Pigmentary Disorders Introduction😊

Pigmentary Disorders Introduction

Include all disorders associated with pigmentation.

Terms:

Hypopigmentation:

Decrease or little loss of pigmentation.

Depigmentation:

No pigment;
complete absence.

Hyperpigmentation:

Increase in pigmentation.

Fitzpatrick scale grades skin types (1 to 6):

Type 6: Black.

Always tans.
Never burns.

Type 1: Very fair.

Tends to burn.
Never tans.

Melanin and Skin Colour

Melanocytes transfer melanin via melanosomes to 36 keratinocytes.

Called the epidermal melanin unit.

Skin colour is not dependent on melanocyte number.

Melanin types:

Eumelanin:

Brown or black.
Protective.
Helps to tan, protects from sunburns.

Pheomelanin:

Orangish or yellowish.
More in lighter skin types.
Not protective.
Causes burning.
Mnemonic: Fo means fake (not helping).

Skin colour depends on:

Type of melanin.

Number of melanosomes.

Distribution of melanosomes.

Mnemonic: Solely depends on somes

Patients with light skin:

Melanocytes present in clusters.

Patients with dark skin:

Individual melanosomes are larger.

Hyperpigmentary Disorders

Cafe au Lait Macule (CALM)

Hyperpigmented lesion: Single or multiple.

"Coffee on milk".

Present at birth.

Typically has a serrated border.

Basic defect: Increased number of melanosomes.

Mnemonic: Cafe () coffee (Coffee on milk) → In Coast of California and Maine ()

Types:

Regular and well-demarcated margins / Smooth border:

Called Coast of California.
Usually seen in NF1.

Irregular margins/ Rough border:

Called Coast of Maine.
Classic feature of McCune-Albright syndrome
Usually seen in segmental pigmentary disorders.

Can be present in Leopard syndrome or Tuberous Sclerosis.

Acquired Melanocytic Nevi (Moles)

Commonly seen on faces and other body parts.

Defect: Some proliferation of nevi cells in the epidermis.

Types:

Junctional nevi:

Nevi cells proliferating at dermo-epidermal junction.
Black in colour and more flat.
Highest tendency to turn into a melanoma among acquired melanocytic nevi.

Dermal nevi:

Nevi cells in the dermis.
Actually skin-coloured or lightly coloured.

Compound nevi:

Present in both junction and dermis.
More raised and hyperpigmented.
Not as black as junctional nevi.

Congenital Melanocytic Nevi

Usually present at birth.

Usually single lesions.

Associated with hypertrihosis

excessive hair growth

Rubosities are present.

Large congenital nevi

covering whole/part of trunk

Called bathing trunk or garment nevi.

High tendency to develop into a melanoma.

Note:

Becker's nevi

hypertrihosis at adolescence, not birth.

Dermal Melanocytic Nevi

Pigment in dermis appears bluish due to Tyndall effect.

Smaller wavelengths (violet/indigo) reflected.
(Epidermal → brown)

Mongolian Spots:

Bluish spot, usually in sacral area.

Typically seen in Mongoloid races.

Present at birth.

till 2 years

No treatment needed

Nevus of Ota:

Bluish lesions in conjunctiva and forehead

Unilateral.

Also called Nevus fuscoceruleus ophthalmo-maxillaris.

More common in Japanese population.

Present along ophthalmic and maxillary division of trigeminal nerve.

Associated with scleral deposits of pigmentation.

Mnemonic: Otta kannu

Nevus of Ito:

Bluish lesions.

Present along acromial and clavicular nerve distribution (branches of brachial nerve).

Will be on shoulders and upper back.

Also called Nevus fuscoceruleus acromio-clavicularis.

All dermal melanocytic nevi are asymptomatic lesions.

Nevus of Ota and Nevus of Ito

Treated using lasers.

Alexandrite

Ruby

Q-switched Nd : YAG (pigment-specific).

Melasma

Melasma → Most common pigmentary disorder → photoexposed areas → Sun exposure, Pregnancy (chloasma), OCP use, Hypothyroidism → Always hyperpigmented macules → Sunscreen is a must → Topical depigmenting agents → Triple combination cream (Hydroquinone (depigmenting),Tretinoin (exfoliating),Mild steroid )→ Kligman's formula → Oral Tranexamic acid → Q-switched Nd:YAG

Classical predisposing factors:

Sun exposure.
Pregnancy (chloasma).
OCP use.
Hypothyroidism.

ESTROGEN

Most common pigmentary disorder.

Typically in photoexposed areas.

Pathogenesis:

Melanocytes become

hyperactive
larger
more dendritic
produce more melanin

Presentation

Always hyperpigmented macules.

Asymptomatic.

Types (based on site):

Centrofacial.

Malar.

Mandibular.

Types (based on depth of pigmentation):

Types	Appearance
Epidermal melasma	Mainly epidermal.
Dermal melasma	Mainly dermal, appears bluish.
Mixed melasma	Both epidermal and dermal.

Diagnosis/Differentiation:

Wood's lamp.

Treatment:

Sunscreen is a must

Topical depigmenting agents:

Hydroquinone.
Kojic acid.
Arbutin.
Glycolic acid.

Triple combination cream:

Kligman's formula.
Combines:

Hydroquinone (depigmenting).
Tretinoin (exfoliating).
Mild steroid (hydrocortisone, for inflammation).

Oral treatment:

Tranexamic acid (also topical).

Peels:

Glycolic acid, lactic acid, others.

Lasers:

Mostly Q-switched Nd:YAG or other pigmentary lasers.

Depigmentary/Hypopigmentary Disorders

Nevus Depigmentosus

Is stable:

Does not increase in size

(only proportional to body growth).

Type of nevi with depigmented to hypopigmented macule.

Present since birth (congenital).

Commonly confused with vitiligo.

Unlike vitiligo:

Usually a single lesion.

Present since birth.

Localized to one area.

Does not grow/spread.

Totally asymptomatic.

Nevus Anemicus

Presents with depigmented lesion.

A pharmacological nevi

not congenital
Capillaries hyper-responsive to catecholamines:

Leads to vasoconstriction and pale appearance.

Differentiation from Nevus Depigmentosus:

Test: Diascopy

blanch with glass slide

When blanched, further vasoconstriction.

Margins will merge with normal surrounding skin.

Margins will not change.

Not dependent on vasoconstriction.

Albinism

A congenital disorder.

Universal absence of eumelanin synthesis.

Skin, hair, and eyes all affected.

Also called "albino kids".

Types:

Ocular Albinism:

Affects just the ocular area.
X-linked recessive.

Oculocutaneous Albinism (OCA):

Autosomal recessive.
Kids are also called albino kids.

Further divided:

Tyrosinase negative (OCA1):

No tyrosinase (important for eumelanin synthesis).
Patient will never have pigmentation.

Tyrosinase positive (OCA2):

Some tyrosinase activity.
At birth, complete pigment loss from hair, eyes, skin.
Gradually patient will get some pigmentation.

Complications:

Since melanin is protective, OCA patients are prone to:

Sunburn.
Seborrheic keratosis.
Skin cancers.
Malignancies.

Genetic disorder with no treatment.

Piebaldism

Inherited in an autosomal dominant pattern.

Defect:

Mutation in the KIT gene on chromosome 14.

Mnemonic:

Bald → dominant → father to son

when 14 yr old (CHr 14)

Pie → Need KIT (KIT gene) to make

Clinical Features:

Isolated congenital leukoderma or white skin.

Typically present in a distinct ventral midline pattern.

Classical features

Pie-shaped area of depigmentation

Typically present in median and paramedian area.

islands of sparing/normal pigmentation.

white hair or poliosis.

Differentiation from other syndromes:

NOTE:

Medial canthi → far apart
Interpupillary distance → normal

ㅤ	Waardenburg Syndrome
ㅤ	• White forehead • Piebaldism + • Dystopia canthorum • Cochlear deafness. • Heterochromia iridis. Bald (Piebald) ayittulla Wardernu (Wardenburg) Vote kodutha Aarada (Vogt Harada)
ㅤ	Vogt Koyanagi Harada (VKH) Syndrome:
CF	• Granulomatous Panuveitis
Age	• Third or fourth decade
Signs	• Sunset glow fundus • Perilimbal Vitilligo: Suiguira sign
3 Phases	1. Meningoencephalitic phase (Distinguished) 2. Uveitis and Choroiditis (Distinguished) 3. Leukoderma, poliosis, and alopecia
ㅤ	Sympathetic ophthalmitis
CF	• Granulomatous Panuveitis
Signs	• Retrolental Flare • Dalen Fuchs nodules
Pathology	ㅤ
↳ Exciting Eye	• Eye that sustains initial injury. • Penetrating Trauma • Affecting ciliary body
↳ Sympathizing Eye	• The fellow eye, not initially injured. • Develops after 2 weeks (>2 weeks) from initial trauma.
Treatment	• Steroids
Prevention	• Enucleation of the traumatic eye within 14 days

Granulomatous Panuveitis seen in

Sympathetic Ophthalmitis
VKH syndrome

Wardenberg syndrome

Wartenburg sign

Involuntary abduction of little finger at rest
Loss of hypothenar function → Digiti minimi

Wartenburg syndrome

Radial cutaneous nerve
Also called Cheiralgia paresthetica.
Both Warts in Hand

Type	Cause
Posterior	• Lowe syndrome ↳ Oculo Cerebro Renal syndrome • Opacity at posterior capsule center
Anterior	SAW Spina bifida Alport syndrome Waardenburg syndrome

Fuchs heterochromia iridocyclitis
• R eye normal
• L hypochromic eye affected — **Fuchs heterochromia iridocyclitis**
• R eye normal
• L hypochromic eye affected

Fuchs Terms	Notes
Fuchs heterochromia iridocyclitis	Chronic AU ⇒ • U/L Diffuse Iris atrophy + Heterochromia + Posterior SCC • Painless, No redness, No posterior synechiae Positive Amsler's Sign: ◦ Bleeding into Anterior chamber on paracentesis ◦ Without trauma to Iris/Angle ◦ D/t abnormal fragile Iris Stellate Keratin Precipitates ↳ Herpetic uveitis ↳ Toxoplasmosis ↳ Fuchs Heterochromia Iridocyclitis • Young stella → Fucked () by Toxic () Herpes () Guy
Dalens Fuchs	• Seen in Sympathetic ophthalmitis ↳ (granulomatous panuveitis) • Dalen Fucked Granny () sympathetically ()
Foster Fuchs	• In Pathological Myopia • Bleeding at macula • Fucking in Foster () home ↳ Blind child (Pathological myopia) ↳ Bled (Bleeding at macula)
Fuchs Endothelial dystrophy	• Cornea guttata: • Wart-like excrescences on posterior cornea • Fuck her Guts→ endothelial Stages • Stage 1: Central corneal guttata that spreads peripherally • Stage 2: Corneal oedema - beaten metal-like appearance • Stage 3: Bullous keratopathy • Stage 4: Subepithelial scarring and superficial vascularization

Vitiligo

T-cells mediated autoimmune destruction of melanocytes → melanocytopenia.

Has a positive family history (20-30%).

Presents with depigmented macules.

Asymptomatic.
Not raised.

Commonest association:

Thyroiditis

especially Hashimoto's thyroiditis.

Pernicious anemia, Type 1 DM, others.

Theories for pathogenesis:

Genetic disorder:

Defect in catalase gene.

Immune hypothesis:

Autoimmune disorder.

Neural hypothesis:

Certain neurotransmitter causes melanocytopenia.
Especially true for segmental vitiligo.

Autotoxic, self-destructive, or free radical hypothesis:

Products self-destroy, leading to loss.
Depigmented macules + leukotrichia or white hair.

Levels of pigmentation:

Trichrome vitiligo:

Three layers (depigmented, hypopigmented, hyperpigmented).

Quadrichrome vitiligo:

Four zones (trichrome + perfollicular pigmentation).

Shows positive Koebner phenomenon (isomorphic phenomena).

Types:

Segmental Vitiligo:

Probably neurogenic hypothesis holds true.

Neural hypothesis:

Certain neurotransmitter causes melanocytopenia.
Especially true for segmental vitiligo.

Has a stable course;

usually does not spread.
Intially grows → then stops progressing
Does not show Koebner phenomenon.

Presentation

Since childhood.
Depigmented lesion
along a segment or dermatome.

A/w leukotrichia.

Treatment

Does not respond to medical treatment.

Usually requires surgical treatment.

Non-Segmental Vitiligo:

Focal:

Single or two-three lesions in a foci, or just mucosal vitiligo.

Generalized or Diffused:

Three forms:

Vitiligo Vulgaris:

Bilateral symmetrical depigmented lesions.

Acro facial Vitiligo/ Lip tip variant:

Acral areas (hands, feet, face),
mucosal involvement.
Poor prognosis, poor treatment response.

Vitiligo Universalis:

Almost >90% of body surface area depigmentation.

Repigmentation difficult;

Monobenzyl ether of hydroquinone (MBH)

Reverse treatment
used for depigmenting.
Causes depigmentation of remaining 10%.

Treatment:

General treatment:

Topical agents: Localized disorder

Topical tacrilimus
Corticosteroids,
topical calcineurin inhibitors.

Avoiding Koebner phenomenon.

Avoid trauma, rubber chappals, any trauma.

Topical phototherapy.

Phototherapy:

NB-UVB, PUVA, excimer lasers (targeted).

Medical treatment:

Systemic agents:
Steroids.
Cyclophosphamide.
Azathioprine.
Levamisole.
JAK inhibitors: Tofacitinib.

Surgical treatments:

For stable patches not repigmenting.

An 18-year-old female patient arrives with a hypopigmented patch and feathery edge on the medial part of her foot. The rest of the physical exam goes as expected. Which medication from the list below should be avoided when treating this patient?

Topical tacrolimus

Clobetasol

Isotretinoin

PUVA

Ans

Isotretinoin: Used for acne; not for vitiligo.

Contraindicated in young females → teratogenic risk.

Vitiligo treatment options

Topical steroids
Calcineurin inhibitors
Phototherapy (NB-UVB, PUVA)
Surgical grafting (for stable vitiligo)

Chemical Leukoderma

Presents similar to vitiligo.

Lesions in area exposed to a chemical.

Depigmented patches at site of contact.

Common examples and agents:

Item	Agent	Effect
Rubber chappals	Monobenzyl ether of hydroquinone (MBH)	Causes depigmentation.
Bindi	Para tertiary butyl phenol (PTBP)	Causes bindi dermatitis and leukoderma. Mnemonic: BP kudiyapo bindi ittu
Hair dye	Para tertiary butyl catechol (PTBC) Para phenylenediamine (PPD)	Can lead to hair dye induced depigmentation. Busy (PTBC) ayapo → dye () cheythu but parupadi (PPD → allergy) ethiyapo allergy adichu

NOTE:

ㅤ	Waardenburg Syndrome
ㅤ	• White forehead • Piebaldism + • Dystopia canthorum • Cochlear deafness. • Heterochromia iridis. Bald (Piebald) ayittulla Wardernu (Wardenburg) Vote kodutha Aarada (Vogt Harada)
ㅤ	Vogt Koyanagi Harada (VKH) Syndrome:
CF	• Granulomatous Panuveitis
Age	• Third or fourth decade
Signs	• Sunset glow fundus • Perilimbal Vitilligo: Suiguira sign
3 Phases	1. Meningoencephalitic phase (Distinguished) 2. Uveitis and Choroiditis (Distinguished) 3. Leukoderma, poliosis, and alopecia
ㅤ	Sympathetic ophthalmitis
CF	• Granulomatous Panuveitis
Signs	• Retrolental Flare • Dalen Fuchs nodules
Pathology	ㅤ
↳ Exciting Eye	• Eye that sustains initial injury. • Penetrating Trauma • Affecting ciliary body
↳ Sympathizing Eye	• The fellow eye, not initially injured. • Develops after 2 weeks (>2 weeks) from initial trauma.
Treatment	• Steroids
Prevention	• Enucleation of the traumatic eye within 14 days

Granulomatous Panuveitis seen in

Sympathetic Ophthalmitis
VKH syndrome

Wardenberg syndrome

Wartenburg sign

Involuntary abduction of little finger at rest
Loss of hypothenar function → Digiti minimi

Wartenburg syndrome

Radial cutaneous nerve
Also called Cheiralgia paresthetica.
Both Warts in Hand

Type	Cause
Posterior	• Lowe syndrome ↳ Oculo Cerebro Renal syndrome • Opacity at posterior capsule center
Anterior	SAW Spina bifida Alport syndrome Waardenburg syndrome

Fuchs Terms	Notes
Fuchs heterochromia iridocyclitis	Chronic AU ⇒ • U/L Diffuse Iris atrophy + Heterochromia + Posterior SCC • Painless, No redness, No posterior synechiae Positive Amsler's Sign: ◦ Bleeding into Anterior chamber on paracentesis ◦ Without trauma to Iris/Angle ◦ D/t abnormal fragile Iris Stellate Keratin Precipitates ↳ Herpetic uveitis ↳ Toxoplasmosis ↳ Fuchs Heterochromia Iridocyclitis • Young stella → Fucked () by Toxic () Herpes () Guy
Dalens Fuchs	• Seen in Sympathetic ophthalmitis ↳ (granulomatous panuveitis) • Dalen Fucked Granny () sympathetically ()
Foster Fuchs	• In Pathological Myopia • Bleeding at macula • Fucking in Foster () home ↳ Blind child (Pathological myopia) ↳ Bled (Bleeding at macula)
Fuchs Endothelial dystrophy	• Cornea guttata: • Wart-like excrescences on posterior cornea • Fuck her Guts→ endothelial Stages • Stage 1: Central corneal guttata that spreads peripherally • Stage 2: Corneal oedema - beaten metal-like appearance • Stage 3: Bullous keratopathy • Stage 4: Subepithelial scarring and superficial vascularization