Literature DB >> 11897123

Characterization of proteases involved in the processing of Plasmodium falciparum serine repeat antigen (SERA).

Jie Li1, Hiroyuki Matsuoka, Toshihide Mitamura, Toshihiro Horii.   

Abstract

The Plasmodium falciparum serine repeat antigen (SERA), a malaria vaccine candidate, is processed into several fragments (P73, P47, P56, P50, and P18) at the late schizont stage prior to schizont rupture in the erythrocytic cycle of the parasite. We have established an in vitro cell-free system using a baculovirus-expressed recombinant SERA (bvSERA) that mimics the SERA processing that occurs in parasitized erythrocytes. SERA processing was mediated by parasite-derived trans-acting proteases, but not an autocatalytic event. The processing activities appeared at late schizont stage. The proteases are membrane associated, correlating with the secretion and accumulation of SERA within the parasitophorous vacuole membrane (PVM). The activity responsible for the primary processing step of SERA to P47 and P73 was inhibited by serine protease inhibitor DFP. In contrast, the activity responsible for the conversion of P56 into P50 was inhibited by each of the cysteine protease inhibitors E-64, leupeptin and iodoacetoamide. Moreover, addition of DFP, E-64 or leupeptin to the cultures of schizont-stage parasites blocked schizont rupture and release of merozoites from PVM. These results indicate that SERA processing correlates to schizont rupture and the processing is mediated by at least three distinct proteases.

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Year:  2002        PMID: 11897123     DOI: 10.1016/s0166-6851(01)00452-2

Source DB:  PubMed          Journal:  Mol Biochem Parasitol        ISSN: 0166-6851            Impact factor:   1.759


  16 in total

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3.  Immunomic Identification of Malaria Antigens Associated With Protection in Mice.

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4.  Data-mining approaches reveal hidden families of proteases in the genome of malaria parasite.

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Journal:  Genome Res       Date:  2003-04       Impact factor: 9.043

Review 5.  Plasmodium falciparum apicoplast and its transcriptional regulation through calcium signaling.

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6.  Regulated maturation of malaria merozoite surface protein-1 is essential for parasite growth.

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7.  Inhibition of malaria parasite development by a cyclic peptide that targets the vital parasite protein SERA5.

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8.  Irreversible effect of cysteine protease inhibitors on the release of malaria parasites from infected erythrocytes.

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9.  Phylogeny and evolution of the SERA multigene family in the genus Plasmodium.

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Review 10.  Malarial proteases and host cell egress: an 'emerging' cascade.

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