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Leishmaniasis

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19 71. Secondary prophylaxis is NOT recommended for initial management in persons with VL who have not manifested a relapse (W-L). Remark: Immunosuppressed persons with VL who are not coinfected with HIV typically have higher response rates to initial treatment and lower recurrence rates than HIV-coinfected persons. 72. Routine serologic screening of organ donors from leishmaniasis- endemic areas is NOT recommended. If an available donor is known to be seropositive, it is advisable to perform clinical and laboratory monitoring of the recipient in the post-transplant period rather than to reject the organ for transplant (S-L). 73. The Panel suggests that clinicians NOT routinely perform diagnostic testing to assess persons for evidence of asymptomatic visceral infection, including persons who have lived or traveled in leishmaniasis-endemic regions (Figure 3) and are considering organ transplantation or initiation of therapy with biologic immunomodulating agents. Immunosuppressed persons known or found to be asymptomatically infected and those with a history of VL warrant close monitoring. Neither preemptive treatment nor primary prophylaxis for VL in asymptomatically infected persons is suggested (W-VL). 74. Immunosuppressed persons with VL who are not coinfected with HIV should be monitored for ≥1 year (ideally lifelong or until effective immune reconstitution) to assess for posttreatment relapse. During clinical follow-up, assess for symptoms and, if present, pursue parasitologic confirmation of relapse (S-VL). 75. Confirmed VL therapeutic failure typically can be managed by retreatment using L-AmB at the same or a higher total dose (S-VL). Remark: Pentavalent antimonials could be used in some persons with VL under close follow-up. 76. The Panel suggests that CL/ML associated with the use of tumor necrosis factor (TNF)-alpha antagonist therapy be managed with systemic therapy and standard drug regimens for the pertinent setting/species (eg, geographic area where the infection was acquired) (W-VL). Remark: Withdrawal of TNF-α antagonists during antileishmanial therapy may be appropriate: the risks, benefits, and feasibility of this action should be assessed on a case-by-case basis.

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