Abstract
INTRODUCTION:
American tegumentary leishmaniasis (ATL) and leprosy share common areas of prevalence, but reports of coinfection are scarce.
METHODS:
We report a series of 9 ATL-leprosy cases and discuss the association. An integrative diagram to analyze the clinico-immunological features of coinfection with both diseases.
RESULTS:
Nine patients with leishmaniasis (5 cutaneous, 3 mucocutaneous, 1 disseminated case) exhibited concurrent infection with distinct clinical forms of leprosy. Our diagram-based analysis evidenced a divergent clinico-immunological spectrum for each disease in 8 out of 9 cases.
CONCLUSIONS:
The spectrum of ATL-leprosy comorbidity suggests that the host has a specific immune response against each pathogen.
Keywords:
Leishmaniasis; leprosy; Coinfection; Cutaneous leishmaniasis; Mucocutaneous leishmaniasis
American tegumentary leishmaniasis (ATL) and leprosy remain the major neglected diseases in some developing countries11. World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186.,22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61.. Leishmaniasis encompasses a spectrum of vector-borne parasitic infections caused by protozoa belonging to the genus Leishmania, which is represented mainly by the species Leishmania (Leishmania) amazonensis and Leishmania (Viannia) braziliensis, in Brazil11. World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186.. ATL caused by L. (V.) braziliensis initiates as a single skin ulcer or as multiple skin ulcers that can be followed by mucosal involvement months or years later11. World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186.. Leprosy is a chronic infectious disease caused by the non-cultivable bacillus Mycobacterium leprae that affects the skin and peripheral nerves22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61.. Both diseases have become important public health concerns due to their wide geographic distribution, high incidence rates, and clinical manifestations with subsequent permanent serious injuries and mutilations11. World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186.,22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61.. ATL and leprosy are endemic to Brazil, where most of the new cases in the Americas emerge11. World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186.,22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61..
Although both diseases are prevalent in some countries, reports on comorbidity in the same patient are scarce. In 1978, 8 patients with coinfections of leprosy and cutaneous leishmaniasis (CL) were reported in Ethiopia33. Barnetson RSC, Bryceson ADM. Cutaneous leishmaniasis and leprosy. Trans R Soc Trop Med Hyg. 1978;72(2):160-3., followed by reports of ATL-leprosy concurrence in Venezuela44. Torrealba J, Mendoza I, Ocanto T, Barroeta S, Mejia de Alejos MA, Bonfante-Garrido R. Concomitant cutaneous leishmaniasis and leprosy in Venezuela. Trans R Soc Trop Med Hyg . 1995;89(1):69., India55. Patrao NA, Bhat RM, Dandekeri S, Kambil SM. Diffuse cutaneous leishmaniasis in coexistence with leprosy. Int J Dermatol. 2015;54(12):1402-6.,66. Al-Aboud K, Al-Hawasawi K, Ramesh V, Al-Aboud D, Al-Githami A. Linear cutaneous leishmaniasis occurring on a leg affected by tuberculoid leprosy. Br J Dermatol. 2002;147(5):1022-3., Northeastern Brazil77. Costa JML, Saldanha ACR, Melo LS, da Silva AR, Ferreira LA, Costa G, et al. Cutaneous Leishmaniasis (CL) associated with leprosy: a new and emerging clinicoepidemiological entity observed in the northeast of Brazil. Gaz Med Bahia. 2009;79(Supl.3):95-102., Southeastern Brazil88. Goulart IMB, Patrocínio LG, Nishioka SA, Patrocínio JA, Ferreira MS, Fleury RN. Concurrent leprosy and leishmaniasis with mucosal involvement. Lepr Rev. 2002;73(3):283-4.
9. Delobel P, Launois P, Djossou F, Sainte-Marie D, Pradinaud R. American cutaneous leishmaniasis, lepromatous leprosy, and pulmonary tuberculosis coinfection with downregulation of the T-helper 1 cell response. Clin Infect Dis. 2003;37(5):628-33.
10. Azeredo-Coutinho RBG, Matos DCS, Nery JAC, Valete-Rosalino CM, Mendonça SCF. Interleukin-10-dependent down-regulation of interferon-gamma response to Leishmania by Mycobacterium leprae antigens during the clinical course of a coinfection. Braz J Med Biol Res. 2012;45(7):632-6.
11. Di Luca DG, De Andrade PJ, Sales AM, De Menezes VM, Galhardo MC, Pimentel MI, et al. Superposition of leprosy and other neglected tropical diseases in the state of Rio de Janeiro: a case series report. Lepr Rev . 2013;84(4):302-7.-1212. Mercadante LM, Santos MAS, Pegas ES, Kadunc BV. Leprosy and American cutaneous leishmaniasis coinfection. An Bras Dermatol. 2018;93(1):123-5., and Central America1313. Soto LA, Caballero N, Fuentes LR, Muñoz PT, Gómez-Echevarría JR, López MP, et al. Leprosy Associated with Atypical Cutaneous Leishmaniasis in Nicaragua and Honduras. Am J Trop Med Hyg. 2017;97(4)1103-10..
ATL and leprosy share some intriguing features, as both are caused by obligate intracellular organisms and characterized by a spectrum of clinico-immunological manifestations that depend on T-cell-mediated immunity1414. Silveira FT, Lainson R, Corbett CE. Clinical and immunopathological spectrum of American cutaneous leishmaniasis with special reference to the disease in Amazonian Brazil: a review. Mem Inst Oswaldo Cruz. 2004;99(3):239-51.,1515. Polycarpou A, Walker SL, Lockwood DN. New findings in the pathogenesis of leprosy and implications for the management of leprosy. Curr Opin Infect Dis. 2013;26(5):413-9.. Intracellular pathogens such as M. leprae and Leishmania spp. can be effectively controlled by the Th1 CD4+ subpopulation of the T-cell response. The immune hyperergic pole of both ATL and leprosy is characterized by a strong macrophage activation stimulated mainly by interferon (IFN)-γ and interleukin (IL)-2. Clinically, the Th1 pole of leprosy is represented by the paucibacillary (PB) forms indeterminate (I), tuberculoid (TT), and borderline-tuberculoid (BT) of the Ridley-Jopling classification22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61., and that of ATL by the mucocutaneous leishmaniasis (ML) form11. World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186.. These clinical forms typically show a strong reaction in the intradermal lepromin (or Mitsuda) test and the leishmanin (or Montenegro) test, respectively. Furthermore, the anergic pole is characterized by a depressed specific T-cell response with Th2 pole predominance. This pole is represented by the multibacillary (MB) clinical forms of leprosy, borderline-borderline (BB), borderline-lepromatous (BL), and lepromatous leprosy (LL), and by the diffuse anergic cutaneous form of leishmaniasis (CL) caused by L. (L.) amazonensis or the disseminated form (DL) caused by L. (V.) braziliensis infection1414. Silveira FT, Lainson R, Corbett CE. Clinical and immunopathological spectrum of American cutaneous leishmaniasis with special reference to the disease in Amazonian Brazil: a review. Mem Inst Oswaldo Cruz. 2004;99(3):239-51.,1515. Polycarpou A, Walker SL, Lockwood DN. New findings in the pathogenesis of leprosy and implications for the management of leprosy. Curr Opin Infect Dis. 2013;26(5):413-9.. Although ATL-leprosy coinfection in an immunocompetent patient is still a rare occurrence, it is a comorbidity of growing concern. The specific immune response to one disease seems to influence the clinical picture of the other, which explains the unpredictable course and difficult management of both infections occurring in the same patient1010. Azeredo-Coutinho RBG, Matos DCS, Nery JAC, Valete-Rosalino CM, Mendonça SCF. Interleukin-10-dependent down-regulation of interferon-gamma response to Leishmania by Mycobacterium leprae antigens during the clinical course of a coinfection. Braz J Med Biol Res. 2012;45(7):632-6..
We aimed to report a case series of ATL-leprosy coinfections on the basis of an integrative diagram that emphasizes the clinico-laboratory features to establish a possible Th1/Th2 immunological spectrum relationship between these infectious diseases.
Diagnoses of ATL and leprosy were confirmed on the basis of the World Health Organization recommendations11. World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186.,22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61.. For ATL diagnosis, exclusive skin involvement was defined as the CL form, whereas lesions affecting the skin and mucosa or just the mucosa were classified as the ML form. Patients with 10 or more pleomorphic lesions in 2 or more body parts were classified as having DL. The Ridley-Joplin classification was used to determine the clinical form of leprosy22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61.. Leishmanin11. World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186. and lepromin22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61. intradermal tests were performed to assess the cellular immune response. Enzyme-linked immunosorbent assay (ELISA) with an anti-phenolic glycolipid 1 (PGL1) antibody was conducted to measure the humoral response associated with leprosy22. World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61.. Patients were negative for HIV and hepatitis B and C serology, except for case 9 who was positive for hepatitis C. ATL diagnosis was confirmed by polymerase chain reaction (PCR) using primers (forward: based on a minicircle kDNA from the Leishmania sp. 120-bp sequence 5'-(G/C)(G/C)(C/G)CC(A/C)CTAT(A/T)TTACACCCAACCCC-3', reverse: 5'-GGGGAGGGGCGTTCTGCGAA-3') based on the sequence of a minicircle kDNA of Leishmania spp rendering a 120-bp PCR product. The ATL subgenus Viannia was identified by consecutive digestion of the PCR product with the restriction enzymes HaeIII and BsrI. Leprosy was diagnosed by PCR with primers targeting a 336-bp sequence of the M. leprae gene MntH (forward: 5'-CGGCTTCACGTCCAGTTTCTTC-3', reverse: 5'-TAAGTGCCCTCGATGTAAGCGG-3').
Based on the clinico-immunological spectra of ATL and leprosy described in the literature1414. Silveira FT, Lainson R, Corbett CE. Clinical and immunopathological spectrum of American cutaneous leishmaniasis with special reference to the disease in Amazonian Brazil: a review. Mem Inst Oswaldo Cruz. 2004;99(3):239-51.,1515. Polycarpou A, Walker SL, Lockwood DN. New findings in the pathogenesis of leprosy and implications for the management of leprosy. Curr Opin Infect Dis. 2013;26(5):413-9., we generated an integrative figure to identify overlaps between the clinical forms of ATL and leprosy in terms of immunological spectrum and intradermal tests (cellular immune response), serology (humoral response), and histopathology (presence or absence of pathogen)1414. Silveira FT, Lainson R, Corbett CE. Clinical and immunopathological spectrum of American cutaneous leishmaniasis with special reference to the disease in Amazonian Brazil: a review. Mem Inst Oswaldo Cruz. 2004;99(3):239-51.,1515. Polycarpou A, Walker SL, Lockwood DN. New findings in the pathogenesis of leprosy and implications for the management of leprosy. Curr Opin Infect Dis. 2013;26(5):413-9.. This diagram served to clarify and compare the association between both diseases in this case report series (Figure 1A).
(A) Clinical and immunological spectra of American tegumentary leishmaniasis and leprosy and placement of the reported 9 cases within the proposed spectra. (B) Clinical laboratory features of each patient according to the clinical spectrum for leprosy and American tegumentary leishmaniasis. BB: borderline-borderline, BL: borderline-lepromatous, BT: borderline-tuberculoid, CL: cutaneous leishmaniasis, DL: disseminated leishmaniasis, LL: lepromatous leprosy, ML: mucocutaneous leishmaniasis, N.D.: not determined, PGL: phenolic glycolipid 1, TT: tuberculoid leprosy.
The 9 cases were also presented based on their clinical, laboratory, and immunological spectra to identify associations between both diseases (Figure 1B). Tables 1 and 2 summarize the demographical, clinical, and laboratory features of each patient.
Clinical and immunological features of the initially diagnosed disease of 9 patients with American tegumentary leishmaniasis and leprosy in Southeastern Brazil.
Clinical and immunological features of the secondary disease of 9 patients with American tegumentary leishmaniasis and leprosy in Southeastern Brazil
In 3 cases (patients 4, 8, and 9) the subgenera L. Viannia and M. leprae were simultaneously identified by PCR in the same skin or mucosa sample. Three patients (cases 1, 2, and 6) were initially diagnosed with ATL, were treated and cured, and presented again later with clinical features of leprosy. In the remaining 3 patients, the order of disease manifestation was opposite: they first presented with leprosy and later exhibited clinical features of ATL during or after leprosy treatment (cases 3, 5, and 7).
ATL and leprosy share a clinico-immunological spectrum ranging from a strong T-cell response to a predominant B-cell response1414. Silveira FT, Lainson R, Corbett CE. Clinical and immunopathological spectrum of American cutaneous leishmaniasis with special reference to the disease in Amazonian Brazil: a review. Mem Inst Oswaldo Cruz. 2004;99(3):239-51.,1515. Polycarpou A, Walker SL, Lockwood DN. New findings in the pathogenesis of leprosy and implications for the management of leprosy. Curr Opin Infect Dis. 2013;26(5):413-9., but we are the first to compare the spectra of both diseases in a case series.
Concurrent ATL and leprosy have previously been reported33. Barnetson RSC, Bryceson ADM. Cutaneous leishmaniasis and leprosy. Trans R Soc Trop Med Hyg. 1978;72(2):160-3.
4. Torrealba J, Mendoza I, Ocanto T, Barroeta S, Mejia de Alejos MA, Bonfante-Garrido R. Concomitant cutaneous leishmaniasis and leprosy in Venezuela. Trans R Soc Trop Med Hyg . 1995;89(1):69.-55. Patrao NA, Bhat RM, Dandekeri S, Kambil SM. Diffuse cutaneous leishmaniasis in coexistence with leprosy. Int J Dermatol. 2015;54(12):1402-6.,1212. Mercadante LM, Santos MAS, Pegas ES, Kadunc BV. Leprosy and American cutaneous leishmaniasis coinfection. An Bras Dermatol. 2018;93(1):123-5.. Initial MB leprosy manifestation followed by clinical ML several years later has also been described1010. Azeredo-Coutinho RBG, Matos DCS, Nery JAC, Valete-Rosalino CM, Mendonça SCF. Interleukin-10-dependent down-regulation of interferon-gamma response to Leishmania by Mycobacterium leprae antigens during the clinical course of a coinfection. Braz J Med Biol Res. 2012;45(7):632-6.. Both ML and MB leprosy cause latent infections and sometimes decades elapse before these diseases become clinically recognizable1414. Silveira FT, Lainson R, Corbett CE. Clinical and immunopathological spectrum of American cutaneous leishmaniasis with special reference to the disease in Amazonian Brazil: a review. Mem Inst Oswaldo Cruz. 2004;99(3):239-51.,1515. Polycarpou A, Walker SL, Lockwood DN. New findings in the pathogenesis of leprosy and implications for the management of leprosy. Curr Opin Infect Dis. 2013;26(5):413-9., which complicates determination of the time of infection and concomitant manifestation.
The delay in clinical manifestations may also reflect lack of adhesion to treatment of one or both diseases77. Costa JML, Saldanha ACR, Melo LS, da Silva AR, Ferreira LA, Costa G, et al. Cutaneous Leishmaniasis (CL) associated with leprosy: a new and emerging clinicoepidemiological entity observed in the northeast of Brazil. Gaz Med Bahia. 2009;79(Supl.3):95-102.. Case 4 was treated with irregular multidrug therapy for leprosy for 1 year following clinical manifestation of ML, making it practically impossible to determine which disease was contracted first due to the long latency of both diseases. A case series in Ethiopia33. Barnetson RSC, Bryceson ADM. Cutaneous leishmaniasis and leprosy. Trans R Soc Trop Med Hyg. 1978;72(2):160-3. identified patients that presented with leprosy for 2 to 7 years before clinical manifestation of CL. Nevertheless, an exact comparison with our study is difficult because L. (L.) tropica was the causative pathogen in these patients. Likewise, comorbidity of leishmaniasis with the BL clinical leprosy form55. Patrao NA, Bhat RM, Dandekeri S, Kambil SM. Diffuse cutaneous leishmaniasis in coexistence with leprosy. Int J Dermatol. 2015;54(12):1402-6. and TT leprosy66. Al-Aboud K, Al-Hawasawi K, Ramesh V, Al-Aboud D, Al-Githami A. Linear cutaneous leishmaniasis occurring on a leg affected by tuberculoid leprosy. Br J Dermatol. 2002;147(5):1022-3. has been reported in India. Nevertheless, the anergic pole was attributed to the Leishmania spp. complex.
The subgenus L. Viannia was identified in a patient with LL in Venezuela that also showed CL association 5 years after leprosy was diagnosed44. Torrealba J, Mendoza I, Ocanto T, Barroeta S, Mejia de Alejos MA, Bonfante-Garrido R. Concomitant cutaneous leishmaniasis and leprosy in Venezuela. Trans R Soc Trop Med Hyg . 1995;89(1):69.. In 2002, Goulart et al.88. Goulart IMB, Patrocínio LG, Nishioka SA, Patrocínio JA, Ferreira MS, Fleury RN. Concurrent leprosy and leishmaniasis with mucosal involvement. Lepr Rev. 2002;73(3):283-4. reported the first association between ATL caused by the subgenus L. Viannia and leprosy in Southeastern Brazil. Interestingly, this patient presented with the BL leprosy form with septal obstruction and was diagnosed with ML 3 years later88. Goulart IMB, Patrocínio LG, Nishioka SA, Patrocínio JA, Ferreira MS, Fleury RN. Concurrent leprosy and leishmaniasis with mucosal involvement. Lepr Rev. 2002;73(3):283-4., a pattern resembling the time-lapse observed in our case 4. Since then, 8 cases have been reported in the state of Maranhão in Northeastern Brazil, 7 of which experienced BB-CL comorbidity and 1 CL associated with indeterminate leprosy77. Costa JML, Saldanha ACR, Melo LS, da Silva AR, Ferreira LA, Costa G, et al. Cutaneous Leishmaniasis (CL) associated with leprosy: a new and emerging clinicoepidemiological entity observed in the northeast of Brazil. Gaz Med Bahia. 2009;79(Supl.3):95-102..
Genetic variations have been related to infectivity and pathogenicity of Leishmania. Certain L. (V.) braziliensis strains were proposed as causative pathogens for DL which is an emerging in Brazil but has never been reported as a coinfection with leprosy (patient 9). The concomitant chronic hepatitis C infection of this patient may have increased the susceptibility to ATL and leprosy coinfection.
ML is allocated to the maximum resistance pole of the Th1 immune profile. This exacerbated immune response accounts for local mucous destruction1414. Silveira FT, Lainson R, Corbett CE. Clinical and immunopathological spectrum of American cutaneous leishmaniasis with special reference to the disease in Amazonian Brazil: a review. Mem Inst Oswaldo Cruz. 2004;99(3):239-51.. The immune response of ML patients did not resemble the immune spectrum of leprosy in this study1010. Azeredo-Coutinho RBG, Matos DCS, Nery JAC, Valete-Rosalino CM, Mendonça SCF. Interleukin-10-dependent down-regulation of interferon-gamma response to Leishmania by Mycobacterium leprae antigens during the clinical course of a coinfection. Braz J Med Biol Res. 2012;45(7):632-6. (Figure 1). For example, case 2 presented with the LL form in the anergic pole, and high levels of anti-PGL1 antibodies and presence of bacillus-forming globias in the skin confirmed the Th2 immune pattern and consequently deficient macrophage activity in this patient. Nevertheless, the patient exhibited the ML hyperergic pole representing ATL with granulomatous infiltrate and the amastigote form of Leishmania spp. was still present in the histopathological exam. Case 4 also presented with ML with no evidence of previous cutaneous ulcers but with concurrence of the LL clinical form.
The complex interaction between the parasite and the immune response of the host may complicate the interpretation of the ATL spectrum. ML induces a strong Th1 response resulting in a granulomatous immune response. Nonetheless, ML usually results from previous CL that disseminated to the mucosa via the blood or lymphatic system, a process that is probably attributed to failure in the local cellular immune response1010. Azeredo-Coutinho RBG, Matos DCS, Nery JAC, Valete-Rosalino CM, Mendonça SCF. Interleukin-10-dependent down-regulation of interferon-gamma response to Leishmania by Mycobacterium leprae antigens during the clinical course of a coinfection. Braz J Med Biol Res. 2012;45(7):632-6.. Thus, it appears that ML should not be placed within the spectral pole of a strong T-cell immune response.
The fact that the immune response of the host to each of the pathogens may alter the course of the other disease may lead to a clinical picture that differs from that expected for each disease alone, and physicians should be aware that the diagnosis of coinfection could be challenging. Azeredo-Coutinho et al.1010. Azeredo-Coutinho RBG, Matos DCS, Nery JAC, Valete-Rosalino CM, Mendonça SCF. Interleukin-10-dependent down-regulation of interferon-gamma response to Leishmania by Mycobacterium leprae antigens during the clinical course of a coinfection. Braz J Med Biol Res. 2012;45(7):632-6. reported a case of LL with an IL-10-mediated regulatory response controlling the ML immunopathology, which may explain the opposing spectral Th1/Th2 poles for leprosy and ATL observed in cases 2 and 4. Moreover, the genetic profile of the host should be carefully analyzed to identify specific predispositions for ATL and leprosy that possibly explain the infrequent occurrence of both diseases in the same patient.
To our knowledge, this is the first study proposing a comparison between the clinical and laboratory features of ATL and leprosy based on the Th1/Th2 immunological spectrum. The diagram shown here could prove useful to researchers and physicians working in areas where leprosy and leishmaniasis are prevalent (Figure 1A).
Due to the retrospective character of this case series, the genetic background of the patients and certain other parameters such as the immunological profile (e.g., cytokines) and intercurrences during disease progression were not analyzed. Nonetheless, we described important immunological tests and clinical features, allowing us to conduct a clinico-immunological comparison of both diseases in 9 patients.
The cases described herein included patients that were particularly susceptible to a coinfection with ATL and leprosy because they live in an area where both diseases are endemic. Although epidemiological susceptibility is probably the most important risk factor for contracting both diseases, immunological and genetic conditions that favor a coinfection cannot be excluded.
The present study has shown no correlation between the Th1/Th2 immunological spectra of the clinical forms of ATL and leprosy in this case series, which suggests a specific host immune response against each pathogen. Increasing incidence rates of ATL and leprosy concurrence must be acknowledged to improve diagnostic and therapeutic strategies in regions where both diseases are prevalent.
Acknowledgements
We thank Dr. Margarida Moraes for revision of the histopathological laryngeal biopsy and the staff of the Head and Neck Surgery Department for the laryngoscope exam of case 2. We further thank Dr. Marcela A. Ambiel, Dr. Norma T. Foss, and the clinical staff at the University Hospital for assessing the ATL and leprosy outpatients. We thank the biologists Flavia T. A. Vieira, Natalia A. de Paula, and Sandra Silva Rodrigues Santos for their support in the laboratory.
REFERENCES
-
1World Health Organization (WHO). Control of the leishmaniasis. World Health Organ Tech Rep Ser. 2010;949(XII-XIII):1-186.
-
2World Health Organization (WHO). WHO Expert Committee on Leprosy. World Health Organ Tech Rep Ser . 2012;968:1-61.
-
3Barnetson RSC, Bryceson ADM. Cutaneous leishmaniasis and leprosy. Trans R Soc Trop Med Hyg. 1978;72(2):160-3.
-
4Torrealba J, Mendoza I, Ocanto T, Barroeta S, Mejia de Alejos MA, Bonfante-Garrido R. Concomitant cutaneous leishmaniasis and leprosy in Venezuela. Trans R Soc Trop Med Hyg . 1995;89(1):69.
-
5Patrao NA, Bhat RM, Dandekeri S, Kambil SM. Diffuse cutaneous leishmaniasis in coexistence with leprosy. Int J Dermatol. 2015;54(12):1402-6.
-
6Al-Aboud K, Al-Hawasawi K, Ramesh V, Al-Aboud D, Al-Githami A. Linear cutaneous leishmaniasis occurring on a leg affected by tuberculoid leprosy. Br J Dermatol. 2002;147(5):1022-3.
-
7Costa JML, Saldanha ACR, Melo LS, da Silva AR, Ferreira LA, Costa G, et al. Cutaneous Leishmaniasis (CL) associated with leprosy: a new and emerging clinicoepidemiological entity observed in the northeast of Brazil. Gaz Med Bahia. 2009;79(Supl.3):95-102.
-
8Goulart IMB, Patrocínio LG, Nishioka SA, Patrocínio JA, Ferreira MS, Fleury RN. Concurrent leprosy and leishmaniasis with mucosal involvement. Lepr Rev. 2002;73(3):283-4.
-
9Delobel P, Launois P, Djossou F, Sainte-Marie D, Pradinaud R. American cutaneous leishmaniasis, lepromatous leprosy, and pulmonary tuberculosis coinfection with downregulation of the T-helper 1 cell response. Clin Infect Dis. 2003;37(5):628-33.
-
10Azeredo-Coutinho RBG, Matos DCS, Nery JAC, Valete-Rosalino CM, Mendonça SCF. Interleukin-10-dependent down-regulation of interferon-gamma response to Leishmania by Mycobacterium leprae antigens during the clinical course of a coinfection. Braz J Med Biol Res. 2012;45(7):632-6.
-
11Di Luca DG, De Andrade PJ, Sales AM, De Menezes VM, Galhardo MC, Pimentel MI, et al. Superposition of leprosy and other neglected tropical diseases in the state of Rio de Janeiro: a case series report. Lepr Rev . 2013;84(4):302-7.
-
12Mercadante LM, Santos MAS, Pegas ES, Kadunc BV. Leprosy and American cutaneous leishmaniasis coinfection. An Bras Dermatol. 2018;93(1):123-5.
-
13Soto LA, Caballero N, Fuentes LR, Muñoz PT, Gómez-Echevarría JR, López MP, et al. Leprosy Associated with Atypical Cutaneous Leishmaniasis in Nicaragua and Honduras. Am J Trop Med Hyg. 2017;97(4)1103-10.
-
14Silveira FT, Lainson R, Corbett CE. Clinical and immunopathological spectrum of American cutaneous leishmaniasis with special reference to the disease in Amazonian Brazil: a review. Mem Inst Oswaldo Cruz. 2004;99(3):239-51.
-
15Polycarpou A, Walker SL, Lockwood DN. New findings in the pathogenesis of leprosy and implications for the management of leprosy. Curr Opin Infect Dis. 2013;26(5):413-9.
-
Financial Support: This research was not funded by any specific grant from a funding agency. SV received a PhD scholarship from CAPES (Coordenação de Aperfeiçoamento de Pessoal de Nível Superior).
Publication Dates
-
Publication in this collection
11 Apr 2019 -
Date of issue
2019
History
-
Received
10 May 2018 -
Accepted
05 Dec 2018