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Open AccessJournal ArticleDOI

Development of a Natural Model of Cutaneous Leishmaniasis: Powerful Effects of Vector Saliva and Saliva Preexposure on the Long-Term Outcome of Leishmania major Infection in the Mouse Ear Dermis

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TLDR
The studies reveal a dramatic exacerbating effect of SGS on lesion development in the dermal site, and a complete abrogation of this effect in mice preexposed to salivary components, the first to suggest that for individuals at risk of vector-borne infections, history of exposure to vector saliva might influence the outcome of Exposure to transmitted parasites.
Abstract
We have developed a model of cutaneous leishmaniasis due to Leishmania major that seeks to mimic the natural conditions of infection. 1,000 metacyclic promastigotes were coinoculated with a salivary gland sonicate (SGS) obtained from a natural vector, Phlebotomus papatasii, into the ear dermis of naive mice or of mice preexposed to SGS. The studies reveal a dramatic exacerbating effect of SGS on lesion development in the dermal site, and a complete abrogation of this effect in mice preexposed to salivary components. In both BALB/c and C57Bl/6 (B/6) mice, the dermal lesions appeared earlier, were more destructive, and contained greater numbers of parasites after infection in the presence of SGS. Furthermore, coinoculation of SGS converted B/6 mice into a nonhealing phenotype. No effect of SGS was seen in either IL-4- deficient or in SCID mice. Disease exacerbation in both BALB/c and B/6 mice was associated with an early (6 h) increase in the frequency of epidermal cells producing type 2 cytokines. SGS did not elicit type 2 cytokines in the epidermis of mice previously injected with SGS. These mice made antisaliva antibodies that were able to neutralize the ability of SGS to enhance infection and to elicit IL-4 and IL-5 responses in the epidermis. These results are the first to suggest that for individuals at risk of vector-borne infections, history of exposure to vector saliva might influence the outcome of exposure to transmitted parasites.

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Citations
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Journal ArticleDOI

Kinetics of Antibody Response in BALB/c and C57BL/6 Mice Bitten by Phlebotomus papatasi

TL;DR: The concept of using anti-sand fly saliva antibodies as a marker of sand fly exposure in Phlebotomus papatasi–mice model is confirmed and a combination of recombinant salivary proteins is recommended for evaluation of intensity of sandFly exposure in endemic areas and for estimation of risk of Leishmania transmission.
Journal ArticleDOI

DNA plasmid coding for Phlebotomus sergenti salivary protein PsSP9, a member of the SP15 family of proteins, protects against Leishmania tropica.

TL;DR: Results suggest that this family of proteins in Ph. sergenti, Ph. duboscqi and Ph. papatasi may have similar immunogenic and protective properties against different Leishmania species, and may act as an adjuvant to accelerate the cell-mediated immune response to co-administered Leishmaniasis, or cause the activation of infected macrophages to remove parasites more efficiently.
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The importance of CD11b+ dendritic cells in CD4+ T cell activation in vivo: with help from interleukin 1.

TL;DR: A murine model of cutaneous leishmaniasis, using needle inoculation of Leishmania major, represents perhaps the most widely used system to study the contrasting effects of Th1 versus Th2 immunity in disease control.
Journal ArticleDOI

Human cellular immune response to the saliva of Phlebotomus papatasi is mediated by IL-10-producing CD8+ T cells and Th1-polarized CD4+ lymphocytes.

TL;DR: The overall effect of Phlebotomus papatasi saliva was dominated by the activation of IL-10-producing CD8+ cells suggesting a possible detrimental effect of pre-exposure to saliva on human leishmaniasis outcome.
Journal ArticleDOI

The Salivary Adenosine/AMP Content of Phlebotomus argentipes Annandale and Brunetti, the Main Vector of Human Kala-Azar

TL;DR: It is proposed that these salivary nucleotides help the fly to blood feed and may affect Leishmania transmission.
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Journal ArticleDOI

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