Extracellular release of virulence factor major surface protease via exosomes in Leishmania infantum promastigotes

Skye Marshall; Patrick H. Kelly; Brajesh K. Singh; R. Marshall Pope; Peter Kim; Bayan Zhanbolat; Mary E. Wilson; Chaoqun Yao

doi:10.1186/s13071-018-2937-y

Parasites & Vectors (Jun 2018)

Extracellular release of virulence factor major surface protease via exosomes in Leishmania infantum promastigotes

Skye Marshall,
Patrick H. Kelly,
Brajesh K. Singh,
R. Marshall Pope,
Peter Kim,
Bayan Zhanbolat,
Mary E. Wilson,
Chaoqun Yao

Affiliations

Skye Marshall: Department of Biomedical Sciences and One Health Center for Zoonoses and Tropical Veterinary Medicine, Ross University School of Veterinary Medicine
Patrick H. Kelly: Department of Microbiology, University of Iowa
Brajesh K. Singh: Department of Internal Medicine, University of Iowa
R. Marshall Pope: The Proteomics Facility, University of Iowa
Peter Kim: Carver College of Medicine, University of Iowa
Bayan Zhanbolat: Department of Internal Medicine, University of Iowa
Mary E. Wilson: Department of Microbiology, University of Iowa
Chaoqun Yao: Department of Biomedical Sciences and One Health Center for Zoonoses and Tropical Veterinary Medicine, Ross University School of Veterinary Medicine

DOI: https://doi.org/10.1186/s13071-018-2937-y
Journal volume & issue: Vol. 11, no. 1
pp. 1 – 10

Abstract

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Abstract Background The Leishmania spp. protozoa are introduced into humans through a sand fly blood meal, depositing the infectious metacyclic promastigote form of the parasite into human skin. Parasites enter a variety of host cells, although a majority are found in macrophages where they replicate intracellularly during chronic leishmaniasis. Symptomatic leishmaniasis causes considerable human morbidity in endemic regions. The Leishmania spp. evade host microbicidal mechanisms partially through virulence-associated proteins such as the major surface protease (MSP or GP63), to inactivate immune factors in the host environment. MSP is a metalloprotease encoded by a tandem array of genes belonging to three msp gene classes, whose mRNAs are differentially expressed in different life stages of the parasite. Like other cells, Leishmania spp. release small membrane-bound vesicles called exosomes into their environment. The purpose of this study was to detect MSP proteins in exosomal vesicles of Leishmania spp. protozoa. Methods Using mass spectrometry data we determined the profile of MSP class proteins released in L. infantum exosomes derived from promastigotes in their avirulent procyclic (logarithmic) stage and virulent stationary and metacyclic stages. MSP protein isoforms belonging to each of the three msp gene classes could be identified by unique peptides. Results Metacyclic promastigote exosomes contained the highest, and logarithmic exosomes had the lowest abundance of total MSP. Among the MSP classes, MSPC class had the greatest variety of isoforms, but was least abundant in all exosomes. Nonetheless, all MSP classes were present at higher levels in exosomes released from stationary or metacyclic promastigotes than logarithmic promastigotes. Conclusions The data suggest the efficiency of exosome release may be more important than the identity of MSP isoform in determining the MSP content of Leishmania spp. exosomes.

Published in Parasites & Vectors

ISSN: 1756-3305 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Infectious and parasitic diseases
Website: https://parasitesandvectors.biomedcentral.com/

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