERATES AGEING

Cortisol is one of the most destructive hormones for the skin.

It causes:

collagen breakdown
inflammation
redness
sensitivity
dehydration
slower healing
barrier disruption
pigmentation
increased vasodilation
worsening rosacea patterns
tired, flat skin

Long-term cortisol elevation

inflammageing + structural ageing + faster visible ageing

THYROID HORMONES — THE SKIN’S METABOLIC REGULATORS

Thyroid hormones (T3/T4) control:

cell turnover
hydration
microcirculation
barrier function
oil balance

Low thyroid (underactive):

dry skin
coarse texture
slow healing
puffiness
increased inflammation
dullness
poor circulation

High thyroid (overactive):

flushing
thinning skin
redness
sensitivity
accelerated ageing

INSULIN — THE SUGAR-INFLAMMATION HORMONE

High insulin levels:

increase inflammation
increase breakouts
drive pigmentation
contribute to PIH
worsen redness
accelerate collagen glycation (stiff, dull collagen fibers)

Glycation is a major cause of:

yellow undertones
reduced firmness
quicker ageing

This is seen across all genders and ethnicities.

GROWTH HORMONE (GH) — THE REPAIR & REGENERATION HORMONE

GH supports:

collagen synthesis
wound healing
cell turnover
structural rebuilding

GH declines from age 25 onward — reducing healing speed and collagen density.

PROLACTIN — A HIDDEN PIGMENT + INFLAMMATION HORMONE

High prolactin (stress, breastfeeding, medications) can cause:

pigmentation
uneven tone
inflammation
dullness
jawline breakouts

It is under-recognised but significant.

PERIMENOPAUSE — THE CHAOTIC HORMONE PHASE

Perimenopause causes:

fluctuating oestrogen
declining progesterone
increasing inflammation
increased sensitivity
unexpected breakouts
redness
inconsistent collagen production
accelerated structural ageing

Clients often describe:

“I don’t recognise my skin anymore.”

Fully rooted in hormonal fluctuation.

MENOPAUSE — THE COLLAGEN CRASH

At menopause:

oestrogen drops sharply
collagen drops rapidly
elastin declines
fat pads shift
ligaments weaken
SMAS loosens
dermis thins
sensitivity rises
pigment increases

This is the second-biggest change in female ageing after puberty.

ANDROPAUSE — MALE HORMONAL AGEING

Gradual testosterone decline causes:

structural heaviness
jawline sagging
deeper folds
thickened lower face ageing
oil reduction
dry surface texture

Men age later — but faster when decline begins.

TRANSGENDER HORMONE THERAPY — UNIQUE HORMONAL AGEING PATTERNS

MTF (male-to-female):

increased sensitivity
reduced thickness
reduced oil
increased pigment risk
more feminine ageing patterns
under-eye ageing increases
better barrier function

FTM (female-to-male):

increased oil
increased inflammation
higher acne risk
stronger collagen network
slower wrinkle development

Aeternitas must tailor settings accordingly.