Compartilhar
Informação da revista
Vol. 94. Núm. 3.
Páginas 355-357 (1 maio 2019)
Compartilhar
Compartilhar
Baixar PDF
Mais opções do artigo
Vol. 94. Núm. 3.
Páginas 355-357 (1 maio 2019)
Open Access
American tegumentary leishmaniasis: severe side effects of pentavalent antimonial in a patient with chronic renal failure*
Visitas
4847
Sílvio Alencar Marques1, Maira Renata Merlotto1, Paulo Müller Ramos1, Mariangela Esther Alencar Marques2
1 Department of Dermatology, Faculdade de Medicina de Botucatu, Universidade Estadual Paulista, Botucatu (SP), Brazil.
2 Department of Pathology, Faculdade de Medicina de Botucatu, Universidade Estadual Paulista, Botucatu (SP), Brazil.
Este item recebeu

Under a Creative Commons license
Informação do artigo
Resume
Texto Completo
Bibliografia
Baixar PDF
Estatísticas
Figuras (4)
Mostrar maisMostrar menos

Pentavalent antimonials are the first-line drug treatment for American tegumentary leishmaniasis. We report on a patient with chronic renal failure on hemodialysis who presented with cutaneous lesions of leishmaniasis for four months. The patient was treated with intravenous meglumine under strict nephrological surveillance, but cardiotoxicity, acute pancreatitis, pancytopenia, and cardiogenic shock developed rapidly. Deficient renal clearance of meglumine antimoniate can result in severe toxicity, as observed in this case. These side effects are related to cumulative plasma levels of the drug. Therefore, second-line drugs like amphotericin B are a better choice for patients on dialysis.

Keywords:
Amphotericin B
Kidney failure, chronic
Leishmaniasis
Leishmaniasis, cutaneous
Meglumine
Pancreatitis
Renal insufficiency, chronic
Skin ulcer
Texto Completo

American tegumentary leishmaniasis (ATL) is an endemic parasitic disease that in Brazil is caused mostly by Leishmania (Viannia) braziliensis.1 Pentavalent antimonials are the first-line drug treatment for ATL.2,3 Musculoskeletal pain, headache, nausea, and asthenia are reported as common side effects, and cardiotoxicity, hepatotoxicity, nephrotoxicity, and pancreatitis as rare, and associated with cumulative doses. 4-7 The authors report severe side effects associated with the use of meglumine antimoniate (Glucantime®) in a patient presenting chronic renal failure (CRF) due to systemic hypertension, on hemodialysis for two years.

A 42-year-old male patient from São Paulo State, Brazil, complained of rapidly growing cutaneous lesions on the face for four months. Upon examination we observed an ulcerated and verrucous lesion measuring 10.0 cm on the left malar-zygomatic region associated with similar lesions on the lower lip and right infra-au-ricular area. (Figures 1 and 2). Clinical examination was unremarkable. With the hypothesis of paracoccidioidomycosis or leishmaniasis, the patient underwent a biopsy, and the anatomopathological exam showed chronic inflammatory infiltrate with lymphocytes, plasma cells, and epithelioid granulomas. Amastigotes were seen in the cytoplasm of macrophages, confirming leishmaniasis (Figures 3 and 4). Montenegro skin test was positive, measuring 15 x 15mm. Pre-treatment laboratory workup revealed anemia and confirmed the patient's renal failure. Other exams were normal or negative including HIV serology. Following the nephrological evaluation, we initiated Glucantime® 13.5mg/Sbv/kg/IV/daily with the patient hospitalized and under monitored management and routine hemodialysis sessions. On treatment day 5, the patient presented transient supraventricular arrhythmia during Glucantime® administration, which was interrupted. On the same day, the patient developed signs and symptoms of severe acute pancreatitis (Ranson 3), rising liver enzymes, pancytopenia (hemoglobin = 6.9 g/dl; white blood cells = 2600/mm3; platelets = 52000/ mm3), and shock. Transferred to the ICU, the patient quickly recovered from shock under volume replacement and vasoactive drugs, but symptomatic improvement of pancreatitis was slow. Although the antimonial treatment was discontinued, surprisingly the cutaneous lesions nearly vanished in a short period of time. With clinical improvement and a residual lesion, we started amphotericin B deoxycholate 0.5mg/kg/daily on hospital day (HD) 28, in maintenance hemodialysis and support treatment. The patient was discharged on HD 50 in good health and complete resolution of lesions. One year later he was submitted to renal transplantation and is currently in good clinical condition.

Figure 1.

Leishmaniasis: ulcerated and verrucous lesion on the left malar-zygomatic region. Ulcerated and infiltrated lesion on the lower-lip

(0.03MB).
Figure 2.

Leishmaniasis: ulcerated lesion, partially covered by crusts with infiltrated edges on the right infra-auricular area.

(0.03MB).
Figure 3.

Leishmaniasis: pseudo-hyperplasia of the epidermis plus chronic inflammatory infiltrate with lymphocytes, plasma cells, and epithelioid granulomas. (hematoxylin & eosin x400)

(0.04MB).
Figure 4.

Leishmaniasis: close-up showing amastigotes in the cytoplasm of macrophages. (Hematoxylin & eosin x1000/oil)

(0.03MB).

Glucantime® is excreted 80% through the kidneys as active drug.8 Therefore, there are strict limits for its use in patients presenting reduced renal clearence.9 Management of this clinical case was initially based on the assumption that hemodialysis would be capable of filtering the antimonial, which did not occur or only occurred partially, resulting in drug accumulation up to 4050 mg/Sbv (810mg/Sbv/day). Consequently, side effects appeared quickly and were severe, particularly cardiotoxicity and pancreatitis. When a patient presents with definitive and total renal failure, the suggestion is to prescribe amphotericin B deoxycholate, which is eliminated mainly by metabolism and is a dialyzable drug, with the liposomal formulation as an alternative.10 A beneficial effect of the high plasma antimonial level was the fast and almost complete resolution of the leishmaniasis cutaneous lesions.

References
[1.]
Anversa L, Tiburcio MGS, Richini-Pereira VB, Ramirez LE..
Human leishmaniasis in Brazil: a general review..
Rev Assoc Med Bras (1992)., 64 (2018), pp. 281-289
[2.]
Almeida OL, Santos JB..
Advances in the treatment of cutaneous leishmaniasis in the New World in the last ten years: a systematic literature review.
An Bras Dermatol., 86 (2011), pp. 497-506
[3.]
Reveiz L, Maia-Elkhoury AN, Nicholls RS, Romero GA, Yadon ZE..
Intervention for American cutaneous and mucocutaneous leishmaniasis: A systematic review update..
[4.]
Oliveira LF, Schubach AO, Martins MM, Passos SL, Oliveira RV, Marzochi MC, et al.
Systematic review of the adverse effects of cutaneous leishmaniasis treatment in the New World..
[5.]
Clementi A, Battaglia G, Floris M, Castellino P, Ronco C, Cruz DN..
Renal involvement in leishmaniasis: a review of the literature..
NDT Plus., 4 (2011), pp. 147-152
[6.]
Lyra MR, Passos SR, Pimentel MI, Bedoya-Pacheco SJ, Valete-Rosalino CM, Vasconcellos EC, et al.
Pancreatic toxicity as an adverse effect induced by meglumine antimoniate therapy in a clinical trial for cutaneous leishmaniasis..
Rev Inst Med Trop Sao Paulo., 58 (2016), pp. 68
[7.]
El Jeri HK, Harzallah A, Barbouch S, Bacha MM, Kheder R, Turki S, et al.
Visceral leishmaniasis in adults with nephropathy..
Saudi J Kidney Dis Transpl., 28 (2017), pp. 95-101
[8.]
Portal.anvisa.gov.br [Internet]. Agência Nacional de Vigilância Sanitária (ANVISA). Glucantime® (antimoniato de meglumine). [cited 2018 Apr 6]. Available from: http://portal.anvisa.gov.br/datavisa/fila_bula/frmVisualizarBula.asp?pNuTransacao=991282015&pIdAnexo=2435258
[9.]
Fontenele E, Silva JS, Galvao TF, Pereira MG, Silva MT..
Treatment of American tegumentary leishmaniasis in special population: a summary of evidence..
Rev Soc Bras Med Trop., 46 (2013), pp. 669-677
[10.]
Bellmann R, Smuszkiewicz P..
Pharmacokinetics of antifungal drugs: practical implications for optimized treatment of patients..
Infection., 45 (2017), pp. 737-739

Work conducted at the Department of Dermatology and Radiotherapy, Faculdade de Medicina de Botucatu, Universidade Estadual Paulista, Botucatu (SP), Brazil.

Copyright © 2019. Anais Brasileiros de Dermatologia
Baixar PDF
Idiomas
Anais Brasileiros de Dermatologia (Portuguese)
Opções de artigo
Ferramentas
en pt
Cookies policy Política de cookies
To improve our services and products, we use "cookies" (own or third parties authorized) to show advertising related to client preferences through the analyses of navigation customer behavior. Continuing navigation will be considered as acceptance of this use. You can change the settings or obtain more information by clicking here. Utilizamos cookies próprios e de terceiros para melhorar nossos serviços e mostrar publicidade relacionada às suas preferências, analisando seus hábitos de navegação. Se continuar a navegar, consideramos que aceita o seu uso. Você pode alterar a configuração ou obter mais informações aqui.