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they have no competing interests. Authors’ contributions CP carried AZD8055 cell line out the experimental studies and drafted the manuscript. MJ conducted the redox potential measurements and the gel staining experiments, RGS and FS conceived and coordinated the study and drafted the manuscript. All authors read and approved the final manuscript.”
“Background Vector-borne helminthic diseases, such as onchocerciasis and lymphatic filariasis, are major human diseases in endemic areas. Novel treatment approaches have been recently
focusing on the interaction between the causative helminth agent and its bacterial symbiont. Consequently, antibiotics, such as doxycycline, are used instead of, or with, anti-helminthic drugs for treatment [1, 2]. However, because of difficulties in application, various bacterial targets are constantly studied [3]. This approach has also been adopted in veterinary helminthic diseases, such as bovine onchocerciasis and canine heartworm disease [4–6]. Spirocercosis is a vector-borne helminthic disease, mostly Cytidine deaminase affecting carnivores, especially canids [7, 8]. It is caused by the esophageal nematode Spirocerca lupi (Spirurida: Thelaziidae) that has a wide distribution, but is mostly prevalent in warm, humid areas. The exact annual number of dogs affected annually worldwide has never been assessed. However, the disease has a wide distribution in the Mediterranean basin, Africa, Central and South America [9]. The definitive canid host of S. lupi is infected by ingesting an obligate intermediate coprophagous beetle vector, or a variety of paratenic hosts including birds, reptiles, amphibians and small mammals [10] that are infected by S.