Riehl Melanosis (Pigmented Contact Dermatitis)

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Riehl Melanosis (Pigmented Contact Dermatitis)

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Thousands of darker-skinned people (Fitzpatrick types III-VI) around the world have a variety of possibly interrelated acquired macular dermal hyperpigmentation disorders of unknown etiology, including ashy dermatosis (AD), lichen planus pigmentosus (LPP)/lichen dyschromicum perstans, erythema dyschromicum perstans (EDP), and idiopathic eruptive macular pigmentation. Although many people also include Riehl melanosis within the aforementioned acquired pigmentary disorders, international pigmentary consensus meetings reported in 2018 have determined that Riehl melanosis is better classified as a separate entity because the clinical presentation slightly differs and it is hypothesized to arise as a result of contact dermatitis. [1]

It was in the spring of 1917, during World War I, when Riehl first identified approximately 17 patients who had striking dark-brown to grayish-brown facial pigmentation that was most pronounced on the lateral aspects of the face and neck and primarily concentrated on the forehead, ears, temple, and zygomatic regions. [2, 3] The hyperpigmentation was also noted on the thorax, but it was less pronounced in this region and primarily consisted of small follicular-based pigmented macules. Subtle hyperpigmentation was also identified on the hands, forearms, and intertriginous regions. [3] All patients were white and from Vienna, and all had no evidence of an underlying illness. The patients varied in age and sex. In addition to the hyperpigmentation, erythematous macules and papules were also identified. [3, 4, 5] Histologically, the lesions were marked by a dense inflammatory cell infiltrate in the superficial dermis admixed with melanophages. [3, 4]

Although Riehl was unable to identify the cause of the eruption, he speculated that the hyperpigmentation occurred because of some nutritional alteration that he attributed to wartime conditions. [2, 3, 4, 5] Concomitant with the end of the war, no further cases were identified; thereby, supporting his hypothesis. [3] Subsequently in World War II, a similar eruption surfaced in approximately 165 people in France, again associated with the scarce food supplies and disappearing with the end of the war; however, this latter situation differed from that seen in World War I in that the majority of cases were reported in women. [3, 4]

Later, Hoffmann and Habermann described a condition referred to as melanodermatitis toxica that was hypothesized to be a form of contact dermatitis associated with the use of certain oils and hydrocarbons. Although these authors emphasized the clinical similarities between Riehl melanosis and melanodermatitis toxica, Riehl could not accept that the melanosis that he described was due to a local chemical irritant and felt that the conditions were separate entities. The role of nutrition as a possible cause of this unusual melanosis was further addressed in a paper by Findlay, who described several cases of Riehl melanosis in the Bantu people in South Africa; however, no further reports in the literature linked Riehl melanosis to nutritional deficiencies. [6]

Subsequent to the great wars, the majority of cases of Riehl melanosis described in the literature differ from the cases originally described by Riehl. In 1950, Minami and Noma described a pigmented dermatitis in Asian women unrelated to the war and named the condition melanosis faciei feminae. [4] The etiology of this latter pigmentation was unknown for many years, until 2 studies from Argentina in the late 1940s and 1950s described facial pigmentation similar to Riehl melanosis that was subsequently attributed to the use of cosmetics. In the first study, patch testing identified aniline dye (orange II) present in facial powder as the cause of the pigmented contact dermatitis, whereas the second study emphasized that photosensitizing may play an addition role in the pigmentation. [3]

In 1970, Osmundsen subsequently reported 7 patients who had a similar bizarre hyperpigmentation that occurred as a result of contact dermatitis to an optical whitener, Tinopal CH 3566, in washing powder and called the condition pigmented contact dermatitis (PCD). [7] Subsequently in 1973, Nakayama introduced the term pigmented cosmetic contact dermatitis for cases that were ascribed to the use of certain cosmetics.

To date, the etiology of Riehl melanosis remains controversial, and although the majority of experts believe it is synonymous with pigmented contact dermatitis, some authors insist that this is an erroneous assumption because the cases reported by Riehl appear to have been related to nutritional alterations that arose during World War I, with no further case reports noted after the war ended, and thereby insist that Riehl melanosis should be classified as a distinct entity. [2, 3, 4, 5] Pigmented contact dermatitis, on the other hand, is caused by an allergic contact dermatitis to a variety of topical and airborne allergens or a lichenoid immune reaction that may be caused by intrinsic or extrinsic factors. [8, 9]

The hyperpigmentation in pigmented contact dermatitis is postulated to be caused by frequent and repeated contact with small amounts of sensitizing allergens primarily in cosmetic and textile materials. Nakayama hypothesized that allergens used in commercial products were too low in concentration to produce typical eczematous dermatitis, but rather accumulation of these allergens resulted allergic contact dermatitis, a type IV cytolytic reaction. [10, 11] This later reaction is characterized by vacuolar degeneration of the basal layer of the epidermis associated with pigment incontinence in the superficial dermis. The melanin pigment is slowly engulfed by macrophages; therefore, resolution of the hyperpigmentation is a prolonged process. Because most cases of pigmented contact dermatitis occur in patients with a darker completion, one hypothesis is that various pigment-genetic interactions contribute to the development of this condition. [5] Furthermore, Imokawa and Kawai have provided clinical evidence that various allergens implicated in allergic contact dermatitis can stimulate melanogenesis. [12]

A variety of contact allergens have been implicated in pigmented contact dermatitis, as described below. [4, 5, 13] Although the majority of cases occur because of direct contact with these allergens, a few cases secondary to contact with airborne allergens have been described. [5, 14, 15]

Textile allergens are as follows:

Tinopal CH3566 – Optical whitener in washing powder

Napthol AS – Coupling agent for azo dyes

Biocheck 60 – Pesticide for textiles

PPP-HB – Textile finish

Mercury compounds – Bactericides

Formaldehyde – Preservative

Azo dyes – Dye [16]

Disperse Blue 106 – Dye

Disperse Blue 124 – Dye

CI Blue 19 (Brilliant Blue) – Dye

Rubber components

Cosmetic allergens are as follows [17] :

D&C Red 31 – Pigment

Brilliant Lake Red R – Pigment [18, 19]

D&C Yellow No. 11 and 10 – Pigment

PAN (phenyl-azo-2-napthol) – Impurity in azo pigments

Chromium hydroxide – Pigment

Carbanilides (trichlorocarbanilide and Irgasan CF3) – Bactericidal

Aniline dyes – Pigment

Hair dyes

Ricinoleic acid (castor oil acid) – Bactericide (deodorants, lipstick, military camouflage) [20]

Kumkum (red) – Cosmetic powder and liquid (Hindu women) [21]

Fragrances

Fragrance allergens are as follows:

Jasmine absolute

Benzyl salicylate

Hydroxycitronellal

Ylang-ylang oil

Cinnamic alcohol

Musk ambrette [14, 22]

Cananga oil

Sandalwood oil

Synthetic sandalwood (containing bornyl methoxy cyclohexanol)

Geraniol oil

Eugenol

Isoeugenol

Balsam of Peru [23, 24]

Lavender oil

Lemon oil [25, 26]

Methoxycitronellal

Benzyl alcohol

Cinnamic derivatives

Miscellaneous allergens are as follows:

Chromate (K dichromate) – Leather, soaps

Nickel/nickel sulfate – Component metal products and jewelry

PTBPFR (paratertiary butyl-phenol formaldehyde resin) – Neoprene adhesive in leather products [27]

Plathymenia foliosa – Wood dust [15]

Minoxidil 5% – Topical vasodilator for hair loss treatment [28]

Cases of pigmented contact dermatitis have been reported in the Indian literature, and the most common allergen to be implicated is kumkum, a colored cosmetic used by Hindu women that is applied most often to the central forehead and along the hair line. [5, 21] Only commercially available red kumkum can sensitize and cause pigmented contact dermatitis. Components of kumkum include azo dyes, coal tar dyes, toludine red, erythrosine, lithal red calcium salt, fragrances, tumeric powder, groundnut oil, tragacanth gum, Cananga oil, and parabens. [5]

In addition to contact allergens, a Riehl melanosis–like eruption has been reported in Japanese women with Sjögren syndrome related to the development of anti-SSA (Ro) antibodies. The lesions are most pronounced on sun-exposed areas, primarily on the face, and the pigmentation typically resolves with the institution of ultraviolet protection. One hypothesis is that ultraviolet radiation induces expression of the SSA antigen on keratinocytes, which then becomes the target of circulating anti-SSA antibodies, resulting in an interface dermatitis and associated pigment incontinence. [29]

The incidence is not known. Most cases are reported outside of the United States, with a large proportion of cases reported in Japan. No international statistics are available, but cases have been reported in France, Denmark, South America, Japan, India, and South Africa.

In general, pigmented contact dermatitis is most pronounced in darkly pigmented races.

Women appear to have a greater predilection for pigmented contact dermatitis.

Although it has been reported in a wide range of patients, the majority of cases appear to occur in young to middle-aged women.

Although the hyperpigmentation has a tendency to lighten over time and with avoidance of the eliciting agent, some pigmentation may persist.

Because ultraviolet light has been implicated as a contributing factor in some cases of pigmented contact dermatitis, sun avoidance and sunblock usage are prudent. See Sunscreens and Photoprotection for detailed information.

Kumarasinghe SPW, Pandya A, Chandran V, Rodrigues M, Dlova NC, Kang HY, et al. A global consensus statement on ashy dermatosis, erythema dyschromicum perstans, lichen planus pigmentosus, idiopathic eruptive macular pigmentation, and Riehl’s melanosis. Int J Dermatol. 2018 Sep 3. [Medline].

Riehl G. Uber eine eigenartige melanose. Wien Klin Wochensschr. 1917. 30:280-1.

Rorsman H. Riehl’s melanosis. Int J Dermatol. 1982 Mar. 21(2):75-8. [Medline].

Nakayama H. Pigmented Contact Dermatitis and Chemical Depigmentation. Rycroft R, Menne T, Frosch P, Lepoittevin J, eds. Textbook of Contact Dermatitis. 3rd ed. New York, NY: Springer; 2001. 319-333.

Shenoi SD, Rao R. Pigmented contact dermatitis. Indian J Dermatol Venereol Leprol. 2007 Sep-Oct. 73(5):285-7. [Medline].

Findlay GH. Some observations on the melanosis of Riehl. S Afr Med J. 1952 May 3. 26(18):373-5. [Medline].

Osmundsen PE. Pigmented contact dermatitis. Br J Dermatol. 1970 Aug. 83(2):296-301. [Medline].

Smucker JE, Kirby JS. Riehl melanosis treated successfully with Q-switch Nd:YAG laser. J Drugs Dermatol. 2014 Mar. 13 (3):356-8. [Medline].

Seike M, Hirose Y, Ikeda M, Kodama H. Coexistence of Riehl’s melanosis and lichen planus. J Dermatol. 2003 Feb. 30 (2):132-4. [Medline].

Nakayama H, Harada R, Toda M. Pigmented cosmetic dermatitis. Int J Dermatol. 1976 Nov. 15(9):673-5. [Medline].

Nakayama H, Matsuo S, Hayakawa K, Takhashi K, Shigematsu T, Ota S. Pigmented cosmetic dermatitis. Int J Dermatol. 1984 Jun. 23(5):299-305. [Medline].

Imokawa G, Kawai M. Differential hypermelanosis induced by allergic contact dermatitis. J Invest Dermatol. 1987 Dec. 89(6):540-6. [Medline].

Ebihara T, Nakayama H. Pigmented contact dermatitis. Clin Dermatol. 1997 Jul-Aug. 15(4):593-9. [Medline].

Hayakawa R, Matsunaga K, Arima Y. Airborne pigmented contact dermatitis due to musk ambrette in incense. Contact Dermatitis. 1987 Feb. 16(2):96-8. [Medline].

Pires MC, Manoel Silva dos Reis V, Mitelmann R, Moreira F. Pigmented contact dermatitis due to Plathymenia foliosa dust. Contact Dermatitis. 1999 Jun. 40(6):339. [Medline].

Fujimoto K, Hashimoto S, Kozuka T, Tashiro M, Sano S. Occupational pigmented contact dermatitis from azo-dyes. Contact Dermatitis. 1985 Jan. 12(1):15-7. [Medline].

el Sayed F, Manzur F, Bazex J. Pigmented contact dermatitis from cosmetics. Contact Dermatitis. 1995 Feb. 32(2):111. [Medline].

Kozuka T, Tashiro M, Sano S, et al. Brilliant Lake Red R as a cause of pigmented contact dermatitis. Contact Dermatitis. 1979 Sep. 5(5):297-304. [Medline].

Sugai T, Takahashi Y, Takagi T. Pigmented cosmetic dermatitis and coal tar dyes. Contact Dermatitis. 1977 Oct. 3(5):249-56. [Medline].

Leow YH, Tan SH, Ng SK. Pigmented contact cheilitis from ricinoleic acid in lipsticks. Contact Dermatitis. 2003 Jul. 49(1):48-9. [Medline].

Nath AK, Thappa DM. Kumkum-induced dermatitis: an analysis of 46 cases. Clin Exp Dermatol. 2007 Jul. 32(4):385-7. [Medline].

Parodi G, Guarrera M, Rebora A. Lichenoid photocontact dermatitis to musk ambrette. Contact Dermatitis. 1987 Mar. 16(3):136-8. [Medline].

Admani S, Goldenberg A, Jacob SE. Contact Alopecia: Improvement of Alopecia with Discontinuation of Fluocinolone Oil in Individuals Allergic to Balsam Fragrance. Pediatr Dermatol. 2017 Jan. 34 (1):e57-e60. [Medline].

Liu KX, Zimarowski MJ, Wu PA. Contact Dermatitis Associated with Alopecia and Hyperpigmentation. Pediatr Dermatol. 2017 Sep. 34 (5):624-625. [Medline].

Naganuma M, Hirose S, Nakayama Y, Nakajima K, Someya T. A study of the phototoxicity of lemon oil. Arch Dermatol Res. 1985. 278(1):31-6. [Medline].

Serrano G, Pujol C, Cuadra J, Gallo S, Aliaga A. Riehl’s melanosis: pigmented contact dermatitis caused by fragrances. J Am Acad Dermatol. 1989 Nov. 21(5 Pt 2):1057-60. [Medline].

Ozkaya-Bayazit E, Buyukbabani N. Non-eczematous pigmented interface dermatitis from para-tertiary-butylphenol-formaldehyde resin in a watchstrap adhesive. Contact Dermatitis. 2001 Jan. 44(1):45-6. [Medline].

Trattner A, David M. Pigmented contact dermatitis from topical minoxidil 5%. Contact Dermatitis. 2002 Apr. 46(4):246. [Medline].

Miyoshi K, Kodama H. Riehl’s melanosis-like eruption associated with Sjogren’s syndrome. J Dermatol. 1997 Dec. 24(12):784-6. [Medline].

Wang L, Xu AE. Four views of Riehl’s melanosis: clinical appearance, dermoscopy, confocal microscopy and histopathology. J Eur Acad Dermatol Venereol. 2014 Sep. 28 (9):1199-206. [Medline].

Vinay K, Bishnoi A, Parsad D, Saikia UN, Sendhil Kumaran M. Dermatoscopic evaluation and histopathological correlation of acquired dermal macular hyperpigmentation. Int J Dermatol. 2017 Dec. 56 (12):1395-1399. [Medline].

Perez-Bernal A, Munoz-Perez MA, Camacho F. Management of facial hyperpigmentation. Am J Clin Dermatol. 2000 Sep-Oct. 1(5):261-8. [Medline].

Kobori T, Araki, Toda K. Photoleukomelanodermatitis (Kobori) caused by benzothiazidiazine derivatives. Jap J Dermatol. 1966. 76:665.

Nirmal B, Santhikiran B, Mukhopadhyay S. Multispectral Dermatoscopic Features of Chemical Leucoderma with Pigmented Contact Dermatitis. Indian Dermatol Online J. 2018 Mar-Apr. 9 (2):107-109. [Medline].

On HR, Hong WJ, Roh MR. Low-pulse energy Q-switched Nd:YAG laser treatment for hair-dye-induced Riehl’s melanosis. J Cosmet Laser Ther. 2015 Jun. 17 (3):135-8. [Medline].

Chung BY, Kim JE, Ko JY, Chang SE. A pilot study of a novel dual–pulsed 1064 nm Q-switched Nd: YAG laser to treat Riehl’s melanosis. J Cosmet Laser Ther. 2014 Dec. 16 (6):290-2. [Medline].

Xu Z, Xing X, Zhang C, Chen L, Flora Xiang L. A pilot study of oral tranexamic acid and Glycyrrhizin compound in the treatment of recalcitrant Riehl’s melanosis. J Cosmet Dermatol. 2018 Oct 19. [Medline].

Kwon HH, Ohn J, Suh DH, Park HY, Choi SC, Jung JY, et al. A pilot study for triple combination therapy with a low-fluence 1064 nm Q-switched Nd:YAG laser, hydroquinone cream and oral tranexamic acid for recalcitrant Riehl’s Melanosis. J Dermatolog Treat. 2017 Mar. 28 (2):155-159. [Medline].

Elizabeth K Satter, MD, MPH Dermatologist and Dermatopathologist

Elizabeth K Satter, MD, MPH is a member of the following medical societies: Alpha Omega Alpha, American Medical Womens Association

Disclosure: Nothing to disclose.

Richard P Vinson, MD Assistant Clinical Professor, Department of Dermatology, Texas Tech University Health Sciences Center, Paul L Foster School of Medicine; Consulting Staff, Mountain View Dermatology, PA

Richard P Vinson, MD is a member of the following medical societies: American Academy of Dermatology, Texas Medical Association, Association of Military Dermatologists, Texas Dermatological Society

Disclosure: Nothing to disclose.

Paul Krusinski, MD Director of Dermatology, Fletcher Allen Health Care; Professor, Department of Internal Medicine, University of Vermont College of Medicine

Paul Krusinski, MD is a member of the following medical societies: American Academy of Dermatology, American College of Physicians, Society for Investigative Dermatology

Disclosure: Nothing to disclose.

William D James, MD Paul R Gross Professor of Dermatology, Vice-Chairman, Residency Program Director, Department of Dermatology, University of Pennsylvania School of Medicine

William D James, MD is a member of the following medical societies: American Academy of Dermatology, Society for Investigative Dermatology

Disclosure: Received income in an amount equal to or greater than $250 from: Elsevier; WebMD.

John D Wilkinson, MD, MBBS, MRCS, FRCP Chairman, Clinical Director, Department of Dermatology, Amersham Hospital and High Wycombe Hospital, UK

John D Wilkinson, MD, MBBS, MRCS, FRCP is a member of the following medical societies: American Academy of Dermatology, Royal College of Physicians

Disclosure: Nothing to disclose.

Helena A Longin, MD Resident Physician, Department of Dermatology, Naval Medical Center San Diego

Helena A Longin, MD is a member of the following medical societies: American Academy of Dermatology

Disclosure: Nothing to disclose.

The authors and editors of Medscape Reference acknowledge the contributions of previous author, Mohsin Ali, MBBS, FRCP, MRCP, to the development and writing of this article.

Riehl Melanosis (Pigmented Contact Dermatitis)

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