November 16, 2016
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IDSA, ASTMH release leishmaniasis guidelines following increase in US cases

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An increase in leishmaniasis cases among travelers, immigrants and soldiers in the United States prompted the Infectious Diseases Society of America and the American Society of Tropical Medicine and Hygiene to develop new evidence-based recommendations.

Perspective from

“Leishmaniasis is an increasingly common infection in ecotourists traveling to Central and South America. Travelers visiting the jungle in the Amazon basin have a high likelihood of being exposed,” Naomi E. Aronson, MD, of the Uniformed Services University of the Health Sciences in Bethesda, Maryland, said in a press release. “The cutaneous and mucosal forms of the infection cause serious scarring and visceral leishmaniasis can be deadly, so timely diagnosis and treatment managed by an infectious disease physician is vital.”

Leishmaniasis is a parasitic disease that is transmitted through the bite of infected sand flies. There are more than 20 Leishmania species that are pathogenic for humans, according to Aronson and colleagues. The parasites are prevalent in more than 90 countries, including Central and South America, Asia, Africa, the Middle East and southern Europe. In the United States, several autochthonous cases have been reported in Texas and Oklahoma; however, almost all leishmaniasis cases in North America occur among immigrants, international travelers and military personnel returning from endemic regions.  

The most common clinical syndromes of Leishmania are cutaneous leishmaniasis (CL), mucosal leishmaniasis (ML) and visceral leishmaniasis (VL). The CDC estimates that 700,000 to 1.2 million cases of CL are reported each year. Skin lesions caused by CL are often painless and may heal on their own. In some cases, Leishmania can spread from the skin to the nasopharyngeal mucosa and cause ML. The disease may damage nasal and pharyngeal structures and could lead to death due to complicating aspiration pneumonia. VL is caused by systemic infection and may be fatal if left untreated. According to the CDC, 200,000 to 400,000 new cases of VL occur each year.

Diagnosing leishmaniasis can be challenging because the clinical manifestations of disease vary and may appear more than a month after exposure. Furthermore, inconsistent study data, the incidence of recurrent infections and limited treatment options make leishmaniasis difficult to treat. The only FDA–approved therapies are IV liposomal amphotericin B (L-AmB) for VL, heat treatment with the ThermoMed device (Thermosurgery Technologies Inc.) for CL, and Impavido (miltefosine; Knight Therapeutics Inc.) for specific cases of CL, ML and VL. Although these therapies are more than 80% effective, they don’t always eradicate the parasite and additional treatment may be necessary, according to the press release. There is no definitive method to parasitologic cure for leishmaniasis; therefore, the IDSA and ASTMH recommend that patients with prior infection avoid donating blood. In addition, a patient’s history of leishmaniasis should be considered before organ and tissue donations. 

Since there are no vaccines or preventive medications for leishmaniasis, travelers visiting endemic areas are urged to wear protective clothing, apply insect repellents containing DEET and use insecticide-impregnated bed nets. If a patient is suspected of having CL, health care providers can use PCR testing or culture to identify the type of Leishmania and determine how to treat the infection. If VL is suspected, physicians can use a rapid diagnostic blood test, rK39 (Kalazar Detect, InBios), and confirm the results with PCR or culture.

According to the guidelines, published in Clinical Infectious Diseases, systemic therapy is recommended for patients with complex CL lesions who are at risk for ML, as well as those with ML and abnormalities compatible with VL. The agent, dose and duration of therapy should be individualized based on the parasite species and host factors. There is no ideal therapy for CL. ML, however, is traditionally treated with a pentavalent antimonial (SbV) compound (20 mg SbV/kg daily IV or intramuscular for 28 to 30 days) or amphotericin B deoxycholate (0.5-1.0 mg/kg IV daily or every other day for a cumulative total of 20-45 mg/kg). More recently, the armamentarium for ML has expanded to include L-AmB (cumulative dose of 20-60 mg/kg) and oral miltefosine (approximately 2.5 mg/kg for 28 days). Patients with VL are recommended to receive 3 mg/kg of L-AmB intravenously on days 1 to 5, 14 and 21; however, certain patients can receive 2.5 mg/kg of oral miltefosine for 28 days. Leishmaniasis treatments vary among immunocompromised patients, such as those with HIV, lymphatic or hematological malignancies, as well as other special populations, including pregnant or lactating women, young children and older adults.

“In general, clinically manifest cases of VL and ML should be treated even in these special populations of persons because the benefits of treatment typically outweigh the risks,” Aronson and colleagues wrote. “Decisions regarding whether and how to treat cases of CL in persons with special characteristics or comorbid conditions should take into account the potential risks and benefits of various approaches, such as initially observing without antileishmanial therapy, deferring treatment, and using local therapy as the sole approach or as a temporizing measure, if otherwise appropriate and feasible.” – by Stephanie Viguers

Disclosure: Aronson received payments from Up to Date. Please see the full study for a list of all other authors’ relevant financial disclosures.