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Individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function

BACKGROUND: In Mali, cutaneous leishmaniasis (CL) and filariasis are co-endemic. Previous studies in animal models of infection have shown that sand fly saliva enhance infectivity of Leishmania parasites in naïve hosts while saliva-specific adaptive immune responses may protect against cutaneous and...

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Autores principales: Sangare, Moussa, Coulibaly, Yaya Ibrahim, Huda, Naureen, Vidal, Silvia, Tariq, Sameha, Coulibaly, Michel Emmanuel, Coulibaly, Siaka Yamoussa, Soumaoro, Lamine, Dicko, Ilo, Traore, Bourama, Sissoko, Ibrahim Moussa, Traore, Sekou Fantamady, Faye, Ousmane, Nutman, Thomas B., Valenzuela, Jesus G., Oliveira, Fabiano, Doumbia, Seydou, Kamhawi, Shaden, Semnani, Roshanak Tolouei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8189443/
https://www.ncbi.nlm.nih.gov/pubmed/34106920
http://dx.doi.org/10.1371/journal.pntd.0009448
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author Sangare, Moussa
Coulibaly, Yaya Ibrahim
Huda, Naureen
Vidal, Silvia
Tariq, Sameha
Coulibaly, Michel Emmanuel
Coulibaly, Siaka Yamoussa
Soumaoro, Lamine
Dicko, Ilo
Traore, Bourama
Sissoko, Ibrahim Moussa
Traore, Sekou Fantamady
Faye, Ousmane
Nutman, Thomas B.
Valenzuela, Jesus G.
Oliveira, Fabiano
Doumbia, Seydou
Kamhawi, Shaden
Semnani, Roshanak Tolouei
author_facet Sangare, Moussa
Coulibaly, Yaya Ibrahim
Huda, Naureen
Vidal, Silvia
Tariq, Sameha
Coulibaly, Michel Emmanuel
Coulibaly, Siaka Yamoussa
Soumaoro, Lamine
Dicko, Ilo
Traore, Bourama
Sissoko, Ibrahim Moussa
Traore, Sekou Fantamady
Faye, Ousmane
Nutman, Thomas B.
Valenzuela, Jesus G.
Oliveira, Fabiano
Doumbia, Seydou
Kamhawi, Shaden
Semnani, Roshanak Tolouei
author_sort Sangare, Moussa
collection PubMed
description BACKGROUND: In Mali, cutaneous leishmaniasis (CL) and filariasis are co-endemic. Previous studies in animal models of infection have shown that sand fly saliva enhance infectivity of Leishmania parasites in naïve hosts while saliva-specific adaptive immune responses may protect against cutaneous and visceral leishmaniasis. In contrast, the human immune response to Phlebotomus duboscqi (Pd) saliva, the principal sand fly vector in Mali, was found to be dichotomously polarized with some individuals having a Th1-dominated response and others having a Th2-biased response. We hypothesized that co-infection with filarial parasites may be an underlying factor that modulates the immune response to Pd saliva in endemic regions. METHODOLOGY/PRINCIPAL FINDINGS: To understand which cell types may be responsible for polarizing human responses to sand fly saliva, we investigated the effect of salivary glands (SG) of Pd on human monocytes. To this end, elutriated monocytes were cultured in vitro, alone, or with SG, microfilariae antigen (MF ag) of Brugia malayi, or LPS, a positive control. The mRNA expression of genes involved in inflammatory or regulatory responses was then measured as were cytokines and chemokines associated with these responses. Monocytes of individuals who were not exposed to sand fly bites (mainly North American controls) significantly upregulated the production of IL-6 and CCL4; cytokines that enhance leishmania parasite establishment, in response to SG from Pd or other vector species. This selective inflammatory response was lost in individuals that were exposed to sand fly bites which was not changed by co-infection with filarial parasites. Furthermore, infection with filarial parasites resulted in upregulation of CCL22, a type-2 associated chemokine, both at the mRNA levels and by its observed effect on the frequency of recruited monocytes. CONCLUSIONS/SIGNIFICANCE: Together, our data suggest that SG or recombinant salivary proteins from Pd alter human monocyte function by upregulating selective inflammatory cytokines.
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spelling pubmed-81894432021-06-16 Individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function Sangare, Moussa Coulibaly, Yaya Ibrahim Huda, Naureen Vidal, Silvia Tariq, Sameha Coulibaly, Michel Emmanuel Coulibaly, Siaka Yamoussa Soumaoro, Lamine Dicko, Ilo Traore, Bourama Sissoko, Ibrahim Moussa Traore, Sekou Fantamady Faye, Ousmane Nutman, Thomas B. Valenzuela, Jesus G. Oliveira, Fabiano Doumbia, Seydou Kamhawi, Shaden Semnani, Roshanak Tolouei PLoS Negl Trop Dis Research Article BACKGROUND: In Mali, cutaneous leishmaniasis (CL) and filariasis are co-endemic. Previous studies in animal models of infection have shown that sand fly saliva enhance infectivity of Leishmania parasites in naïve hosts while saliva-specific adaptive immune responses may protect against cutaneous and visceral leishmaniasis. In contrast, the human immune response to Phlebotomus duboscqi (Pd) saliva, the principal sand fly vector in Mali, was found to be dichotomously polarized with some individuals having a Th1-dominated response and others having a Th2-biased response. We hypothesized that co-infection with filarial parasites may be an underlying factor that modulates the immune response to Pd saliva in endemic regions. METHODOLOGY/PRINCIPAL FINDINGS: To understand which cell types may be responsible for polarizing human responses to sand fly saliva, we investigated the effect of salivary glands (SG) of Pd on human monocytes. To this end, elutriated monocytes were cultured in vitro, alone, or with SG, microfilariae antigen (MF ag) of Brugia malayi, or LPS, a positive control. The mRNA expression of genes involved in inflammatory or regulatory responses was then measured as were cytokines and chemokines associated with these responses. Monocytes of individuals who were not exposed to sand fly bites (mainly North American controls) significantly upregulated the production of IL-6 and CCL4; cytokines that enhance leishmania parasite establishment, in response to SG from Pd or other vector species. This selective inflammatory response was lost in individuals that were exposed to sand fly bites which was not changed by co-infection with filarial parasites. Furthermore, infection with filarial parasites resulted in upregulation of CCL22, a type-2 associated chemokine, both at the mRNA levels and by its observed effect on the frequency of recruited monocytes. CONCLUSIONS/SIGNIFICANCE: Together, our data suggest that SG or recombinant salivary proteins from Pd alter human monocyte function by upregulating selective inflammatory cytokines. Public Library of Science 2021-06-09 /pmc/articles/PMC8189443/ /pubmed/34106920 http://dx.doi.org/10.1371/journal.pntd.0009448 Text en https://creativecommons.org/publicdomain/zero/1.0/This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Sangare, Moussa
Coulibaly, Yaya Ibrahim
Huda, Naureen
Vidal, Silvia
Tariq, Sameha
Coulibaly, Michel Emmanuel
Coulibaly, Siaka Yamoussa
Soumaoro, Lamine
Dicko, Ilo
Traore, Bourama
Sissoko, Ibrahim Moussa
Traore, Sekou Fantamady
Faye, Ousmane
Nutman, Thomas B.
Valenzuela, Jesus G.
Oliveira, Fabiano
Doumbia, Seydou
Kamhawi, Shaden
Semnani, Roshanak Tolouei
Individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function
title Individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function
title_full Individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function
title_fullStr Individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function
title_full_unstemmed Individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function
title_short Individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function
title_sort individuals co-exposed to sand fly saliva and filarial parasites exhibit altered monocyte function
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8189443/
https://www.ncbi.nlm.nih.gov/pubmed/34106920
http://dx.doi.org/10.1371/journal.pntd.0009448
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