Peer Reviewed
An Atlas of Lumps and Bumps: Part 20
AFFILIATIONS:
1Department of Pediatrics, University of Calgary, Calgary, Alberta, Canada
2Alberta Children’s Hospital, Calgary, Alberta, Canada
3Toronto Dermatology Centre, Toronto, Ontario, Canada
4Department of Pediatrics and Department of Dermatology and Skin Sciences, University of British Columbia, Vancouver, British Columbia, Canada
5Medical staff, Asian Medical Clinic, an affiliate with the University of Calgary Medical Clinic, Calgary, Alberta, Canada
6Pediatric Institute, Kuala Lumpur General Hospital, Kuala Lumpur, Malaysia
CITATION:
Leung AKC, Barankin B, Lam JM, Leong KF. An atlas of lumps and bumps, part 20. Consultant. 2022;62(9):e29-e32. doi:10.25270/con.2022.07.000013
DISCLOSURES:
Dr Leung is the series editor. He was not involved with the handling of this paper, which was sent out for independent external peer review.
CORRESPONDENCE:
Alexander K. C. Leung, MD, #200, 233 16th Ave NW, Calgary, AB T2M 0H5, Canada (aleung@ucalgary.ca)
EDITOR’S NOTE:
This article is part of a series describing and differentiating dermatologic lumps and bumps. To access previously published articles in the series, visit https://www.consultant360.com/resource-center/atlas-lumps-and-bumps.
Syringomas
The word “syringoma” is derived from the Greek word “syrinx” meaning tube or pipe.1 Syringomas are common, benign, sweat gland tumors that originate from the straight intradermal portion of the eccrine sweat duct.2,3 Histologically, multiple small and dilated eccrine ducts within a dense fibrous stroma are characteristic features.4
Syringomas usually present during puberty or the third and fourth decades of life.3,5 The reported prevalence ranges from 0.6% to 1% of the population.1,6 The prevalence is higher in Asians and Africans.7 The female-to-male ratio is approximately 2:1 in most studies.3 Most cases occur sporadically, although familial cases have been described.8 Familial cases may have an autosomal-dominant mode of inheritance.8,9 The condition is more common in patients with Down syndrome, Ehlers-Danlos syndrome, Costello syndrome, Marfan syndrome, Nicolau-Balus (syringomas, milia, and atrophodermia vermiculata) syndrome, alopecia (cicatricial alopecia and rarely alopecia areata), and type 2 diabetes.10,11
Typically, syringomas present as small, soft, skin-colored to slightly yellowish papules (Figures 1 and 2).5,12 The papules are usually 1 to 3 mm in diameter, asymptomatic, and symmetrically distributed.3 The lesions may be solitary or, most often, multiple. The distribution may be localized or generalized. Localized syringomas are the most common clinical variant, and the lesions are typically observed in the periorbital region, especially infraorbitally (Figures 1 and 2).13,14 Generalized syringomas are found mainly on the neck and trunk, followed by the forearms (Figures 3 and 4).5 However, syringomas may appear on other body areas such as the penis, vulva, axillae, and buttocks.13,15-17 Generally, patients with generalized syringomas are younger than those with localized syringomas.5
Figure 1. Syringomas present as small, soft, skin-colored to slightly yellowish papules.
Figure 2. Syringomas are usually 1 to 3 mm in diameter, asymptomatic, and symmetrically distributed.
Figure 3. Generalized syringomas can present on the face but are more common on the neck and trunk.
Figure 4. Generalized syringomas are found mainly on the neck and trunk, followed by the forearms.
Eruptive syringoma is a rare variant that typically presents as multiple skin-colored, pink, or yellow-brown papules and appear in successive crops on the anterior parts of the neck, chest, abdomen, axillae, upper extremities, and genital areas in addition to the usual site on the face.2,5,14,18,19 In contrast to classic syringomas, eruptive syringomas occur most frequently before or around puberty, especially after an inflammatory condition, and may be associated with pruritus.2,6,18 Some authors categorize eruptive syringomas as a hyperplastic response to an inflammatory reaction rather than a true adnexal neoplasm.20 Other rare variants include plaque-like, urticaria pigmentosa-like, lichen planus-like, milia-like, and unilateral linear nevoidal-like syringomas.11,21,22
Milia
Milia are benign, transient, superficial keratinous cysts.23 They present as asymptomatic, small (generally less than 3 mm), firm, white to yellow, smooth, dome-shaped papules.24 Histologically, they appear as small infundibular cysts that are lined with stratified squamous epithelium with a granular cell layer.25 The cyst contains laminated layers of keratin. Milia may arise spontaneously without a known cause (primary milia) or secondary to various processes (secondary milia). Primary milia may be congenital (congenital primary milia) or have an onset later in life (benign primary milia of children and adults).
Congenital primary milia are present in 40 to 50% of newborn infants with no sex predilection.26 The condition is less common in premature infants.23,25 Its onset in premature infants could be delayed by several weeks.23 While congenital primary milia favor the nose (Figure 5), benign primary milia of children and adults favor the eyelids, periocular areas, cheeks, and forehead (Figures 6 to 8).23,24 Other unusual sites of involvement include the nasal crease, trunk, extremities, vulva, glans penis, auricle, and areola (Figures 9 and 10).23-25,27,28
Figure 5. Congenital primary milia favor the nose.
Figure 6. Benign primary milia of children favor the eyelids.
Figure 7. Benign primary milia of adults favor the eyelids and periocular areas.
Figure 8. Benign primary milia of adults favor the eyelids and periocular areas.
Figure 9. Unusual sites of involvement include the auricle.
Figure 10. Unusual sites of involvement include the areola.
Primary milia may be a feature of trisomy 13, Gorlin-Goltz syndrome, Rombo syndrome, basal cell nevus syndrome, Bazex-Dupre-Christol syndrome, Basan syndrome, Brooke-Spiegler syndrome, Marie-Unna hypotrichosis (congenital hereditary trichodysplasia), Nicolau-Balus syndrome, pachyonychia congenita type 2 and oro-facial-digital syndrome type 1.23,25,29,30
Multiple eruptive milia and milia en plaque are considered clinical variants of milia.31,32 Multiple eruptive milia are characterized by a sudden onset of multiple asymptomatic milia over a period of weeks to months, mainly on the head, neck, and trunk.31 Milia en plaque is characterized by numerous tiny milia on an erythematous plaque.32-34 The condition is asymptomatic and is most common in middle-aged individuals with a female predominance and no predilection for race.32 The periocular area is most commonly affected.33 Other sites of involvement include the postauricular area, nasal bridge, cheek, submandibular area, supraclavicular area, trunk, arms, and lower limbs.32
Secondary milia usually occur in older children.23 They may occur in association with systemic disease (eg, porphyria cutanea tarda, epidermolysis bullosa, lichen planus, discoid lupus erythematosus, bullous pemphigoid,), medication use (eg, topical corticosteroids, oral cyclosporine, oral 5-fluorouracil, oral isotretinoin, oral dovitinib, oral vemurafenib, oral penicillamine), photodynamic therapy use, radiotherapy use, or trauma (chemical peels, dermabrasion, tattoos, burns, skin grafts).35-47
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2. Avhad G, Ghuge P, Jerajani HR. Generalized eruptive syringoma. Indian J Dermatol. 2015;60(2):214. doi:10.4103/0019-5154.152586
3. Nosrati N, Coleman NM, Hsu S. Axillary syringomas. Dermatol Online J. 2008;14(4):13. doi.10.5070/D34jt089ht
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36. Baek SW, Seo YJ, Lee HJ. Multiple milia associated with use of the tyrosine kinase inhibitor dovitinib. Australas J Dermatol. 2018;59(1):57-58. doi:10.1111/ajd.12620
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40. Kimes K, Beasley K, Dalton SR. Eruptive milia and comedones during treatment with dovitinib. Dermatol Online J. 2015;21(9). doi.10.5070/D3219028692
41. Kluger N. Eruptive milia and acneiform hyperkeratosis with comedones (pseudo-epidermal cysts) within tattoos. Ann Dermatol Venereol. 2019;146(12):801-806. doi:10.1016/j.annder.2019.01.026
42. Kumudhini S, Rao R, Pai K, Shetty S, Pai S. Extensive milia formation in a young woman with bullous pemphigoid. Indian J Dermatol Venereol Leprol. 2018;84(2):248. doi:10.4103/ijdvl.IJDVL_402_16
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45. Ross N, Farber M, Sahu J. Eruptive milia within a tattoo: A case report and review of the literature. J Drugs Dermatol. 2017;16(6):621-624. https://jddonline.com/articles/eruptive-milia-within-a-tattoo-a-case-report-and-review-of-the-literature-S1545961617P0621X/
46. Sambrano BL, Riddel CE, Chon SY. Eruptive milia secondary to vemurafenib. J Am Acad Dermatol. 2013;69(5):e258-e260. doi:10.1016/j.jaad.2013.06.031
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