Co-Treatment with Human Leukocyte Extract and Albendazole Stimulates Drug’s Efficacy and Th1 Biased Immune Response in <i>Mesocestoides vogae</i> (Cestoda) Infection via Modulation of Transcription Factors, Macrophage Polarization, and Cytokine Profiles

Gabriela Hrčková; Terézia Mačak Kubašková; Dagmar Mudroňová; Zuzana Jurčacková; Denisa Ciglanová

doi:10.3390/pharmaceutics15020541

Pharmaceutics (Feb 2023)

Co-Treatment with Human Leukocyte Extract and Albendazole Stimulates Drug’s Efficacy and Th1 Biased Immune Response in <i>Mesocestoides vogae</i> (Cestoda) Infection via Modulation of Transcription Factors, Macrophage Polarization, and Cytokine Profiles

Gabriela Hrčková,
Terézia Mačak Kubašková,
Dagmar Mudroňová,
Zuzana Jurčacková,
Denisa Ciglanová

Affiliations

Gabriela Hrčková: Institute of Parasitology, The Slovak Academy of Sciences, Hlinkova 3, 040 01 Košice, Slovakia
Terézia Mačak Kubašková: Institute of Parasitology, The Slovak Academy of Sciences, Hlinkova 3, 040 01 Košice, Slovakia
Dagmar Mudroňová: Department of Microbiology and Immunology, University of Veterinary Medicine and Pharmacy, Komenského 68/73, 041 81 Košice, Slovakia
Zuzana Jurčacková: Institute of Parasitology, The Slovak Academy of Sciences, Hlinkova 3, 040 01 Košice, Slovakia
Denisa Ciglanová: Institute of Parasitology, The Slovak Academy of Sciences, Hlinkova 3, 040 01 Košice, Slovakia

DOI: https://doi.org/10.3390/pharmaceutics15020541
Journal volume & issue: Vol. 15, no. 2
p. 541

Abstract

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The model flatworm Mesocestoides vogae proliferating stage of infection elicits immunosuppression in the host. It was used to investigate the effects of human leukocyte extract (DLE) alone and in combination with anthelmintic albendazole (ABZ) on the reduction in peritoneal infection, peritoneal exudate cells (PECs), their adherent counterparts, and peritoneal exudates after the termination of therapy. Balb/c mice were infected with the larvae of M. vogae. PECs and adherent macrophages were studied via flow cytometry, mRNA transcript levels, and immunofluorescence. The cytokine levels were measured via ELISA and larvae were counted. ABZ significantly reduced larval counts (581.2 ± 65, p p mid/highMHCIIhigh macrophages/monocytes (22.2 ± 5.4%). Transcripts of the M2 macrophage markers (arginase 1, FIZZ-1, and Ym-1) were downregulated after DLE and combined therapy but not after ABZ, and the opposite trend was seen for iNOS. This contrasts with reduced ex vivo NO production by LPS-stimulated PECs from DLE and ABZ+DLE groups, where adherent macrophages/monocytes had elevated transcripts of the INF-γ receptor and STAT1 and reduced expression of STAT3, STAT6, and IL-10. Each therapy differentially modulated transcription profiles and concentrations of IFN-γ, TNF-α, IL-12p40, IL-6, IL-10, and TGF-β cytokines. DLE strongly ameliorated ABZ-induced suppression of INF-γ and IL-12 and preserved downregulation for IL-4, IL-10, and TGF-β. Epigenetic study on adherent macrophages from infected mice showed that ABZ, ABZ-sulfoxide, and DLE could interact with the mRNA of examined markers in a dose-dependent pattern. Co-administration of DLE with ABZ seemed to augment the drug’s larvicidal effect via modulation of immunity. In comparison with ABZ, combined therapy was the most effective in alleviating parasite-induced Th2/Treg/STAT3/STA6 directed immunosuppression by stimulating the Th1 cytokines, M1 macrophage polarization, and activation of the IFNγ/STAT1 signaling pathway.

Published in Pharmaceutics

ISSN: 1999-4923 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Pharmacy and materia medica
Website: http://www.mdpi.com/journal/pharmaceutics/

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