https://orcid.org/0000-0002-3010-5052
Abstract
Molluscum contagiosum (MC) is a benign papular skin infection caused by Molluscum contagiosum virus (MCV). Over the past 30 years, the incidence of MK has continued to increased association with sexually transmitted infections and human immunodeficiency virus (HIV) infection. The incidence of MC in HIV patients is quite high at 5–8%. Until now there is no standard therapy used for the treatment of MC in patients with HIV. In HIV patients, anti retro viral therapy (ARV) is the main therapy with several other additional therapies such as cantaridin, chemical peeling agents such as glycolic acid (20–70%) and trichloroacetic acid (20–100%), cryosurgery, electrosurgery, incision, lactic acid, laser surgery, podophyllin, retinoic acid, and urea. There have been no studies regarding the administration of topical 20% glycolic acid in MC patients. We report a case of MC in an HIV patient who was treated with 20% topical glycolic acid after failing treatment with topical tretinoin. The diagnosis was made clinically, cytologically, and histopathologically, a white mass was found on compression of the lesion and Henderson-Paterson bodies. The lesions on the face, arms, and legs were given glycolic acid lotion 20% which was applied once a day at night. The lesions started to show responses to the treatment at week 6th as some of the MC papules became hyperpigmented macules. The side effects of therapy that appeared were itching and hyperpigmentation. Topical 20% glycolic acid can be used for MC therapy with minimal side effects, easy to apply and safe.
Introduction
Molluscum contagiosum (MC) is a skin infection in the form of benign popular lesions caused by Molluscum contagiosum virus (MCV).Citation1 It is more common in children and young adults.Citation2–4 In Indonesia, the prevalence of molluscum contagiosum is high, at 40.4% of other skin diseases. The incidence of molluscum contagiosum in HIV patients is quite high at 5–8%, and in patients with CD4+ <100 the incidence of molluscum contagiosum is reported at 33%.Citation5–7 Molluscum contagiosum has a typical clinical picture of a white, pink, or skin-colored, pearly, dome-shaped protrusion with central umbilication, measuring 1 mm to 1 cm in size, so that the diagnosis can be made clinically.Citation1,Citation8 Unusual clinical manifestations in HIV patients include atypical, disseminated, facial MC, or can be large with a diameter of more than 1 cm, referred to as giant MC.Citation9,Citation10 Management of MC in HIV patients is very difficult.Citation11 There are several aspects that must be considered in choosing therapy, namely the patient’s physical and psychological endurance to receive therapy, especially if the number of lesions is large, the choice of the patient or the patient’s parents, cost, availability of therapeutic materials or tools, and ease of application. Curettage has been used as the gold standard therapy for MC.Citation12 Tretinoin is one of the chemicals that can be used for molluscum therapy. There are a number of other destructive therapy modalities such as topical glycolic acid (GA) 20–70%.Citation13
Here we report one case MC in an HIV patient who was treated with 20% topical GA after failing therapy with 0.05% topical tretinoin.
Clinical Case
A 26-year-old homosexual male presented with a chief complaint of skin-colored pustules on the face, right arm, and right leg that were neither itchy nor painful and had not improved after eight weeks of treatment with vitacid® cream. In the anamnesis, it was found that since two years before treatment, the patient experienced excessive weight loss and diarrhea for one month and was diagnosed with HIV accompanied by the onset of skin-colored papules on the face with size of a pin on the right cheek that did not feel itchy or painful. Two months later the facial papules increased in number on the left cheek, right arm and right leg. The patient did not treat the skin disorder. Three months before he came to RSHS, complaints of papules getting bigger and more numerous to the eyelids, so the patient sought treatment at Cicendo Eye Hospital and they excised the papules on the eyelids. The patient was then referred to Dr. Hasan Sadikin General Hospital for further treatment of papules on the face, arms and legs. The patient was said to have a viral infection and was treated with vitacid® for two months but there was no improvement and the complaints of papules became erythema with the size of corn kernels. There was a history of repeated homosexual-anogenital exposures with the patient being the receptive partner. The patient has first sexual intercourse at the age of 18 years with a male casual friend, unprotected, anogenital, and orogenital. He has had sex with approximately 20 men in her lifetime. The last sexual intercourse with a male acquaintance six months ago was anogenital and orogenital, without using a condom. On physical examination, vital signs were within normal limits. The generalized status was found to be underweight. On the face, right arm, and right leg there were multiple lesions, discrete, round shape, size 0.2×0.2x0.1 cm to 0.8×0.3x0.2 cm, firm borders, arising from the skin surface, dry, in the form of skin-colored papules with central umbilication (). The results of cytological examination of Tzanck smears with Giemsa staining of white masses taken from skin lesions on the face and neck found round-shaped hyperbasophilic masses (Henderson-Paterson bodies) (). Histopathologic examination of the lesion on the right cheek revealed hyperplastic, endophytic, lobularly arranged, keratinized spongy epithelium with nuclei within normal limits (). The cytoplasm appeared to form molluscum bodies in the form of eosinophilic inclusion bodies. In the center of the lesion, there was ostia formation containing keratinous debris. The dermis in the form of fibrocollagenous connective tissue is pressed into the lesion forming septa between the lobules. CD4+ test result was 26 cells/uL. Skin disorders showed improvement after 54 months of therapy with post inflammatory hyperpigmentation ().
Figure 1 Clinical manifestation of MC lesion on face, right arm, and right leg before therapy.
Figure 2 The cytological examination of Tzanck smears with Giemsa staining of white masses taken from skin lesions on the face and neck found round-shaped hyperbasophilic masses (Henderson-Paterson bodies).
Figure 3 Histopathologic examination of the lesion on the right cheek revealed hyperplastic, endophytic, lobularly arranged, keratinized spongy epithelium with nuclei within normal limits.
Figure 4 Clinical manifestation of MC lesion on face, right arm, and right leg before therapy, after 54th days of therapy.
Discussion
Molluscum contagiosum (MC) is a self-limiting disease caused by infection with molluscum contagiosum virus (MCV) which is the only genus of molluscipoxvirus in the poxviridae family.Citation1,Citation9 MCV has 4 major subtypes namely MCV-1, MCV-2, MCV-3, and MCV-4 with MCV-1 being the most common cause of MC covering 75–96% of cases.Citation14,Citation15 MC cases in adolescents and adults are more often caused by MCV-2 because they experience transmission through sexual intercourse. In patients with HIV, 60% of MC cases are caused by MCV-2.Citation8 MCV infection can also occur in adults who are sexually active or in immunosuppressed conditions, especially patients with HIV.Citation16 The prevalence of MC co-infection with HIV or AIDS is around 5–18%.Citation1,Citation6 The World Health Organization (WHO) divides HIV into 4 clinical stages based on comorbidities found in history and physical examination. Supportive examinations such as CD4+ values can also be used to classify the degree of immunodeficiency of HIV patients which can be distinguished based on the number of CD4+ T cells, namely the acute phase, stage 1–2 with CD4+ counts >200 cells/uL (early chronic phase), stage 3–4 with CD4+ counts <200 cells/uL (advanced chronic phase), and <100 cells/uL in stage 4 (severe immunosuppression). Each of these stages can cause different mucocutaneous clinical manifestations, MC is usually found in patients with severe immunosuppression (stage 4) and CD4+ T cell count <100 cells/uL.Citation10 The incubation period of the virus ranges from one week to six months, with an average time of 2–3 months.Citation1,Citation12 Transmission of MC can occur through direct skin-to-skin contact through sexual and non-sexual routes.Citation12 In adults, MC with genital lesions is generally transmitted through sexual intercourse, so it is necessary to screening for sexually transmitted infections.Citation14,Citation17 The spread of MC through non-sexual routes can occur through the shared use of contaminated clothes, towels, and fomites.Citation18 Living in the same house with an infected person, poor hygiene, overcrowded environment, having a history of atopic dermatitis, the use of topical steroids, immunosuppression such as in malignancy, and HIV are risk factors for the incidence of MC.Citation17,Citation19 Transmission of MCV to other locations is obtained through inoculation of the virus on the skin after trauma or micro-abrasion of the lesion. MC virus can enter the host epithelial cells by endocytosis or cell fusion and will replicate in the stratum spinosum of the epidermis. The virus will release the capsid and viral DNA transcription occurs to produce infective virions. Cells infected with the virus will increase the expression of epidermal growth factor receptors resulting in increased cell mitosis. The virus replicates in the cytoplasm of the cell producing cytoplasmic inclusion bodies (Henderson-Paterson bodies). The clinical picture of MC is a skin-colored papule, pearly or pink, dome-shaped, has a smooth surface, spongy consistency, with umbilication in the central part, contains a white mass containing molluscum bodies and can be seen when removed with pressure.Citation20,Citation21 Within a few weeks the size of MC can reach 3–5 mm in diameter, sometimes it can reach 1.5 cm in diameter, especially in immunosuppressed patients.Citation21,Citation22 The number of papules is usually less than 20 or can even reach 100 pieces or more.Citation22 In HIV patients, the majority of MC lesions are found on the face and neck.Citation6 In addition, although rare, MC lesions in HIV patients can appear in other locations, such as the soles of the feet, areolas, fingers, or eyelids.Citation23 In this case report patient, MC lesions were in the form of skin-colored papules with umbilication in the center, white masses were found when pressing on the lesions, and most of the lesions were in the facial area in accordance with the majority of MC predilection in patients with HIV. The diagnosis of MC can be made based on the typical characteristics of the lesion.Citation14 On suppression of the lesion, a grayish white mass is found.Citation9 The discovery of molluscum bodies (Henderson-Paterson bodies) on cytological examination of Tzanck smear with Giemsa staining is pathognomonic in MC.Citation20,Citation24 On histopathologic examination MC shows hypertrophy or hyperplasia of the epidermis surrounding lobules containing keratinized debris and molluscum bodies.Citation20 The diagnosis can be made through histopathological examination of the tissue using methenamine silver staining and the characteristic yeast cells divided by the septum as small cells (2–4 μm in diameter).Citation25 In this case report patient, the diagnosis of MC was made based on the typical clinical picture, supported by the discovery of round masses (Henderson-Paterson bodies) on direct cytological examination with Giemsa staining and on histopathological examination. The duration of onset to disappearance of lesions varies with most occurrences self-limiting within 6–9 months in immunocompetent individuals. Some cases of lesions may persist for more than 3 or 4 years.Citation4 In HIV patients, MC may not undergo spontaneous resolution without treatment.Citation26 In this case report patient, the lesions appeared since two years before seeking treatment at RSHS and the complaints were still apparent when the patient sought treatment at RSHS when the patient came to RSHS. In general, there are 4 therapeutic approaches for MC, destructive therapy, chemical agents, immunomodulators, and antivirals.Citation3 Destructive therapy works by damaging the intracytoplasmic sac containing viral particles and triggering an immunological response that will clear the infection.Citation1 Some destructive therapies that can be performed are cryosurgery, curettage, tape stripping, and laser.Citation3,Citation9 In HIV patients, optimal management to restore immune system function with antiretroviral therapy is the main treatment of choice with several other adjunctive therapies.Citation23 There are a number of treatment modalities available for HIV patients with MC including cantaridine, chemical peeling agents such as glycolic acid (20–70%) and trichloroacetic acid (20–100%), cryosurgery, electrosurgery, incision, lactic acid, laser surgery, podophylline, retinoic acid, urea,Citation13 and intravenous or topical cidofovir.Citation27 Treatment that destroys lesions such as curettage is not ideal as it may increase the risk of infection and disease transmission. In patients with HIV, MC lesions often do not undergo spontaneous resolution and may expand.Citation13,Citation14 Tretinoin is a retinol (vitamin A) derivative that can be used for MC therapy and is available in various concentrations. Tretinoin concentration of 0.05% can be an appropriate choice in MC therapy. The mechanism of tretinoin to break the viral lipid protein by controlling the growth and differentiation of keratinocytes, affecting the body’s immune response by producing cytokines, and inducing inflammation. The patient in this case report was treated with tretinoin 0.05% at night for 8 weeks, but there was no improvement in the lesions. Glycolic acid (GA) is one of the alpha hydroxy acids (AHA) belonging to the family of carboxylic acids derived from sugarcane.Citation28 At low concentrations, AHA causes a decrease in corneocyte adhesion. At higher concentrations they promote epidermolysis. Glycolic acid 20%-70% belongs to superficial peeling agents and has anti-inflammatory, keratolytic, and antioxidant effects. Corneocyte are the main target of GA by increasing breakdown and reducing cohesiveness, leading to desquamation.Citation29 In 2009, Fabbrocini classified GA as very superficial peeling agents (30–50% GA, applied for 1–2 minutes); superficial peeling agents (50–70% GA, applied for 2–5 minutes); and medium-depth peeling agents (70% GA, applied for 3–15 minutes).Citation20 Glycolic acid is available in various concentrations. Concentrations of less than 20% can be used by patients themselves as home peels.Citation30 In this case report, the patient was treated with 20% GA lotion applied every night to the MC papules lesion on the face, right arm and right leg. At first application, the 20% GA lotion was applied for 5 minutes, then rinsed off with water. The application time was increased according to the patient’s endurance. Therapeutic response in the form of lesion rupture and some of the MC papules lesion has become hyperpigmented macules starting from the 2nd to 6th week of observation after regular use for 8 hours. Post-inflammatory hyperpigmentation was found in the lesion areas that had resolved.
Conclusion
Overall, topical 20% glycolic acid can be used for MK therapy with minimal side effects, easy to apply and safe.
Ethic Statement
The publications of images were included in the patient’s consent for publication of the case. Institutional approval has been obtained to publish the case details.
Consent Statement
The authors certify that they have obtained all appropriate patient consent forms. The patient signed a consent form for the publication of the case details and images.
Disclosure
The authors report no conflicts of interest in this work.
Acknowledgments
The authors would like to thank the staff of the Department of Dermatology and Venereology, Faculty of Medicine, Universitas Padjadjaran, Bandung, West Java, Indonesia.
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