| Literature DB >> 29696751 |
Sarah C Charnaud1, Thorey K Jonsdottir1,2, Paul R Sanders1, Hayley E Bullen1, Benjamin K Dickerman1, Betty Kouskousis1,3, Catherine S Palmer1,3, Halina M Pietrzak1, Annamarie E Laumaea1, Anna-Belen Erazo1, Emma McHugh4, Leann Tilley4, Brendan S Crabb1,2,5, Paul R Gilson1,5.
Abstract
Plasmodium falciparum, which causes malaria, extensively remodels its human host cells, particularly erythrocytes. Remodelling is essential for parasite survival by helping to avoid host immunity and assisting in the uptake of plasma nutrients to fuel rapid growth. Host cell renovation is carried out by hundreds of parasite effector proteins that are exported into the erythrocyte across an enveloping parasitophorous vacuole membrane (PVM). The Plasmodium translocon for exported (PTEX) proteins is thought to span the PVM and provide a channel that unfolds and extrudes proteins across the PVM into the erythrocyte. We show that exported reporter proteins containing mouse dihydrofolate reductase domains that inducibly resist unfolding become trapped at the parasite surface partly colocalizing with PTEX. When cargo is trapped, loop-like extensions appear at the PVM containing both trapped cargo and PTEX protein EXP2, but not additional components HSP101 and PTEX150. Following removal of the block-inducing compound, export of reporter proteins only partly recovers possibly because much of the trapped cargo is spatially segregated in the loop regions away from PTEX. This suggests that parasites have the means to isolate unfoldable cargo proteins from PTEX-containing export zones to avert disruption of protein export that would reduce parasite growth.Entities:
Keywords: zzm321990Plasmodium falciparum; PEXEL; PTEX; erythrocyte; luciferase; malaria; protein export; protein trafficking; translocon
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Year: 2018 PMID: 29696751 DOI: 10.1111/tra.12577
Source DB: PubMed Journal: Traffic ISSN: 1398-9219 Impact factor: 6.215