Abstract

Functional studies will facilitate characterization of role and essentiality of newly available genome sequences of the human schistosomes, Schistosoma mansoni, S. japonicum and S. haematobium. To develop transgenesis as a functional approach for these pathogens, we previously demonstrated that pseudotyped murine leukemia virus (MLV) can transduce schistosomes leading to chromosomal integration of reporter transgenes and short hairpin RNA cassettes. Here we investigated vertical transmission of transgenes through the developmental cycle of S. mansoni after introducing transgenes into eggs. Although MLV infection of schistosome eggs from mouse livers was efficient in terms of snail infectivity, >10-fold higher transgene copy numbers were detected in cercariae derived from in vitro laid eggs (IVLE). After infecting snails with miracidia from eggs transduced by MLV, sequencing of genomic DNA from cercariae released from the snails also revealed the presence of transgenes, demonstrating that transgenes had been transmitted through the asexual developmental cycle, and thereby confirming germline transgenesis. High-throughput sequencing of genomic DNA from schistosome populations exposed to MLV mapped widespread and random insertion of transgenes throughout the genome, along each of the autosomes and sex chromosomes, validating the utility of this approach for insertional mutagenesis. In addition, the germline-transmitted transgene encoding neomycin phosphotransferase rescued cultured schistosomules from toxicity of the antibiotic G418, and PCR analysis of eggs resulting from sexual reproduction of the transgenic worms in mice confirmed that retroviral transgenes were transmitted to the next (F1) generation. These findings provide the first description of wide-scale, random insertional mutagenesis of chromosomes and of germline transmission of a transgene in schistosomes. Transgenic lines of schistosomes expressing antibiotic resistance could advance functional genomics for these significant human pathogens. Database accessionSequence data from this study have been submitted to the European Nucleotide Archive (http://www.ebi.ac.uk/embl) under accession number ERP000379.

Highlights

  • The schistosomes are considered the most important helminth pathogens in terms of human morbidity and mortality

  • Schistosomes, or blood flukes, are responsible for the major neglected tropical disease called schistosomiasis, which afflicts over 200 million people in impoverished regions of the developing world

  • Transgene integrations were mapped to the genome sequence of Schistosoma mansoni

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Summary

Introduction

The schistosomes are considered the most important helminth pathogens in terms of human morbidity and mortality. More than 200 million people are infected and a further 800 million at risk of schistosomiasis in tropical and sub-tropical latitudes. Treatment and control of schistosomiasis rely on the anthelmintic drug praziquantel; there is concern that drug resistance will develop. New therapeutic approaches including vaccines, drugs and diagnostics are needed for this neglected tropical disease [1,2,3,4,5,6]. Through a complex two-host life cycle, schistosomes are transmitted from freshwater snails to humans. Adult schistosomes dwell as pairs in the blood vessels of the intestines and/or urinary bladder, where female worms release eggs that become embedded in the intestinal wall and other organs to elicit chronic immunemediated disease and other serious complications [7]

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