Abstract
Vitamin D (VitD) deficiency has been shown to be a risk factor for a plethora of disorders. We have shown that dogs with clinical leishmaniasis presented lower VitD serum levels than non-infected dogs, and even lower than those with asymptomatic infection. However, if VitD deficiency is a risk factor to develop clinical leishmaniasis remains to be answered. It is also unknown if VitD participates in Leishmania control. First, we retrospectively analysed VitD concentration in serum samples from 36 healthy dogs collected in different periods of the year concluding that there isn’t a seasonal variation of this vitamin in dogs. We also included 9 dogs with clinical leishmaniasis and 10 non-infected healthy dogs, in which we measured VitD levels at the beginning of the study, when all dogs were negative for serology and qPCR, and 1 year later. Whereas non-infected dogs showed no change in VitD levels along the study, those developing clinical leishmaniasis showed a significant VitD reduction at the end of the study (35%). When we compared VitD concentration between the two groups at the beginning of the study, no differences were detected (43.6 (38–59) ng/mL, P = 0.962). Furthermore, an in vitro model using a canine macrophage cell line proved that adding active VitD leads to a significant reduction in L. infantum load (31.4%). Analyzing expression of genes related to VitD pathway on primary canine monocytes, we showed that CBD103 expression was significantly enhanced after 1,25(OH)2D addition. Our results show that VitD concentration is neither seasonal nor a risk factor for developing canine leishmaniasis, but it diminishes with the onset of clinical disease suggesting a role in parasitic control. Our in vitro results corroborate this hypothesis and point out that VitD regulates infection through CBD103 expression. These results open the possibility for studies testing VitD as an adjuvant in leishmaniasis therapy.
Highlights
Leishmaniases are a group of neglected vector-borne diseases caused by obligate intracellular protozoan parasites of the genus Leishmania (Trypanosomatida: Trypanosomatidae)
Immune system plays a key role in leishmaniasis disease control, Vitamin D (VitD) could have a relevant contribution in leishmaniasis
We shown that clinical leishmaniasis is associated with VitD deficiency
Summary
Leishmaniases are a group of neglected vector-borne diseases caused by obligate intracellular protozoan parasites of the genus Leishmania (Trypanosomatida: Trypanosomatidae). Canids are the main reservoir and hosts of L. infantum, the causative agent of zoonotic VL in the Mediterranean Basin [1]. Most Leishmania-infected humans and dogs show an asymptomatic infection, with only 5–20% of the cases developing the patent disease over a variable period of time [3,4]. The mechanisms that regulate the final outcome of the infection remain unknown, it appears that asymptomatic infections are associated with a strong specific cell-mediated immunity and a Th1-proinflamatory immune response [5]. Susceptible individuals develop progressive disease with increasing parasite burden, concomitant to high antibody levels and a progressive Th2-deactivating immune response in the presence of a strong inflammatory reaction [9,10]. Macrophages are central players in innate immune response and the main host cell for Leishmania spp
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