Vesiculopustular and erosive disorders in newborns and infants

Question 1

Epidemiology of erythema toxicum neonatorum?

Answer 1

Half of full term infants, >2500g; M=F

Question 2

Ddx for eosinophilic spongiosis?

Answer 2

HAAPPIED H: Herpes Gestationis A: Arthropod Allergic contact P: Pemphigus, Pemphigoid, I: Incontinentia pigmenti, ETN Drug reaction

Question 3

Timing for Erythema toxicum neonatorum?

Answer 3

24-48 hours after birth usually but can be seen from birth to 2 weeks.

Question 4

Clinical presentation of Erythema toxicum neonatorum?

Answer 4

Erythematous macules, papules, pustules, and wheals.

DOES NOT OCCUR ON PALMS AND SOLES

Question 5

Histology of Erythema toxicum neonatorum?

Answer 5

Subcorneal and intrafollicular eosinophilic pustules (wright’s stain of pusutles = eos)

Question 6

The clinical course of Erythema toxicum neonatorum?

Answer 6

Self limited, resolves over several weeks

Question 7

What systemic lab findings can be seen in Erythema toxicum neonatorum?

Answer 7

Peripheral blood sample can show eosinophilia

Question 8

Epidemiology of Transient Neonatal Pustular Melanosis?

Answer 8

Term infants, MC in blacks (~5% of darkly pigmented newborns)

Question 9

Timing of Transient Neonatal Pustular Melanosis?

Answer 9

Presents at birth or shortly after, but collarettes or hyperpigmentation can be a few days-weeks of age.

Question 10

3 stages of Transient Neonatal Pustular Melanosis?

Answer 10

1. Pustules w/o underlying erythema
2. Collarettes of scale
3. Hyperpigmentated macules

Question 11

Most common distribution of Transient Neonatal Pustular Melanosis?

Answer 11

MC on forehead, back, fingers and toes

Question 12

Histology of Transient Neonatal Pustular Melanosis?

Answer 12

• Subcorneal pustules w/ neuts, fibrin, and rarely eosinophils
• Wright’s stain of pustule fluid: neutrophils

Question 13

Prognosis of Transient Neonatal Pustular Melanosis?

Answer 13

Self-limited and resolves over sever weeks

Question 14

Subcorneal pustules DDX

Answer 14

CAT PISS

Candida

Acropustulosis of infancy

Transient Neonatal Pustular Melanosis

Pustular psoriasis

Impetigo

Sneddon-Wilkinson (and IgA pemphigus)

Staph Scalded skin

Question 15

Epidemiology of miliaria crystallina?

Answer 15

15% of newborns

Question 16

Most common locations of Miliaria Crystallina?

Answer 16

Forehead, upper trunk, and arms

Question 17

Pathogenesis of Miliaria Crystallina?

Answer 17

Intracorneal obstruction of eccrine duct

Question 18

Timing of Miliaria Crystallina?

Answer 18

Neonates and infants (hx of fever and overheating usually)

Question 19

Clinical presentation of Miliaria Crystallina?

Answer 19

Fragile, clear-colored vesicles without underlying erythema

Self limited

Question 20

Timing of Miliaria Rubra?

Answer 20

After first week of life

Question 21

Pathogenesis of Miliaria Rubra?

Answer 21

Deeper intraepidermal obstruction of eccrine duct w/ inflammation

Question 22

Causes of Miliaria Rubra?

Answer 22

Hx of overwarming, fever, or use of occlusive dressing or garment

Question 23

Clinical presentation of Miliaria Rubra?

Answer 23

Erythematous papules w/ superimposed pustules typically concentrated in one or two areas

Question 24

Most common location of Miliaria Rubra?

Answer 24

Intertriginous/occluded sites (neck, groin, axilla) most commonly

Question 25

Histology of Miliaria Rubra?

Answer 25

Intraepidermal spongiosis and vesicles + chronic inflammatory infiltrate in dermis

Question 26

What is the epidemiology of Neonatal Cephalic Pustulosis?

Answer 26

Appears within the first few weeks, resolves by 3 months. 20% of healthy newborns. M>F

Question 27

Pathogenesis of Neonatal Cephalic Pustulosis?

Answer 27

• KOH may demonstrate Malassezia (subtype of neonatal acne, termed neonatal cephalic pustulosis)
• Other cases likely related to stimulation of sebaceous glands by maternal androgens or transient androgen production

Question 28

Clinical of Neonatal Cephalic Pustulosis?

Answer 28

Inflammatory papules and pustules more common than comedones on the cheeks and nasal bridge common, but may occur anywhere on face/head/neck

Question 29

Treatment for Neonatal Cephalic Pustulosis?

Answer 29

• Usually regresses over few months
• If mild, cleanse with gentle soap and water
• For more severe cases can consider ketoconazole cream or hydrocortisone 1-2.5% cream

If not regressing or if severe rule out neonatal acne

Question 30

What do you need to think about in a baby w/ trisomy 21 and neonatal cephalic pustulosis?

Answer 30

Could also be a leukemoid reaction that can manifest as a severe pustular eruption on the face, mimicking neonatal acne.

Question 31

Epidemiology of Infantile Acne?

Answer 31

Appears around 3-6mo, resolves by 2-3 years

M>F

Question 32

Pathogenesis of infantile acne?

Answer 32

Due to hormonal imbalance (hyperandrogenism)

This is not from the mother as is often hypothesized, from the infants own androgen production

Question 33

Clinical presentation of infantile acne?

Answer 33

• More severe and persistent compared with neonatal acne
• Comedones (primarily) and inflammatory lesions including occasionally deep cysts
• Can result in scarring
• Usually limited to the face

Question 34

Treatment for infantile acne?

Answer 34

• Therapy is often necessary due to risk of scarring
• Same options as neonatal acne
• If occurs between ages 1-7yo (mid-childhood acne) and signs of pubertal development are noted (pubarche, thelarche, etc) an endocrinology evaluation should be considered along with the following laboratory analysis: DHEAS, androstenedione, 17-OH progesterone, and bone age
• May predict propensity towards future acne

Question 35

Timing of Cutaneous Candidiasis?

Answer 35

Presents after first week of life

Question 36

Clinical presentation of cutaneous candidiasis?

Answer 36

• Pink-red patches w/ satellite papules and pustules that favor diaper area or other intertriginous sites and face
• Can often have oral thrush

Question 37

What is congenital candidiasis?

Answer 37

Less common than cutaneous candidiasis, candidiasis infxn in congenital infxn is acquired in utero

• Widespread vesiculopustular eruption, often involving palms and soles
• Nail dystrophy w/ yellowing and transverse ridging may be the only manifestation
• Characteristic yellow-white papules may be found on the umbilical cord

Question 38

What is invasive fungal dermatitis?

Answer 38

Occurs in very low birth weight premature newborns “Invasive fungal dermatitis”

Can present as “burn like” erythema w/ desquamation and erosions

Question 39

What are sucking blisters?

Answer 39

Occurs in 1 in every 250 newborns. Caused by vigorous sucking of the affected area in utero leading to Intact flaccid bullae, erosion, or superficial ulceration on non-inflamed base

• Isolated finding w/o associated issues
• Resolves over days to a week

Question 40

Distribution of sucking blisters?

Answer 40

Radial forearm, wrist, hands, fingers

Question 41

Epidemiology/onset of acropustulosis of infancy?

Answer 41

Onset is typically between birth and 2yo

It is most common in black infants boys

The etiology is unknown; some cases a/w preceding scabies infection

Question 42

What is the clinical presentation of acropustulosis of infancy?

Answer 42

Recurrent crops of vesiculopustules over the palms, soles, and distal extremities

Question 43

Smear findings for acropustulosis of infancy?

Answer 43

Neuts

Question 44

Treatment for acropustulosis of infancy?

Answer 44

Systemic antihistamines and high potency topical corticosteroids

Typically resolves spontaneously by 3yo

Question 45

Epidemiology and timing of Eosinophilic Pustular Folliculitis of Infancy?

Answer 45

Mean age of onset=6mo, M>F, presents at birth or days to weeks of age

Question 46

Clinical presentation of Eosinophilic Pustular Folliculitis of Infancy?

Answer 46

Waxing and waning course over months with recurrent crops of pustules that remit eventually may be pruritic.

The pustules and erythema mainly involves the scalp and face but occasionally the trunk and extremities

Question 47

Histology of Eosinophilic Pustular Folliculitis of Infancy?

Answer 47

Dense perifollicular mixed infiltrate w/ eosinophils

Question 48

Labs for Eosinophilic Pustular Folliculitis of Infancy?

Answer 48

Can show eosinophilia

Question 49

Prognosis of Eosinophilic Pustular Folliculitis of Infancy?

Answer 49

Resolves by 3 y/o

Question 50

Clinical of Congenital and Neonatal Langerhans Cell Histiocytosis?

Answer 50

Starts at birth to a few days after

Skin limited form, rapidly self-healing; widespread (>solitary) red or purple-brown papulonodules +/- erosions, crust, and resolves weeks later

Can develop anywhere including palms and soles

Question 51

Tests that need to be done in Congenital and Neonatal Langerhans Cell Histiocytosis?

Answer 51

R/o systemic involvement: PE, chem panel, LFT, CBC, Urine osmolality, abdominal US, Skeletal survey, CXR

Question 52

What is the histology of congenital and neonatal Langerhans cell histiocytosis?

Answer 52

There is a proliferation of Langerhans cells in the superficial dermis with large ovoid cells w/ coffee bean nuclei

stains + for s100, CD1a, langerin

Question 53

Genetics of Incontinentia pigmenti?

Answer 53

XLD loss of function mutation in nuclear factor-kappaB(NF-kB) essential modulator (NEMO;IKBKG)

Question 54

Pathogenesis of IP?

Answer 54

• Mutation in NEMO prevents activation of NF-kB, a regulator of cell proliferation, inflammation, and TNF-alpha induced apoptosis
• Mutation in lethal in males; seen primarily in women and XXY (Klinefelter’s) males
• Functional mosaicism from lyonization in affected females (random inactivation of affected X chromosome) results in blaschkoid pattern of cutaneous involvement.

Question 55

Clinical of IP?

Answer 55

IP is a neuroectoermal disorder that affects the skin, teeth (hypodontia/anodontia), CNS, and eyes

Cutaneous lesions are typically arranged in streaks and whorls, following blaschkoid pattern

Question 56

What are the 4 morphologic states of IP?

Answer 56

Vesicular, verrucous, hyperpigmented, and hypopigmented.

you can also see patchy scarring alopecia at the vertex, areas of wooly hair, nail dystrophy, and anhidrosis with atrophic linear streaks.

Question 57

What is the histology of the vesicular stage of IP?

Answer 57

Eosinophilic spongiosis; intraepidermal vesicles containing eosinophils; apoptotic keratinocytes in the epidermis

Question 58

Keys points of the histology for each stage of IP?

Answer 58

• Vesicular Stage: eosinophilic spongiosis; intraepidermal vesicles containing eosinophils; apoptotic keratinocytes in the epidermis
• Verrucous stage: papillomatosis, hyperkeratosis, and acanthosis of the epi; apoptotic cells in epi forming squamous eddies
• Hyperpigmented stage: marked pigment incontinence w/ numerous melanophages in the dermis; apoptotic cells may be seen in the epidermis
• Hypopigmented stage: epidermal atrophy, loss of melanin in the basal layer, the complete absence of pilosebaceous units and eccrine glands; apoptotic cells may be seen in the epidermis

Question 59

Can male babies be born with IP?

Answer 59

Generally not (x-linked and fatal to boy babies). However, women with missense mutations in NEMO (Milder phenotype of IP) can bear children (usually male) with hypohidrotic ectodermal dysplasia with immunodeficiency

Question 60

Other clinical findings in IP?

Answer 60

Severely affected patients may develop seizures, developmental delay, and intellectual impairment, and decreased visual acuity/blindness (due to retinal vascular changes and optic atrophy)

Question 61

Pathogenesis of Autosomal Dominant Hyperimmunoglobulin E (Hyper IgE) Syndrome

Answer 61

Primary immunodeficiency syndrome: AD, STAT3 mutations

–Signal transducer and activator of transcription 3 gene

Question 62

Clinical of Autosomal Dominant Hyperimmunoglobulin E (Hyper IgE) Syndrome

Answer 62

Mean onset: 7 days old, Neonatal Papulopustular + vesicular eruption w/ crusting of face, scalp, neck, axillae, diaper area

• Elevated serum IgE levels (>2000), peripheral eosinophilia, “cold” abscesses, eczematous dermatitis, recurrent infections
• AR variant: DOCK8 deficiency

Question 63

What is the most common organism to cause invasive fungal dermatitis in a neonate?

Answer 63

Candida albicans