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LISP1 is important for the egress of Plasmodium berghei parasites from liver cells |
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| Authors: | Tomoko Ishino,Bertrand Boisson,Yuki Orito,Cé line Lacroix,Emmanuel Bischoff,Cé line Loussert,Chris Janse,Robert Mé nard,Masao Yuda , Patricia Baldacci |
| Affiliation: | Institut Pasteur, Biologie et Génétique du Paludisme, 75724 Paris cedex 15, France.; Department of Medical Zoology, Mie University School of Medecine, Mie 514-0001, Japan.; Institut Pasteur, Plateforme Puces àADN Génopole, Paris, France.; Institut Pasteur, Plateforme de Microscopie Ultrastructurale, Paris, France.; Department of Parasitology, Leiden University Medical Centre, Leiden, the Netherlands. |
| Abstract: | Most Apicomplexa are obligatory intracellular parasites that multiply inside a so-called parasitophorous vacuole (PV) formed upon parasite entry into the host cell. Plasmodium , the agent of malaria and the Apicomplexa most deadly to humans, multiplies in both hepatocytes and erythrocytes in the mammalian host. Although much has been learned on how Apicomplexa parasites invade host cells inside a PV, little is known of how they rupture the PV membrane and egress host cells. Here, we characterize a Plasmodium protein, called LISP1 ( li ver- s pecific p rotein 1), which is specifically involved in parasite egress from hepatocytes. LISP1 is expressed late during parasite development inside hepatocytes and locates at the PV membrane. Intracellular parasites deficient in LISP1 develop into hepatic merozoites, which display normal infectivity to erythrocytes. However, LISP1-deficient liver-stage parasites do not rupture the membrane of the PV and remain trapped inside hepatocytes. LISP1 is the first Plasmodium protein shown by gene targeting to be involved in the lysis of the PV membrane. |
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