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Lineage-specific proteins essential for endocytosis in trypanosomes

Manna, Paul T.; Obado, Samson O.; Boehm, Cordula; Gadelha, Catarina; Sali, Andrej; Chait, Brian T.; Rout, Michael P.; Field, Mark C.

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Authors

Paul T. Manna

Samson O. Obado

Cordula Boehm

Andrej Sali

Brian T. Chait

Michael P. Rout

Mark C. Field



Abstract

Clathrin-mediated endocytosis (CME) is the most evolutionarily ancient endocytic mechanism known, and in many lineages the sole mechanism for internalisation. Significantly, in mammalian cells CME is responsible for the vast bulk of endocytic flux and has likely undergone multiple adaptations to accommodate specific requirements by individual species. In African trypanosomes, we previously demonstrated that CME is independent of the AP-2 adaptor protein complex, that orthologues to many of the animal and fungal CME protein cohort are absent, and that a novel, trypanosome-restricted protein cohort interacts with clathrin and drives CME. Here, we used a novel cryomilling affinity isolation strategy to preserve transient low-affinity interactions, giving the most comprehensive trypanosome clathrin interactome to date. We identified the trypanosome AP-1 complex, Trypanosoma brucei (Tb)EpsinR, several endosomal SNAREs plus orthologues of SMAP and the AP-2 associated kinase AAK1 as interacting with clathrin. Novel lineage-specific proteins were identified, which we designate TbCAP80 and TbCAP141. Their depletion produced extensive defects in endocytosis and endomembrane system organisation, revealing a novel molecular pathway subtending an early-branching and highly divergent form of CME, which is conserved and likely functionally important across the kinetoplastid parasites.

Citation

Manna, P. T., Obado, S. O., Boehm, C., Gadelha, C., Sali, A., Chait, B. T., …Field, M. C. (2017). Lineage-specific proteins essential for endocytosis in trypanosomes. Journal of Cell Science, 130, 1379-1392. https://doi.org/10.1242/jcs.191478

Journal Article Type Article
Acceptance Date Feb 13, 2017
Online Publication Date Apr 15, 2017
Publication Date May 15, 2017
Deposit Date Sep 14, 2017
Publicly Available Date Feb 28, 2020
Print ISSN 0021-9533
Electronic ISSN 1477-9137
Publisher Company of Biologists
Peer Reviewed Peer Reviewed
Volume 130
Pages 1379-1392
DOI https://doi.org/10.1242/jcs.191478
Public URL https://nottingham-repository.worktribe.com/output/1120707
Publisher URL https://jcs.biologists.org/content/130/8/1379
PMID 28232524

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