Infantile acne

Infantile acne
Infantile acne
Other names	Neonatal cephalic pustulosis
Specialty	Dermatology

Infantile acne is a form of

pustules most commonly present on the face.^[3]^[4] No cause of infantile acne has been established but it may be caused by increased sebaceous gland secretions due to elevated androgens, genetics and the fetal adrenal gland causing increased sebum production.^[2]^[3]^[4] Infantile acne can resolve by itself by age 1 or 2. However, treatment options include topical benzyl peroxide, topical retinoids and topical antibiotics in most cases.^[5]

Signs and symptoms

Infantile acne has a later onset and is less commonly seen than neonatal acne, occurring between 6 weeks to 1 year of age. It is also more commonly seen in boys rather than girls.^[3] Infantile acne tends to be more inflammatory and wide spread than neonatal acne. It presents with both open and closed comedones, papules and pustules.^[3]^[6]^[4] Cystic lesions are uncommon. Scarring can occur in severe cases.^[7]^[8] Very rarely, facial conglobate acne, a severe form of acne that involves extensive inflammation and nodule formation can develop and lead to extensive scarring.^[3]^[4] Lesions occur most commonly on the cheeks but can also appear on the chest and back.^[4] More severe occurrences may lead to development of more severe forms of acne in adolescence.^[3]^[5]

Causes

The cause of infantile acne is not known for certain. Research into higher occurrence in boys rather than girls imply that higher than normal levels of testicular androgens can cause increased sebaceous gland secretions.^[4] During the first 6–12 months of age, there is increased sebum production stimulated by luteinizing hormone (LH) and testosterone of testicular origin that stops after this period until adrenarche. Girls do not experience this.^[2]^[3]

Genetics and family history play a role in influencing sebaceous gland size and activity, pore size and inflammation that can increase risk of onset and presentation of infantile acne.^[3]^[4]

It is suggested that the fetal adrenal gland along with testicular androgen could be the cause of infantile acne. During the neonatal period, there is increased sebum production through an enlarged zona reticularis (an androgen producing area) on the fetal adrenal gland that gradually decreases to very low levels at around 1 years of age, coinciding with when infantile acne tends to resolve.^[2]^[3] The fetal adrenal gland produces androgens such as dehydroepiandrosterone (DHEA) and dehydroepiandrosterone sulfate (DHEAS) that stimulate sebaceous glands.^[3]

Diagnosis

Diagnosis is based on presentation of comedones primarily on the face of an infant of 6–12 months of age. Severity can be mild, moderate or severe and can be determined from the presence and distribution of comedones and inflammatory lesions such as papules and nodules.^[6]^[9] A physical may be followed up next with particular attention paid to signs of an endocrine disorder including normal growth and weight, testicular growth, breast development, hirsutism or growth of pubic hair.^[6]^[9] Hormonal workup may not be necessary unless one of these abnormalities is present, then work up of testosterone, DHEA, DHEAS, LH and FSH or referral to a pediatric endocrinologist specialist may be recommended.^[2]^[9]

Differential diagnosis

It is important to differentiate infantile acne from other forms of acneiform eruptions. Acne venenata infantum is a form of acne characterized by comedone formation and induced by chemical irritants on the skin. This can include comedogenic products such as lotions, ointments, creams and oils. Upon discontinuation of these products, lesions will heal within 6–8 weeks.^[3]

Other conditions that should be considered include periorificial dermatitis, keratosis pilaris, sebaceous hyperplasia and infections.^[5]^[6] Pyodermas and panniculitis should be considered in severe cases of inflammatory acne or in cases of acne conglobata while hyperandrogenism should be ruled out in cases of persistent infantile acne.^[3]

Treatment

Infantile acne is a self-limiting condition that resolves by itself within 6–12 months of occurrence or occasionally by ages 4–5 and does not require treatment in most cases but topical therapies can be used, especially in more severe cases.^[2]^[6]

The goals of treatment are to reduce sebum production, prevent formation of microcomedones, suppress the growth of bacteria and reduce inflammation.^[9] As there are no US FDA approved medications for treatment of infantile acne due to lack of high quality trials in patients under 9, recommendations for treatment is based on observations in adult and adolescent populations.^[4]

Benzoyl peroxide

free radicals to oxidize proteins in bacteria such as P. acnes. This leads to bacterial death.^[10] It additionally works as a mild comedolytic and anti-inflammatory.^[9] No bacterial resistance has been reported from BPO usage and in fact it can help limit resistance to antibiotics.^[9]^[10] Common side effects include burning, stinging, scaling and dryness at the sight of application and can be managed by reducing quantity applied, frequency of application, using a less potent product and use of non-comedogenic moisturizers.^[4]^[2]

Retinoids

Topical retinoids both alone and in combination are also first line for treating mild to moderate cases of acne. Safety and efficacy has been demonstrated in individuals 12–18 years of age.^[9] Retinoids prevent formation of comedones and promote comedolysis by binding to retinoic receptors and normalizing growth of keratinocytes.^[9]^[11] Tretinoin and adapalene have demonstrated efficacy in reducing inflammation.^[11] Adapalene as a newer retinoid is thought to be more effective and better tolerated than others in this class.^[11] As a topical product, it has similar side effects to topical BPO of burning, stinging, drying and scaling which can be managed much the same way.^[4] Reducing the potency of initial treatment, using a non-comedogenic moisturizers, and applying a small amount on the whole face rather than spot-treating may reduce severity of side effects.^[4]^[9]

In severe cases, oral isotretinoin may be recommended to prevent scarring.^[7] Dosing ranges from 0.2 mg/kg/day to 2 mg/kg/day for several months to over a year with careful monitoring.^[7]^[2]^[4] Monitoring may include complete blood count with differential and baseline liver function and lipids tests followed by routine liver function and lipid tests while on treatment.^[2]^[6]

Antibiotics

Topical antibiotics

Topical antibiotics are often used in cases of inflammatory infantile acne in combination with another topical treatment to prevent emergence of antibiotic resistance especially for periods longer than a few weeks.^[6]^[9] Clindamycin and erythromycin are the most commonly prescribed topical antibiotics for acne with coverage for S. aureus and P. acnes.^[11] These bacteriostatic antibiotics interfere with bacterial protein synthesis, preventing formation of free fatty acids by these bacteria that cause inflammation.^[10]

Oral antibiotics

In severe cases of infantile acne, especially with the presence of nodules and cysts with risks of scarring, oral antibiotics may be used.^[4] First line therapy is erythromycin with sulfamethoxazole-trimethoprim as a secondary choice in cases of P. acnes resistance. It is suggested not to use tetracyclines due to risks of permanently staining teeth in children under the age of 7.^[4] Side effects of erythromycin include gastrointestinal upset.^[9] There has however been concerns about resistant P. acnes due to widespread usage of antibiotics, and therefore steps taken to minimize resistance such as use in combination with BPO is highly recommended by experts.^[9]

Epidemiology

Infantile acne effects around 2% of children with a higher occurrence in males rather than females. Of around 9.2 million visits to outpatient care for pediatric acne, 3% or 276,000 visits, were due to neonatal and pediatric acne in the United States from 2000 to 2010.^[6]

References

External links

Classification
ILDS
L70.400)

v
t
e
Disorders of skin appendages
Nail

thickness: Onychogryphosis

Onychauxis

color: Beau's lines

Yellow nail syndrome

Leukonychia

Azure lunula

shape: Koilonychia

Nail clubbing

behavior: Onychotillomania

Onychophagia

other: Ingrown nail

Anonychia

ungrouped: Paronychia
Acute

Chronic

Chevron nail

Congenital onychodysplasia of the index fingers

Green nails

Half and half nails

Hangnail

Hapalonychia

Hook nail

Ingrown nail

Lichen planus of the nails

Longitudinal erythronychia

Malalignment of the nail plate

Median nail dystrophy

Mees' lines

Melanonychia

Muehrcke's lines

Nail–patella syndrome

Onychoatrophy

Onycholysis

Onychomadesis

Onychomatricoma

Onychomycosis

Onychophosis

Onychoptosis defluvium

Onychorrhexis

Onychoschizia

Platonychia

Pincer nails

Plummer's nail

Psoriatic nails

Pterygium inversum unguis

Pterygium unguis

Purpura of the nail bed

Racquet nail

Red lunulae

Shell nail syndrome

Splinter hemorrhage

Spotted lunulae

Staining of the nail plate

Stippled nails

Subungual hematoma

Terry's nails

Twenty-nail dystrophy

Baldness

noncicatricial alopecia: Alopecia

areata

totalis

universalis

Ophiasis

Androgenic alopecia
(male-pattern baldness)

Hypotrichosis

Telogen effluvium

Traction alopecia

Lichen planopilaris

Trichorrhexis nodosa

Alopecia neoplastica

Anagen effluvium

Alopecia mucinosa

cicatricial alopecia: Pseudopelade of Brocq

Central centrifugal cicatricial alopecia

Pressure alopecia

Traumatic alopecia

Tumor alopecia

Hot comb alopecia

Perifolliculitis capitis abscedens et suffodiens

Graham-Little syndrome

Folliculitis decalvans

ungrouped: Triangular alopecia

Frontal fibrosing alopecia

Marie Unna hereditary hypotrichosis

Hypertrichosis

Hirsutism

Acquired
localised

generalised

patterned

Congenital
generalised

localised

X-linked

Prepubertal

Nevoid hypertrichosis

Acneiform
eruption
Acne

Acne vulgaris

Acne conglobata

Acne miliaris necrotica

Tropical acne

Infantile acne/Neonatal acne

Excoriated acne

Acne fulminans

Acne medicamentosa (e.g., steroid acne)

Halogen acne
Iododerma

Bromoderma

Chloracne

Oil acne

Tar acne

Acne cosmetica

Occupational acne

Acne aestivalis

Acne keloidalis nuchae

Acne mechanica

Acne with facial edema

Pomade acne

Acne necrotica

Blackhead

Lupus miliaris disseminatus faciei

Rosacea

Perioral dermatitis
Granulomatous perioral dermatitis

Phymatous rosacea

Rhinophyma

Blepharophyma

Gnathophyma

Metophyma

Otophyma

Papulopustular rosacea

Lupoid rosacea

Erythrotelangiectatic rosacea

Glandular rosacea

Gram-negative rosacea

Steroid rosacea

Ocular rosacea

Persistent edema of rosacea

Rosacea conglobata

variants
Periorificial dermatitis

Pyoderma faciale

Ungrouped

Granulomatous facial dermatitis

Idiopathic facial aseptic granuloma

Periorbital dermatitis

SAPHO syndrome

Follicular cysts

"Sebaceous cyst"
Epidermoid cyst

Trichilemmal cyst

Steatocystoma
simplex

multiplex

Milia

Inflammation

Folliculitis
Folliculitis nares perforans

Tufted folliculitis

Pseudofolliculitis barbae

Hidradenitis
Hidradenitis suppurativa

Recurrent palmoplantar hidradenitis

Neutrophilic eccrine hidradenitis

Ungrouped

Acrokeratosis paraneoplastica of Bazex

Acroosteolysis

Bubble hair deformity

Disseminate and recurrent infundibulofolliculitis

Erosive pustular dermatosis of the scalp

Erythromelanosis follicularis faciei et colli

Hair casts

Hair follicle nevus

Intermittent hair–follicle dystrophy

Keratosis pilaris atropicans

Kinking hair

Koenen's tumor

Lichen planopilaris

Lichen spinulosus

Loose anagen syndrome

Menkes kinky hair syndrome

Monilethrix

Parakeratosis pustulosa

Pili (Pili annulati

Pili bifurcati

Pili multigemini

Pili pseudoannulati

Pili torti)

Pityriasis amiantacea

Plica neuropathica

Poliosis

Rubinstein–Taybi syndrome

Setleis syndrome

Traumatic anserine folliculosis

Trichomegaly

Trichomycosis axillaris

Trichorrhexis (Trichorrhexis invaginata

Trichorrhexis nodosa)

Trichostasis spinulosa

Uncombable hair syndrome

Wooly hair nevus

Sweat
glands
Eccrine

Miliaria
Colloid milium

Miliaria crystalline

Miliaria profunda

Miliaria pustulosa

Miliaria rubra

Occlusion miliaria

Postmiliarial hypohidrosis

Granulosis rubra nasi

Ross' syndrome

Anhidrosis

Hyperhidrosis
Generalized

Gustatory

Palmoplantar

Hypohidrosis
Acquired idiopathic generalized anhidrosis

Apocrine

Body odor

Chromhidrosis

Fox–Fordyce disease

Sebaceous

Sebaceous hyperplasia

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[Andrew2020-1] ISBN 978-0-323-54753-6
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