Author:
Pena Ana C.,Penacho Nuno,Mancio-Silva Liliana,Neres Rita,Seixas João D.,Fernandes Afonso C.,Romão Carlos C.,Mota Maria M.,Bernardes Gonçalo J. L.,Pamplona Ana
Abstract
ABSTRACTSevere forms of malaria infection, such as cerebral malaria (CM) and acute lung injury (ALI), are mainly caused by the apicomplexan parasitePlasmodium falciparum. Primary therapy with quinine or artemisinin derivatives is generally effective in controllingP. falciparumparasitemia, but mortality from CM and other forms of severe malaria remains unacceptably high. Herein, we report the design and synthesis of a novel carbon monoxide-releasing molecule (CO-RM; ALF492) that fully protects mice against experimental CM (ECM) and ALI. ALF492 enables controlled CO deliveryin vivowithout affecting oxygen transport by hemoglobin, the major limitation in CO inhalation therapy. The protective effect is CO dependent and induces the expression of heme oxygenase-1, which contributes to the observed protection. Importantly, when used in combination with the antimalarial drug artesunate, ALF492 is an effective adjunctive and adjuvant treatment for ECM, conferring protection after the onset of severe disease. This study paves the way for the potential use of CO-RMs, such as ALF492, as adjunctive/adjuvant treatment in severe forms of malaria infection.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Pharmacology (medical),Pharmacology
Cited by
90 articles.
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