Dirofilariasis mouse models for heartworm preclinical research

INTRODUCTION: Dirofilariasis, including heartworm disease, is a major emergent veterinary parasitic infection and a human zoonosis. Currently, experimental infections of cats and dogs are used in veterinary heartworm preclinical drug research. METHODS: As a refined alternative in vivo heartworm prev...

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Autores principales: Marriott, A. E., Dagley, J. L., Hegde, S., Steven, A., Fricks, C., DiCosty, U., Mansour, A., Campbell, E. J., Wilson, C. M., Gusovsky, F., Ward, S. A., Hong, W. D., O'Neill, P., Moorhead, A., McCall, S., McCall, J. W., Taylor, M. J., Turner, J. D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10324412/
https://www.ncbi.nlm.nih.gov/pubmed/37426014
http://dx.doi.org/10.3389/fmicb.2023.1208301
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author Marriott, A. E.
Dagley, J. L.
Hegde, S.
Steven, A.
Fricks, C.
DiCosty, U.
Mansour, A.
Campbell, E. J.
Wilson, C. M.
Gusovsky, F.
Ward, S. A.
Hong, W. D.
O'Neill, P.
Moorhead, A.
McCall, S.
McCall, J. W.
Taylor, M. J.
Turner, J. D.
author_facet Marriott, A. E.
Dagley, J. L.
Hegde, S.
Steven, A.
Fricks, C.
DiCosty, U.
Mansour, A.
Campbell, E. J.
Wilson, C. M.
Gusovsky, F.
Ward, S. A.
Hong, W. D.
O'Neill, P.
Moorhead, A.
McCall, S.
McCall, J. W.
Taylor, M. J.
Turner, J. D.
author_sort Marriott, A. E.
collection PubMed
description INTRODUCTION: Dirofilariasis, including heartworm disease, is a major emergent veterinary parasitic infection and a human zoonosis. Currently, experimental infections of cats and dogs are used in veterinary heartworm preclinical drug research. METHODS: As a refined alternative in vivo heartworm preventative drug screen, we assessed lymphopenic mouse strains with ablation of the interleukin-2/7 common gamma chain (γc) as susceptible to the larval development phase of Dirofilaria immitis. RESULTS: Non-obese diabetic (NOD) severe combined immunodeficiency (SCID)γc(−/−) (NSG and NXG) and recombination-activating gene (RAG)2(−/−)γc(−/−) mouse strains yielded viable D. immitis larvae at 2–4 weeks post-infection, including the use of different batches of D. immitis infectious larvae, different D. immitis isolates, and at different laboratories. Mice did not display any clinical signs associated with infection for up to 4 weeks. Developing larvae were found in subcutaneous and muscle fascia tissues, which is the natural site of this stage of heartworm in dogs. Compared with in vitro-propagated larvae at day 14, in vivo-derived larvae had completed the L4 molt, were significantly larger, and contained expanded Wolbachia endobacteria titres. We established an ex vivo L4 paralytic screening system whereby assays with moxidectin or levamisole highlighted discrepancies in relative drug sensitivities in comparison with in vitro-reared L4 D. immitis. We demonstrated effective depletion of Wolbachia by 70%−90% in D. immitis L4 following 2- to 7-day oral in vivo exposures of NSG- or NXG-infected mice with doxycycline or the rapid-acting investigational drug, AWZ1066S. We validated NSG and NXG D. immitis mouse models as a filaricide screen by in vivo treatments with single injections of moxidectin, which mediated a 60%−88% reduction in L4 larvae at 14–28 days. DISCUSSION: Future adoption of these mouse models will benefit end-user laboratories conducting research and development of novel heartworm preventatives via increased access, rapid turnaround, and reduced costs and may simultaneously decrease the need for experimental cat or dog use.
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spelling pubmed-103244122023-07-07 Dirofilariasis mouse models for heartworm preclinical research Marriott, A. E. Dagley, J. L. Hegde, S. Steven, A. Fricks, C. DiCosty, U. Mansour, A. Campbell, E. J. Wilson, C. M. Gusovsky, F. Ward, S. A. Hong, W. D. O'Neill, P. Moorhead, A. McCall, S. McCall, J. W. Taylor, M. J. Turner, J. D. Front Microbiol Microbiology INTRODUCTION: Dirofilariasis, including heartworm disease, is a major emergent veterinary parasitic infection and a human zoonosis. Currently, experimental infections of cats and dogs are used in veterinary heartworm preclinical drug research. METHODS: As a refined alternative in vivo heartworm preventative drug screen, we assessed lymphopenic mouse strains with ablation of the interleukin-2/7 common gamma chain (γc) as susceptible to the larval development phase of Dirofilaria immitis. RESULTS: Non-obese diabetic (NOD) severe combined immunodeficiency (SCID)γc(−/−) (NSG and NXG) and recombination-activating gene (RAG)2(−/−)γc(−/−) mouse strains yielded viable D. immitis larvae at 2–4 weeks post-infection, including the use of different batches of D. immitis infectious larvae, different D. immitis isolates, and at different laboratories. Mice did not display any clinical signs associated with infection for up to 4 weeks. Developing larvae were found in subcutaneous and muscle fascia tissues, which is the natural site of this stage of heartworm in dogs. Compared with in vitro-propagated larvae at day 14, in vivo-derived larvae had completed the L4 molt, were significantly larger, and contained expanded Wolbachia endobacteria titres. We established an ex vivo L4 paralytic screening system whereby assays with moxidectin or levamisole highlighted discrepancies in relative drug sensitivities in comparison with in vitro-reared L4 D. immitis. We demonstrated effective depletion of Wolbachia by 70%−90% in D. immitis L4 following 2- to 7-day oral in vivo exposures of NSG- or NXG-infected mice with doxycycline or the rapid-acting investigational drug, AWZ1066S. We validated NSG and NXG D. immitis mouse models as a filaricide screen by in vivo treatments with single injections of moxidectin, which mediated a 60%−88% reduction in L4 larvae at 14–28 days. DISCUSSION: Future adoption of these mouse models will benefit end-user laboratories conducting research and development of novel heartworm preventatives via increased access, rapid turnaround, and reduced costs and may simultaneously decrease the need for experimental cat or dog use. Frontiers Media S.A. 2023-06-22 /pmc/articles/PMC10324412/ /pubmed/37426014 http://dx.doi.org/10.3389/fmicb.2023.1208301 Text en Copyright © 2023 Marriott, Dagley, Hegde, Steven, Fricks, DiCosty, Mansour, Campbell, Wilson, Gusovsky, Ward, Hong, O'Neill, Moorhead, McCall, McCall, Taylor and Turner. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Microbiology
Marriott, A. E.
Dagley, J. L.
Hegde, S.
Steven, A.
Fricks, C.
DiCosty, U.
Mansour, A.
Campbell, E. J.
Wilson, C. M.
Gusovsky, F.
Ward, S. A.
Hong, W. D.
O'Neill, P.
Moorhead, A.
McCall, S.
McCall, J. W.
Taylor, M. J.
Turner, J. D.
Dirofilariasis mouse models for heartworm preclinical research
title Dirofilariasis mouse models for heartworm preclinical research
title_full Dirofilariasis mouse models for heartworm preclinical research
title_fullStr Dirofilariasis mouse models for heartworm preclinical research
title_full_unstemmed Dirofilariasis mouse models for heartworm preclinical research
title_short Dirofilariasis mouse models for heartworm preclinical research
title_sort dirofilariasis mouse models for heartworm preclinical research
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10324412/
https://www.ncbi.nlm.nih.gov/pubmed/37426014
http://dx.doi.org/10.3389/fmicb.2023.1208301
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