DISSEMINATED CUTANEOUS LEISHMANIASIS DUE TO LEISHMANIA GUYANENSIS: CASE OF A PATIENT WITH 425 LESIONS

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DISSEMINATED CUTANEOUS LEISHMANIASIS DUE TO LEISHMANIA GUYANENSIS: CASE OF A PATIENT WITH 425 LESIONS

P. COUPPIÉ, E. CLYTI, D. SAINTE-MARIE, J. P. DEDET, B. CARME, AND R. PRADINAUD
Institut Guyanais de Dermatologie Tropicale, Service de Dermatologieet Service Hospitalo-Universitaire de Parasitologie-Mycologie,Centre Hospitalier de Cayenne, Cayenne, French Guiana; CentreNational de Référence des Leishmanies, CentreHospitalier, Universitaire de Montpellier, Montpellier, France;Equipe d’Accueil, Faculté de Médecine, Antilles-Guyane,Cayenne, French Guiana

ABSTRACT

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ABSTRACT
INTRODUCTION
CASE REPORT
DISCUSSION
REFERENCES

Disseminated cutaneous leishmaniasis is characterized by thepresence of a large ( $≥$ 10) number of lesions at several anatomicsites (head, limbs, and trunk). Most of the lesions are small,papular, and appear simultaneously with or secondarily to oneor several ulcerated lesions of localized cutaneous leishmaniasis.We report the first case of disseminated cutaneous leishmaniasisin French Guiana. It concerns a 24-year-old woman who testednegative for human immunodeficiency virus (HIV). The diseasebegan with three lesions that became ulcerated. One week later,multiple papulo-nodular lesions appeared. We counted a totalof 425 lesions. Leishmania were observed in the lesions. Thespecies involved was L. guyanensis, which has never been describedin a case of disseminated cutaneous leishmaniasis. The patientwas rapidly cured by a single course of pentamidine. Disseminatedcutaneous leishmaniasis should be distinguished from other typesof leishmaniasis with multiple lesions. These include anergicdiffuse cutaneous leishmaniasis, post-kala-azar leishmaniasis,and leishmaniasis associated with HIV infection.

INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
CASE REPORT
DISCUSSION
REFERENCES

Certain forms of cutaneous leishmaniasis result in large numbersof lesions. This is the case for anergic diffuse cutaneous leishmaniasis,post-kala-azar cutaneous leishmaniasis, and cutaneous leishmaniasisarising in a context of immunodeficiency, such as infectionwith human immunodeficiency virus (HIV).

Brazilian scientists have identified another form of cutaneousleishmaniasis, which was named disseminated cutaneous leishmaniasis(DCL).^1–³ This form can be differentiated from classiclocalized cutaneous leishmaniasis (LCL) by the large ( $≥$ 10) numberof lesions, the clinical type of the major elementary lesions(papular and or acneiform), and the weaker response to classictreatments. These non-ulcerated secondary lesions are thoughtto be formed following the dissemination of the protozoan inthe lymph and blood from the initial lesions. The species involvedare Leishmania braziliensis and L. amazonensis.²

In French Guiana, LCL is particularly frequent, with an annualincidence of approximately 0.2%.⁴ Leishmania guyanensis is responsiblefor most of the cases.⁴ We present a patient who developed aform of cutaneous leishmaniasis due to L. guyanensis that metthe criteria for DCL.

CASE REPORT

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ABSTRACT
INTRODUCTION
CASE REPORT
DISCUSSION
REFERENCES

A 24-year-old woman with no particular medical history was hospitalizedin the Dermatology Department of the Centre Hospitalier de Cayennein February 1997. She lived in Cayenne, but for two years, shehad regularly accompanied her husband into a forested area tohelp him to develop a small farm, which involved cutting downtrees.

Upon questioning, the patient described the appearance in December1996 of three cutaneous lesions on her right hand, left breast,and back. About a week later, a profusion of lesions appeared,covering almost her entire body. These lesions gradually increasedin size, while the initial lesions became ulcerated. She consulteda general practitioner in January 1997 who prescribed oxacilline.However, she did not respond to this treatment and she was thenreferred to a dermatologist who admitted her to the DermatologyDepartment of the Centre Hospitalier de Cayenne.

Clinical examination on admission showed the patient to be ingood general condition without fever. She presented cutaneouslesions, most of which were papulonodular, infiltrated, andslightly squamous. Her entire body was affected, with the exceptionof the scalp, palms of the hands, and soles of the feet. Wecounted a total of 425 lesions. The largest lesions, locatedon her back (Figure 1), on the middle finger of her right hand,and on her left breast (Figure 2), were ulcerated and had scabs.Palpation revealed signs of painless, non-inflammatory lymphangitisaround certain lesions, and left inguinal adenopathy. The mucousmembranes, particularly those within the nose, were free oflesions.

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FIGURE 1. Multiple papular lesions and an ulceration on the back of the patient.

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FIGURE 2. Ulceration of a finger and the left breast (initial lesions) of the patient.

Smears were performed from scrapings of an ulceration on theleft breast, of a nodule on the forehead, and of a papulouslesion of the right thigh. Direct examination of skin smearsstained with May-Grünwald-Giemsa dye showed the presenceof numerous Leishmania amastigotes, either scattered or withinmacrophages, in all three smears. Histologic examination showeda diffuse non-granulomatous inflammation of the dermis containingmostly lymphocytes, histiocytes, and plasma cells, and manyintrahistiocytic forms of leishmaniasis, primarily concerningthe subpapillary venular plexus. A strain of Leishmania wasisolated from cultures. Isoenzyme analysis showed that thisstrain was L. guyanensis.

The C-reactive protein concentration was 84 mg/L (normal <5 mg/L). The blood eosinophil count was 680/mm³ and CD4 andCD8 lymphocyte counts were normal. The patient tested negativefor HIV-1. A myelogram showed no Leishmania.

The patient was treated with two deep intramuscular injectionsof pentamidine isethionate (Pentacarinat^®; Aventis, Paris,France), 48 hours apart, with a dose of 4 mg/kg of pentamidinebase used for each injection. One month after treatment, alllesions had healed. A checkup in June 2002 (five years later)showed no recurrence.

The patient’s husband was also examined in February 1997.This 34-year-old man was found to have an isolated ulcero-nodularlesion of the neck. Smears confirmed a diagnosis of localizedcutaneous leishmaniasis (presence of Leishmania). Given theuncomplicated presentation, culture and biopsy were not performed.Clinical cure was obtained in one month with the same pentamidinetreatment as that given to his wife.

DISCUSSION

TOP
ABSTRACT
INTRODUCTION
CASE REPORT
DISCUSSION
REFERENCES

Disseminated cutaneous leishmaniasis has been described in thenorthern and northeastern regions of Brazil.^1–³ In theseregions, DCL has been reported in 0.2–1.9% of cutaneousleishmaniasis cases, depending on the series.³ The disseminationof lesions from initial lesions is observed three days to eightweeks after the appearance of the initial lesions.^2,³ The numberof lesions is generally between 10 and 800.^2,³ Treatment withN-methyl-glucamine antimoniate (Glucantime^®; Aventis) curesleishmaniasis within a year in 40% of patients with DCL.^2,³

Our case had the characteristics of DCL: multiples lesions,mostly papulous, full expression of the disease within a fewweeks, presence of ulcerations at the beginning of the disease,and a good therapeutic response. One course of pentamidine isethionate(Pentacarinat^®), which is an effective treatment for LCLin French Guiana,⁵ cured our patient with no recurrence afterfive years of follow-up. The only discordant feature was theabsence of granuloma on histopathologic examination, but granulomais not always present in lesions of DCL.²

The differential diagnoses we made involved the three otherforms of leishmaniasis in which a large number of lesions occur.The first was anergic DCL. This rare form of cutaneous leishmaniasisis secondary to an underlying deficit in cellular immunity specificfor certain species of Leishmania.⁶ In South America, this formis caused by L. amazonensis. Multiple papulo-nodular non-ulceratedlesions appear progressively over several years of evolution.This clinical form is refractory to treatment. The second waspost-kala-azar dermal leishmaniasis. This form is encounteredprincipally in India.⁷ The cutaneous lesions accompany or followvisceral leishmaniasis caused by L. donovani. The third wascutaneous leishmaniasis associated with immunodeficiency, suchas HIV infection. An increasing number of cases of cutaneousleishmaniasis with profuse lesions, and sometimes with visceralinvolvement, are being reported, particularly in patients withHIV infections.^8–¹⁰

In our patient, the diagnosis of DCL can be rejected by severalarguments: the appearance of the lesions was far too rapid forDCL; the isolated species was not L. amazonensis, the only speciesknown to cause DCL in French Guiana; and treatment led to completecure without recurrence in the five years of follow up. Similarly,post-kala-azar was rejected on epidemiologic and clinical grounds(no L. donovani in French Guiana and no visceral leishmaniasisin our patient). Finally, in the absence of clinical or biologicsigns of immunodepression and given the HIV-negative status,the diagnosis of leishmaniasis associated with immunodeficiencywas rejected.

The dissociated clinical presentation between our patient andher husband suggests that most lesions were caused by hemolymphaticdissemination from the initial lesions. Indeed, the multiplelesions of the patient are probably not due to hundreds of phlebotominebites because if that was the case the husband would also beexpected to have numerous lesions. In addition, upon questioningthe patient did not recall multiple painful insect bites.

A number of arguments suggest that dissemination of the lesionsin DCL is determined by the immunogenetic background of thepatient rather than the specific virulence of the parasite itself:the absence of clustered cases of DCL, the fact that our patient’shusband after probable simultaneous contamination by the sameparasite strain only developed LCL, and the description of anew species implicated in DCL (L. guyanensis) in addition toL. braziliensis and L. amazonensis.

In conclusion, this is the first case of DCL to be reportedin French Guiana. The species isolated from our patient wasL. guyanensis. This observation shows that this species canalso cause the disseminated form of the disease, as has beenshown for L. amazonensis and L. braziliensis.²

Received October 5, 2003. Accepted for publication February 3, 2004.

Authors’ addresses: P. Couppié and R. Pradinaud,Institut Guyanais de Dermatologie Tropicale, Service de DermatologieC. H. de Cayenne, Rue des Flamboyants, BP 6006, 97300 Cayenne,French Guiana, et Equipe d’Accueil 3593, Facultéde Médecine Antilles-Guyane, Telephone: 594-39-53-59,Fax: 594-39-52-83, E-mail: couppie.pierre{at}voila.fr. E. Clytiand D. Sainte-Marie, Institut Guyanais de Dermatologie Tropicale,Service de Dermatologie C. H. de Cayenne, Rue des Flamboyants,BP 6006, 97300 Cayenne, French Guiana. J. P. Dedet, Centre Nationalde Référence des Leishmanies, Centre HospitalierUniversitaire de Montpellier, Montpellier, France. B. Carme,Service Hospitalo-Universitaire de Parasitologie-Mycologie,Centre Hospitalier de Cayenne, French Guiana et Equipe d’Accueil3593, Faculté de Médecine Antilles-Guyane.

REFERENCES

TOP
ABSTRACT
INTRODUCTION
CASE REPORT
DISCUSSION
REFERENCES

Costa JM, Marsden PD, Llanos-Cuentas EA, Netto EM, Carvalho EM, Barral A, Rosa AC, Cuba CC, Magalhaes AV, Barreto AC, 1986. Disseminated cutaneous leishmaniasis in a field clinic in Bahia, Brazil: a report of eight cases. J Trop Med Hyg 89: 319–323.[Medline]
Carvalho EM, Barral A, Costa JM, Bittencourt A, Marsden P, 1994. Clinical and immunopathological aspects of disseminated cutaneous leishmaniasis. Acta Trop 56: 315–325.[Medline]
Turetz ML, Machado PR, Ko AI, Alves F, Bittencourt A, Almeida RP, Mobashery N, Johnson WD Jr, Carvalho EM, 2002. Disseminated leishmaniasis: a new and emerging form of leishmaniasis observed in northeastern Brazil. J Infect Dis 186: 1829–1834.[ISI][Medline]
Carme B, Aznar C, Pradinaud R, 2001. Absence of a proven resurgence of Chagas disease or cutaneous leishmaniasis in French Guiana over the last two decades. Ann Trop Med Parasito 95: 623–625.
Nacher M, Carme B, Sainte Marie D, Couppie P, Clyti E, Guibert P, Pradinaud R, 2001. Influence of clinical presentation on the efficacy of a short course of pentamidine in the treatment of cutaneous leishmaniasis in French Guiana. Ann Trop Med Parasitol 95: 331–336.[ISI][Medline]
Convit J, Pinardi ME, Rondon AJ, 1972. Diffuse cutaneous leishmaniasis: a disease due to an immunological defect of the host. Trans R Soc Trop Med Hyg 66: 603–610.[Medline]
Thakur CP, 1984. Epidemiological, clinical and therapeutic features of Bihar kala-azar (including post kala-azar dermal leishmaniasis). Trans R Soc Trop Med Hyg 78: 391–398.[Medline]
Coura JR, Galvao-Castro B, Grimaldi G, 1987. Disseminated American cutaneous leishmaniasis in a patient with AIDS. Mem Inst Oswaldo Cruz, Rio de Janeiro 82: 581–582[Medline]
Cnudde F, Raccurt C, Boulard F, Terron-Aboud B, Nicolas M, Juminer B, 1994. Diffuse cutaneous leishmaniasis with visceral dissemination in an AIDS patient in Guadeloupe, West Indies. AIDS 8: 559–560.[Medline]
Gillis D, Klaus S, Schnur LF, Piscopos P, Maayan S, Okon E, Engelhard D, 1995. Diffusely disseminated cutaneous Leishmania major infection in a child with acquired immunodeficiency syndrome. Pediatr Infect Dis J 14: 247–249.[Medline]

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