A novel Plasmodium-specific prodomain fold regulates the malaria drug target SUB1 subtilase.

Nat Commun

1] Institut Pasteur, Unité d'Immunologie Moléculaires des Parasites, Département de Parasitologie et de Mycologie, F-75015 Paris, France [2] CNRS URA 2581, F-75015 Paris, France.

Published: September 2014

AI Article Synopsis

  • Scientists studied a protein called SUB1 from the malaria parasite Plasmodium vivax, which helps the parasites leave human cells.
  • They found out that SUB1 has a unique structure that includes a special part, like a belt, which helps keep it stable and is important for the parasite's growth.
  • Understanding how SUB1 works could help researchers create new medicines to fight malaria.

Article Abstract

The Plasmodium subtilase SUB1 plays a pivotal role during the egress of malaria parasites from host hepatocytes and erythrocytes. Here we report the crystal structure of full-length SUB1 from the human-infecting parasite Plasmodium vivax, revealing a bacterial-like catalytic domain in complex with a Plasmodium-specific prodomain. The latter displays a novel architecture with an amino-terminal insertion that functions as a 'belt', embracing the catalytic domain to further stabilize the quaternary structure of the pre-protease, and undergoes calcium-dependent autoprocessing during subsequent activation. Although dispensable for recombinant enzymatic activity, the SUB1 'belt' could not be deleted in Plasmodium berghei, suggesting an essential role of this domain for parasite development in vivo. The SUB1 structure not only provides a valuable platform to develop new anti-malarial candidates against this promising drug target, but also defines the Plasmodium-specific 'belt' domain as a key calcium-dependent regulator of SUB1 during parasite egress from host cells.

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Source
http://dx.doi.org/10.1038/ncomms5833DOI Listing

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