20S proteasomes secreted by the malaria parasite promote its growth

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作者
Elya Dekel
Dana Yaffe
Irit Rosenhek-Goldian
Gili Ben-Nissan
Yifat Ofir-Birin
Mattia I. Morandi
Tamar Ziv
Xavier Sisquella
Matthew A. Pimentel
Thomas Nebl
Eugene Kapp
Yael Ohana Daniel
Paula Abou Karam
Daniel Alfandari
Ron Rotkopf
Shimrit Malihi
Tal Block Temin
Debakshi Mullick
Or-Yam Revach
Ariel Rudik
Nir S. Gov
Ido Azuri
Ziv Porat
Giulia Bergamaschi
Raya Sorkin
Gijs J. L. Wuite
Ori Avinoam
Teresa G. Carvalho
Sidney R. Cohen
Michal Sharon
Neta Regev-Rudzki
机构
[1] Weizmann Institute of Science,Department of Biomolecular Sciences
[2] Weizmann Institute of Science,Department of Chemical Research Support
[3] Technion - Israel Institute of Technology,Smoler Proteomics Center, Department of Biology
[4] The Walter and Eliza Hall Institute of Medical Research,Department of Medical Biology
[5] The University of Melbourne,Bioinformatics Unit, Department of Life Sciences Core Facilities
[6] Weizmann Institute of Science,Department of Chemical and Biological Physics
[7] Weizmann Institute of Science,Department of Physics and Astronomy and LaserLab
[8] Flow Cytometry Unit,School of Chemistry
[9] Life Sciences Core Facilities,Center for Physics and Chemistry of Living Systems
[10] Weizmann Institute of Science,Department of Physiology, Anatomy and Microbiology
[11] Vrije Universiteit Amsterdam,undefined
[12] Tel Aviv University,undefined
[13] Tel Aviv University,undefined
[14] La Trobe University,undefined
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摘要
Mature red blood cells (RBCs) lack internal organelles and canonical defense mechanisms, making them both a fascinating host cell, in general, and an intriguing choice for the deadly malaria parasite Plasmodium falciparum (Pf), in particular. Pf, while growing inside its natural host, the human RBC, secretes multipurpose extracellular vesicles (EVs), yet their influence on this essential host cell remains unknown. Here we demonstrate that Pf parasites, cultured in fresh human donor blood, secrete within such EVs assembled and functional 20S proteasome complexes (EV-20S). The EV-20S proteasomes modulate the mechanical properties of naïve human RBCs by remodeling their cytoskeletal network. Furthermore, we identify four degradation targets of the secreted 20S proteasome, the phosphorylated cytoskeletal proteins β-adducin, ankyrin-1, dematin and Epb4.1. Overall, our findings reveal a previously unknown 20S proteasome secretion mechanism employed by the human malaria parasite, which primes RBCs for parasite invasion by altering membrane stiffness, to facilitate malaria parasite growth.
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