The Plasmodium falciparum exportome contains non‐canonical PEXEL/HT proteins |
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Authors: | Jana Schulze Marcel Kwiatkowski Janus Borner Hartmut Schlüter Iris Bruchhaus Thorsten Burmester Christian Pick |
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Affiliation: | 1. University of Hamburg, Institute of Zoology, Hamburg, Germany;2. Department of Clinical Chemistry, University Medical Center Hamburg‐Eppendorf, Hamburg, Germany;3. Bernhard Nocht Institute for Tropical Medicine, Hamburg, Germany |
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Abstract: | The pathogenicity of Plasmodium falciparum is partly due to parasite‐induced host cell modifications. These modifications are facilitated by exported P. falciparum proteins, collectively referred to as the exportome. Export of several hundred proteins is mediated by the PEXEL/HT, a protease cleavage site. The PEXEL/HT is usually comprised of five amino acids, of which R at position 1, L at position 3 and E, D or Q at position 5 are conserved and important for export. Non‐canonical PEXEL/HTs with K or H at position 1 and/or I at position 3 are presently considered non‐functional. Here, we show that non‐canonical PEXEL/HT proteins are overrepresented in P. falciparum and other Plasmodium species. Furthermore, we show that non‐canonical PEXEL/HTs can be cleaved and can promote export in both a REX3 and a GBP reporter, but not in a KAHRP reporter, indicating that non‐canonical PEXEL/HTs are functional in concert with a supportive sequence environment. We then selected P. falciparum proteins with a non‐canonical PEXEL/HT and show that some of these proteins are exported and that their export depends on non‐canonical PEXEL/HTs. We conclude that PEXEL/HT plasticity is higher than appreciated and that non‐canonical PEXEL/HT proteins cannot categorically be excluded from Plasmodium exportome predictions. |
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