Schistosome blood flukes cause more mortality and morbidity than any other human worm infection, but current control methods primarily rely on a single drug. There is a desperate need for new approaches to control this parasite, including vaccines. People become infected when the free-swimming larva, the cercaria, enters through the skin and becomes the schistosomulum. Schistosomula are susceptible to immune responses during their first few days in the host before they become adult parasites. We characterised the genes that these newly transformed parasites switch on when they enter the host to identify molecules that are critical for survival in the human host. Some of these highly up-regulated genes can be targeted for future development of new vaccines and drugs

A Loukas

A Sher

AD Aragon

AJ Simpson

Alex Loukas

AP Mountford

BH Kalinna

BW van Balkom

CA Peck

CM Fitzsimmons

CR Caffrey

Donald P. McManus

DP McManus

EJ Pearce

Elodie Ghedin

ER James

ER Jolly

FC Cardoso

G Payares

Geoffrey N. Gobert

GN Gobert

GP Dillon

GR Newport

H You

J Deng

J Jang-Lee

JA Clegg

Jason Mulvenna

JH McKerrow

JK Lazdins

JM Correnti

JP Salter

JS Morey

L Moertel

LG Pacifico

Luke Moertel

M Berriman

Mai H. Tran

Malcolm K. Jones

MD Wright

ME Morales

MH Tran

MJ Doenhoff

MK Jones

MR Kasschau

O Emanuelsson

OL Goldring

PF Basch

PJ Skelly

PS Coulson

R Correa-Oliveira

R DeMarco

R El Ridi

R Moqbel

R Perez-Sanchez

RA Wilson

S Braschi

S Verjovski-Almeida

SA Bustin

SG Forrester

T Kawamoto

TA Don

TA Patterson

WM Kemp

Y Zhou

YL Lin

Z Zhou

PLoS Neglected Tropical Diseases

English

PubMed

Background: Schistosomes cause more mortality and morbidity than any other human helminth, but control primarily relies on a single drug that kills adult worms. The newly transformed schistosomulum stage is susceptible to the immune response and is a target for vaccine development and rational drug design.\ud
\ud
Methodology/Principal Findings: To identify genes which are up-regulated during the maturation of Schistosoma mansoni schistosomula in vitro, we cultured newly transformed parasites for 3 h or 5 days with and without erythrocytes and compared their transcriptional profiles using cDNA microarrays. The most apparent changes were in the up-regulation of genes between 3 h and 5 day schistosomula involved in blood feeding, tegument and cytoskeletal development, cell adhesion, and stress responses. The most highly up-regulated genes included a tegument tetraspanin Sm-tsp-3 (1,600-fold up-regulation), a protein kinase, a novel serine protease and serine protease inhibitor, and intestinal proteases belonging to distinct mechanistic classes. The inclusion of erythrocytes in the culture medium resulted in a general but less pronounced increase in transcriptional activity, with the highest up-regulation of genes involved in iron metabolism, proteolysis, and transport of fatty acids and sugars.\ud
\ud
Conclusions: We have identified the genes that are up-regulated during the first 5 days of schistosomula development in vitro. Using a combination of gene silencing techniques and murine protection studies, some of these highly up-regulated transcripts can be targeted for future development of new vaccines and drugs

Gobert, Geoffrey N.

Tran, Mai H.

Moertel, Luke

Mulvenna, Jason

Jones, Malcolm K.

McManus, Donald P.

Loukas, Alex

ResearchOnline@JCU

Transcriptional changes in Schistosoma mansoni during early schistosomula development and in the presence of erythrocytes

Background: Schistosomes cause more mortality and morbidity than any other human helminth, but control primarily relies on a single drug that kills adult worms. The newly transformed schistosomulum stage is susceptible to the immune response and is a target for vaccine development and rational drug design.



Methodology/Principal Findings: To identify genes which are up-regulated during the maturation of Schistosoma mansoni schistosomula in vitro, we cultured newly transformed parasites for 3 h or 5 days with and without erythrocytes and compared their transcriptional profiles using cDNA microarrays. The most apparent changes were in the up-regulation of genes between 3 h and 5 day schistosomula involved in blood feeding, tegument and cytoskeletal development, cell adhesion, and stress responses. The most highly up-regulated genes included a tegument tetraspanin Sm-tsp-3 (1,600-fold up-regulation), a protein kinase, a novel serine protease and serine protease inhibitor, and intestinal proteases belonging to distinct mechanistic classes. The inclusion of erythrocytes in the culture medium resulted in a general but less pronounced increase in transcriptional activity, with the highest up-regulation of genes involved in iron metabolism, proteolysis, and transport of fatty acids and sugars.



Conclusions: We have identified the genes that are up-regulated during the first 5 days of schistosomula development in vitro. Using a combination of gene silencing techniques and murine protection studies, some of these highly up-regulated transcripts can be targeted for future development of new vaccines and drugs

ResearchOnline at James Cook University

Crossref

BACKGROUND: Schistosomes cause more mortality and morbidity than any other human helminth, but control primarily relies on a single drug that kills adult worms. The newly transformed schistosomulum stage is susceptible to the immune response and is a target for vaccine development and rational drug design. METHODOLOGY/PRINCIPAL FINDINGS: To identify genes which are up-regulated during the maturation of Schistosoma mansoni schistosomula in vitro, we cultured newly transformed parasites for 3 h or 5 days with and without erythrocytes and compared their transcriptional profiles using cDNA microarrays. The most apparent changes were in the up-regulation of genes between 3 h and 5 day schistosomula involved in blood feeding, tegument and cytoskeletal development, cell adhesion, and stress responses. The most highly up-regulated genes included a tegument tetraspanin Sm-tsp-3 (1,600-fold up-regulation), a protein kinase, a novel serine protease and serine protease inhibitor, and intestinal proteases belonging to distinct mechanistic classes. The inclusion of erythrocytes in the culture medium resulted in a general but less pronounced increase in transcriptional activity, with the highest up-regulation of genes involved in iron metabolism, proteolysis, and transport of fatty acids and sugars. CONCLUSIONS: We have identified the genes that are up-regulated during the first 5 days of schistosomula development in vitro. Using a combination of gene silencing techniques and murine protection studies, some of these highly up-regulated transcripts can be targeted for future development of new vaccines and drugs

Geoffrey N Gobert

Mai H Tran

Malcolm K Jones

Donald P McManus

Directory of Open Access Journals

Transcriptional changes in Schistosoma mansoni during early schistosomula development and in the presence of erythrocytes.

Schistosomes cause more mortality and morbidity than any other human helminth, but control primarily relies on a single drug that kills adult worms. The newly transformed schistosomulum stage is susceptible to the immune response and is a target for vaccine development and rational drug design. (1,600-fold up-regulation), a protein kinase, a novel serine protease and serine protease inhibitor, and intestinal proteases belonging to distinct mechanistic classes. The inclusion of erythrocytes in the culture medium resulted in a general but less pronounced increase in transcriptional activity, with the highest up-regulation of genes involved in iron metabolism, proteolysis, and transport of fatty acids and sugars.. Using a combination of gene silencing techniques and murine protection studies, some of these highly up-regulated transcripts can be targeted for future development of new vaccines and drugs

Gobert Geoffrey N.

Tran Mai H.

Moertel Luke

Mulvenna Jason

Jones Malcolm K.

McManus Donald P.

Loukas Alex

Public Library of Science (PLOS)

 during Early Schistosomula Development and in the Presence of Erythrocytes

Background: Schistosomes cause more mortality and morbidity than any other human helminth, but control primarily relies on a single drug that kills adult worms. The newly transformed schistosomulum stage is susceptible to the immune response and is a target for vaccine development and rational drug design

University of Queensland eSpace

Acquisition of human antigens by Schistosoma mansoni during cultivation in vitro.

Acquisition of human blood group antigens by Schistosoma mansoni.

Acquisition of murine major histocompatibility complex gene products by schistosomula of Schistosoma mansoni.JE x pM e d 148:

An immunogenic Mr 23,000 integral membrane protein of Schistosoma mansoni worms that closely resembles a human tumor-associated antigen.

Antigenicity and immunogenicity of the tegumental outer membrane of adult Schistosoma mansoni.

Antigens derived from lung-stage larvae of Schistosoma mansoni are efficient stimulators of proliferation and gamma interferon secretion by lymphocytes from mice vaccinated with attenuated larvae.

Blood ‘n’ guts: an update on schistosome digestive peptidases.

Cercarial elastase is encoded by a functionally conserved gene family across multiple species of schistosomes.

Changes in the surface antigen profile of Schistosoma mansoni during maturation from cercaria to adult worm.

Cloning of the proteinase that facilitates infection by schistosome parasites.

Cloning, characterization, and functional expression of cDNAs encoding glucose transporter proteins from the human parasite Schistosoma mansoni.

Cultivation of Schistosoma mansoni in vitro. I. Establishment of cultures from cercariae and development until pairing.

Developmental gene expression profiles of the human pathogen Schistosoma japonicum.

Evidence for adsorption of heterospecific host immunoglobulin on the tegument of Schistosoma mansoni.

Gene expression patterns during adaptation of a helminth parasite to different environmental niches.

Gene expression profiling for molecular staging and prognosis prediction in colorectal cancer.

Glycomics analysis of Schistosoma mansoni egg and cercarial secretions.

Human IgE response to the Schistosoma haematobium 22.6 kDa antigen.

Immune effector mechanisms against schistosomiasis: looking for a chink in the parasite’s armour.

Immunization with Schistosoma mansoni 22.6 kDa antigen induces partial protection against experimental infection in a recombinant protein form but not as DNA vaccine.

Immunolocalization of the fatty acid-binding protein Sj-FABPc within adult Schistosoma japonicum.

Locating proteins in the cell using TargetP, SignalP and related tools.

Long-term suppression of cathepsin B levels by RNA interference retards schistosome growth.

Loukas A

Manipulating the manipulators: advances in parasitic helminth transgenesis and RNAi.

Microarray analysis identifies genes preferentially expressed in the lung schistosomulum of Schistosoma mansoni.

Microarray based analysis of temperature and oxidative stress induced messenger RNA in Schistosoma mansoni.

Microarray validation: factors influencing correlation between oligonucleotide microarrays and real-time PCR.

Molecular cloning and identification of a novel Clonorchis sinensis gene encoding a tegumental protein.

Natural versus drug-induced resistance in Schistosoma mansoni infection.

Oleaga A

Oligonucleotide microarray analysis of strain- and gender-associated gene expression in the human blood fluke, Schistosoma japonicum.

Performance comparison of one-color and two-color platforms within the Microarray Quality Control (MAQC) project.

Praziquantel: mechanisms of action, resistance and new derivatives for schistosomiasis.

Proteins exposed at the adult schistosome surface revealed by biotinylation.

Proteomic analysis of the schistosome tegument and its surface membranes.

Purification and characterization of an elastinolytic proteinase secreted by cercariae of Schistosoma mansoni.

Receptor for Fc on the surfaces of schistosomes.

Release of leukotriene C4 (LTC4) from human eosinophils following adherence to IgE- and IgG-coated schistosomula of Schistosoma mansoni.

RNA interference of Schistosoma mansoni cathepsin D, the apical enzyme of the hemoglobin proteolysis cascade.

Schistosoma mansoni ex vivo lung-stage larvae excretory-secretory antigens as vaccine candidates against schistosomiasis.

Schistosoma mansoni: activation of hemolytic activity in homogenates from live adult worms.

Schistosome membrane proteins as vaccines.

Schistosomes–proteomics studies for potential novel vaccines and drug targets.

Sm22.6 antigen is an inhibitor to human thrombin.

Species-related innate resistance to Schistosoma mansoni. Role of mononuclear phagocytes in schistosomula killing in vitro.

Structural and phylogenetic analyses of RGD-CAP/beta ig-h3, a fasciclin-like adhesion protein expressed in chick chondrocytes.

Tegumental expression of a novel type II receptor serine/threonine kinase (SmRK2) in Schistosoma mansoni.

Tetraspanins on the surface of Schistosoma mansoni are protective vaccine antigens in mice and Sm-TSP-2 is selectively recognized by naturally resistant individuals.

The cytoskeleton and motor proteins of human schistosomes and their roles in surface maintenance and host-parasite interactions.

The genome of the blood fluke Schistosoma mansoni.

The immunobiology of schistosomiasis.

The modulation of expression of polypeptide surface antigens on developing schistosomula of Schistosoma mansoni.

The radiation-attenuated vaccine against schistosomes in animal models: paradigm for a human vaccine?

The Role of Microscopy in the Investigation of Paramyosin as a Vaccine Candidate against Schistosoma japonicum.

The Schistosoma japonicum genome reveals features of host-parasite interplay.

The ultrastructural architecture of the adult Schistosoma japonicum tegument.

Tissue Specific Profiling of Females of Schistosoma japonicum by Integrated Laser Microdissection Microscopy and Microarray Analysis.

Transcriptional profiles of adult male and female Schistosoma japonicum in response to insulin reveal increased expression of genes involved in growth and development.

Transcriptome analysis of the acoelomate human parasite Schistosoma mansoni.

Transformation of cercariae to schistosomula: a quantitative comparison of transformation techniques and of infectivity by different injection routes of the organisms produced.

Vaccination against Schistosomiasis: The case for Lung-stage Antigens.

http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=2817720

Transcriptional Changes in Schistosoma mansoni during Early Schistosomula Development and in the Presence of Erythrocytes

Transcriptional Changes in Schistosoma mansoni during Early Schistosomula Development and in the Presence of Erythrocytes

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