Molecular Cloning and Characterization of Novel Glutamate-Gated Chloride Channel Subunits from Schistosoma mansoni

Dufour, Vanessa; Beech, Robin N.; Wever, Claudia M.; Dent, Joseph A.; Geary, Timothy G.

doi:10.1371/journal.ppat.1003586

Cited by 33 publications

(55 citation statements)

References 98 publications

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“…Invertebrate genomes, in contrast, encode a greater assortment of channel types with a wider range of ligand specificities and ligand-ion combinations than those found in vertebrates (Dent, 2006). In addition to the nicotinic acetylcholine and GABA receptors found in vertebrates, invertebrate genomes encode anion-selective acetylcholine (Putrenko et al, 2005;van Nierop et al, 2005), histamine (Gengs et al, 2002;Zheng et al, 2002), glutamate (Dent et al, 1997;Dufour et al, 2013;Kehoe et al, 2009), serotonin (Ranganathan et al, 2000), dopamine (Ringstad et al, 2009), tyramine (Ringstad et al, 2009) and pH (Mounsey et al, 2007;Schnizler et al, 2005) channels, as well as cation-selective GABA (Gisselmann et al, 2004) and proton (Beg et al, 2008) channels. Moreover, multiple putative invertebrate pLGICs have been identified that cannot be assigned to any neurotransmitter family based on sequence homology.…”

Section: Introductionmentioning

confidence: 99%

The orphan pentameric ligand-gated ion channelpHCl-2is gated by pH and regulates fluid secretion inDrosophilaMalpighian tubules

Feingold

Starc

O’Donnell

et al. 2016

Journal of Experimental Biology

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Pentameric ligand-gated ion channels ( pLGICs) constitute a large protein superfamily in metazoa whose role as neurotransmitter receptors mediating rapid, ionotropic synaptic transmission has been extensively studied. Although the vast majority of pLGICs appear to be neurotransmitter receptors, the identification of pLGICs in non-neuronal tissues and homologous pLGIC-like proteins in prokaryotes points to biological functions, possibly ancestral, that are independent of neuronal signalling. Here, we report the molecular and physiological characterization of a highly divergent, orphan pLGIC subunit encoded by the pHCl-2 (CG11340) gene, in Drosophila melanogaster. We show that pHCl-2 forms a channel that is insensitive to a wide array of neurotransmitters, but is instead gated by changes in extracellular pH. pHCl-2 is expressed in the Malpighian tubules, which are non-innervated renal-type secretory tissues. We demonstrate that pHCl-2 is localized to the apical membrane of the epithelial principal cells of the tubules and that loss of pHCl-2 reduces urine production during diuresis. Our data implicate pHCl-2 as an important source of chloride conductance required for proper urine production, highlighting a novel role for pLGICs in epithelial tissues regulating fluid secretion and osmotic homeostasis.

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Section: Introductionmentioning

confidence: 99%

The orphan pentameric ligand-gated ion channelpHCl-2is gated by pH and regulates fluid secretion inDrosophilaMalpighian tubules

Feingold

Starc

O’Donnell

et al. 2016

Journal of Experimental Biology

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“…These compounds were: the antimalarial drug mefloquine (MFQ) [27]; the antihelmintic Ivermectin (IVM) [28, 29]; the bromodomain inhibitor JQ1 [30]; and the reference drug praziquantel (PZQ). The positive and negative controls average absorbance values were used to calculate parasites viability.…”

Section: Resultsmentioning

confidence: 99%

A high-throughput colorimetric assay for detection of Schistosoma mansoni viability based on the tetrazolium salt XTT

et al. 2017

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Background Schistosoma mansoni is a trematode parasite that causes schistosomiasis, one of the most prevalent neglected tropical diseases, leading to the loss of 2.6 million disability-adjusted life years. Praziquantel is the only drug available, and new drugs are required. The most common strategy in schistosomiasis drug discovery is the use of the schistosomula larval-stage for a pre-screen in drug sensitivity assays. However, assessing schistosomula viability by microscopy has always been a limitation to the throughput of such assays. Hence, the development of validated, robust high-throughput in vitro assays for Schistosoma with simple readouts is needed. Here, we present a simple and affordable alternative to assess schistosomula viability. The method employed is based on the hydrosoluble tetrazolium salt XTT which has been widely used in other organisms but has never been used to drug screen in schistosomes.ResultsWe showed that schistosomula reduce XTT salt to a coloured formazan product and that absorbance levels reflected the viability and parasites number. This XTT viability assay was validated for high throughput screening of compounds in schistosomula, and dose-response curves of compounds could be reproduced.ConclusionsWe conclude that the XTT viability assay could be applied for the screening of large compounds collections in S. mansoni and accelerate the identification of novel antischistosomal compounds.

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“…Schistosomes and other platyhelminths are typically not sensitive to macrocyclic lactones [53, 54] (though see [55]), which could suggest an absence of GluCl channels in these organisms. However, exciting recent work [56] has demonstrated that schistosomes in fact do express GluCl channel subunits, but that these subunits are phylogenetically distinct from those of other invertebrates, including nematodes, arthropods, and molluscs. When expressed in Xenopus oocytes, schistosome GluCl subunits form functional L-glutamate-gated, Cl − -permeable channels.…”

Section: Glutamate-gated Chloride Channelsmentioning

confidence: 99%

“…Macrocyclic lactones also appear to interact with nematode GABA-gated channels [57], and there is some evidence that the cyclooctadepsipeptide PF1022A (see below) binds to and interacts with nematode GABA receptors [59], though electrophysiological experiments suggest that it does not act as a GABA agonist [60]. Surprisingly, schistosomes do not appear to have genes for GABA-gated channels [56]. …”

Section: Gaba-gated Chloride Channelsmentioning

confidence: 99%

Ion Channels and Drug Transporters as Targets for Anthelmintics

Greenberg

2014

Curr Clin Micro Rpt

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Infections with parasitic helminths such as schistosomes and soil-transmitted nematodes are hugely prevalent and responsible for a major portion of the global health and economic burdens associated with neglected tropical diseases. In addition, many of these parasites infect livestock and plants used in agriculture, resulting in further impoverishment. Treatment and control of these pathogens rely on anthelmintic drugs, which are few in number, and against which drug resistance can develop rapidly. The neuromuscular system of the parasite, and in particular, the ion channels and associated receptors underlying excitation and signaling, have proven to be outstanding targets for anthelmintics. This review will survey the different ion channels found in helminths, focusing on their unique characteristics and pharmacological sensitivities. It will also briefly review the literature on helminth multidrug efflux that may modulate parasite susceptibility to anthelmintics and may prove useful targets for new or repurposed agents that can enhance parasite drug susceptibility and perhaps overcome drug resistance.

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Molecular Cloning and Characterization of Novel Glutamate-Gated Chloride Channel Subunits from Schistosoma mansoni

Cited by 33 publications

References 98 publications

The orphan pentameric ligand-gated ion channelpHCl-2is gated by pH and regulates fluid secretion inDrosophilaMalpighian tubules

The orphan pentameric ligand-gated ion channelpHCl-2is gated by pH and regulates fluid secretion inDrosophilaMalpighian tubules

A high-throughput colorimetric assay for detection of Schistosoma mansoni viability based on the tetrazolium salt XTT

Ion Channels and Drug Transporters as Targets for Anthelmintics

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