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    Evaluation of activity of triclabendazole against Taenia solium metacestode in naturally infected pigs

    2016-07-07 09:02:47AnaVargasCallaLuisGomezPuertaJuanCalcinaOmarGonzalesVieraCesarGavidiaMariaLopezUrbinaHectorGarciaArmandoGonzalezSchoolofVeterinaryMedicineUniversidadNacionalMayordeSanMarcosLimaPeruCysticercosisEliminationProgramandCenter

    Ana Vargas-Calla, Luis A. Gomez-Puerta*, Juan Calcina, Omar Gonzales-Viera, Cesar Gavidia, Maria T. Lopez-Urbina, Hector H. Garcia, Armando E. GonzalezSchool of Veterinary Medicine, Universidad Nacional Mayor de San Marcos, Lima 4, PeruCysticercosis Elimination Program and Center for Global Heath Tumbes, Universidad Peruana Cayetano Heredia, Tumbes, PeruDepartment of Microbiology, School of Sciences, Universidad Peruana Cayetano Heredia, Lima , Peru

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    Evaluation of activity of triclabendazole against Taenia solium metacestode in naturally infected pigs

    Ana Vargas-Calla1, Luis A. Gomez-Puerta1*, Juan Calcina1, Omar Gonzales-Viera1, Cesar Gavidia1, Maria T. Lopez-Urbina1, Hector H. Garcia2,3, Armando E. Gonzalez1
    1School of Veterinary Medicine, Universidad Nacional Mayor de San Marcos, Lima 41, Peru
    2Cysticercosis Elimination Program and Center for Global Heath Tumbes, Universidad Peruana Cayetano Heredia, Tumbes, Peru
    3Department of Microbiology, School of Sciences, Universidad Peruana Cayetano Heredia, Lima 31, Peru

    ABSTRACT

    Objective: To assess the efficacy of triclabendazole (TCBZ) in porcine cysticercosis. Methods: Eighteen naturally infected cysticercotic pigs were divided into 3 groups of 6 individuals each. The first group was treated orally with TCBZ at a single dose of 30 mg/kg of body weight, the second group was treated orally with oxfendazole at a single dose of 30 mg/kg of body weight and the third group received a placebo (control group). All animals were kept under the same management conditions. The pigs were euthanized 17 wk post-treatment and the number of surviving cysts in muscles was assessed and compared between groups. Results: All pigs treated with oxfendazole had only degenerated cysts in their carcasses. In contrast, TCBZ had very little effect against the parasitic cysts. Cysts from pigs in the TCBZ group looked apparently normal after treatment. However, histological evaluation showed a mild to moderate degree of inflammation. Conclusions: TCBZ is not an efficacious drug against Taenia solium cysticercosis in swine using a single dose.

    ARTICLE INFO

    Article history:

    Received 15 October 2015

    Received in revised form 20 November 2015

    Accepted 15 December 2015

    Available online 20 Junuary 2016

    Keywords:

    Taenia solium

    Cysticercosis

    Triclabendazole

    Oxfendazole

    Treatment

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    1. Introduction

    The disease complex, taeniasis/cysticercosis caused by the pork tapeworm Taenia solium (T. solium), is a very important zoonotic disease in developing countries[1,2]. The adult T. solium tapeworm localizes in the small intestine of humans, the definitive host. The eggs of T. solium are eliminated into gravid proglottids with the faeces, and then they are ingested by pigs, the intermediate host. The T. solium metacestode then develops in different organs of the pig, principally muscles[3,4]. However, humans can act as accidental hosts when they ingest eggs in contaminated food[3,5].

    During the last decade, a variety of strategies have been performed for the control of T. solium cysticercosis including animal inspection, massive chemotherapy for T. solium in humans and pigs from endemics areas, health education, and pig vaccination[2,6-9]. For this purpose, many studies have been performed to evaluate the efficacy of different drugs against porcine cysticercosis[10]. Of these drugs, albendazole and oxfendazole (OFZ), members of the benzimidazole drugs, are efficacious for the treatment of the porcine cysticercosis[11]. Albendazole has been used in humans since 1979, and currently it is considered the drug of preference in humans for its availability, low cost and efficacy[5,11]. Albendazole does not seem to be a good option for field interventions due to the requirement for multiple doses[10]. OFZ, used in a single oral dose of 30 mg/kg, is the drug of choice for the treatment of porcine cysticercosis[12]. The widely used triclabendazole (TCBZ), another member of the benzimidazole family, is efficacious against adults and larval stages of a variety of helminthic parasites[13,14]. The aim of this study was to compare the efficacy of a single oral dose of TCBZ or OFZ against T. solium cysticercosis in naturally infected pigs.

    2. Materials and methods

    2.1. Study design and settings

    The study was conducted at the animal facilities of the Laboratory of Veterinary Epidemiology and Economics, School of Veterinary Medicine, National University of San Marcos in Lima, Peru. Pigs were acquired in a cysticercosis-endemic area and transported to the animal facilities in Lima. Pigs were randomized in three similar groups (TCBZ, OFZ, and placebo) using a random numbers table. All pigs were coded and labeled with ear tags.

    2.2. Animals

    Eighteen adult pigs were acquired in Huancayo, a cysticercosisendemic area in the Peruvian highlands[15]. All animals were positive to cysticercosis by tongue examination, and confirmed by antibody detection on serum enzyme-linked immunoelectro transfer blot[16,17]. Only animals with more than one cyst in the tongue and more than four antigen bands in enzyme-linked immunoelectro transfer blot were included in the study. All pigs were vaccinated against hog cholera immediately after purchase.

    2.3. Treatment protocol

    The pigs were randomly placed in three different groups of six pigs each. Pigs in group 1 received a single oral dose of 30 mg/kg body weight of TCBZ (Trisan 12%, Montana S.A., Peru). Pigs in group 2 were treated orally with OFZ (Synanthic? 9.06%, Fort Dodge, Mexico), using a single dose of 30 mg/kg body weight. Control pigs (group 3) received sugar water as a placebo. Each treatment group was housed in a single pen.

    2.4. Necropsy

    All animals were euthanized 17 wk after treatment, and necropsied at the School of Veterinary Medicine facilities in Lima, Peru. Pigs were anesthetized and sacrificed by intramuscular injection of a combination of ketamine (20 mg/kg) and xylazine (2 mg/kg) followed by intravenous injection of pentobarbital sodium overdose (60 mg/kg). Necropsy was performed immediately after euthanasia, and muscles from arms and legs were dissected, and all cysts were counted and classified. Cysts were classified as viable if a defined cystic structure with clear liquid content was still present, and degenerated if this had been replaced by semi-solid contents or an inflammatory scar (calcified nodule).

    2.5. Histological analysis

    Five randomized cysts from the muscles of each pig were fixed in 10% formalin, embedded in paraffin, then sectioned at 5μm and stained with hematoxyline and eosine (H&E), as well as Von Kossa stain to assess the presence of calcium.

    2.6. Data analysis

    Parasitic load was expressed in median with their respective ranges. A non-parametric one-way analysis of variance (Kruskall-Wallis) test was used to estimate the difference in the number of cysts between treatment groups. Data was analyzed using STATA 10 statistical software (v10.0; StataCorp LP, College Station, TX). Differences were considered statistically significant at P-value <0.05.

    2.7. Ethical approval

    The study was approved by the Animal Ethics Committee of the School of Veterinary Medicine, National University of San Marcos, Lima, Peru.

    3. Results

    During treatment and follow up, pigs from the treated groups involved in this experiment were apparently normal without apparent adverse events. All pigs used in this study were positive to cysticercosis at tongue examination as well as positive to 4 or more antibody bands enzyme-linked immunoelectro transfer blot. After necropsy, the overall parasite load including viable or degenerated cysts for each group was 1 658 (131 – 2 575) (median, interquartile range) cysts for control group, 1 414 (511 – 4 052) cysts for TCBZ treated group, and 259 (38 – 1 953) cysts for OFZ treated group (Table 1). All remaining cysts in the OFZ pigs were evidently degenerated. Furthermore, the numbers of cysts were statistically significantly smaller in OFZ group compared with the TCBZ and control groups (P<0.01).

    Table 1 Median, range and feature of larval stage of T. solium after treatment of pigs.

    TCBZ had very little effect against the parasitic cysts. Cysts from animals in the TCBZ group looked apparently normal after treatment. However, histological evaluation showed a mild to moderate degree of inflammation composed of eosinophils, macrophages, lymphocytes, plasmocytes, and fibroblasts with connective tissue in the surrounding parenchyma (Figure 1) in all samples from this group. On the other hand, OFZ killed 100% of cysts in treated pigs, and all animals in this group showed only degenerated cysts. The inflammatory reaction around cysts from the OFZ group was severe, and also demonstrated areas of dystrophic calcification (Figure 2). No inflammatory reaction was observed in pericystic tissue samples from pigs in the control group.

    Figure 1. Histological section of cysts from a pig treated with TCBZ (H&E stain).

    Figure 2. Histological section of cysts from a pig treated with OFZ (H&E stain).

    4. Discussion

    T. solium cysticercosis remains a public health issue in many developing countries, and therefore, the evaluation of new alternative drugs for its control is urgently required. A very large variety of antiparasitic drugs have been tested against cysticercus so far[10]. Although almost all these anthelmintic drugs are active against adult stages of cestodes, nematodes and trematodes, only a few drugs that have a positive effect against its larval stage[18,19].

    TCBZ, a benzimidazole drug, has a potent effect against adult and larval stages of some tissue helminths such as Fasciola and Paragonimus[14]. Likewise, studies in vitro have been shown effective activity in some nematodes and cestodes[13,20]. On these bases, we evaluated the efficacy of TCBZ against porcine cysticercosis. TCBZ in a single dose of 30 mg/kg was not effective against cysticercosis in this group of naturally infected pigs. On necropsy, there were no apparent differences in cyst burden or cyst appearance between pigs treated with TCBZ and pigs in the control group.

    Microscopic evaluation of cysts from treated pigs with TCBZ evidenced mild to moderate inflammatory reaction with presence of different types of leukocytes. This indicates that cysts is not found completely healthy, as observed at necropsy. This mild inflammatory reaction, macroscopically imperceptible, suggests that TCBZ has a slight effect against cysticerci raising the question of whether higher or multiple doses could be efficacious against cystic cestode larvae, as shown by Richter et al[20]. In that study, TCBZ had a positive activity against Echinococcus multilocularis metacestodes in vitro, using a 20-d treatment regime. Increased doses or multiple doses would still make TCBZ poorly practical for use in porcine cysticercosis in field conditions.

    Several antihelminthic drugs (ie. albendazole, flubendazole, fenbendazole, nitaxozanide, and praziquantel) have been tested for the treatment of porcine cysticercosis. Albendazole was evaluated using a single (50 mg/kg) and multiple doses (30 mg/kg) in experimentally infected pigs, and it was effective using multiple doses (3 consecutive days). However, some pigs treated to single and multiple doses showed secondary effects as anorexia, lethargy, prostration and death[11]. Nitazoxanide was tested in naturally infected pigs using multiple doses (150 mg/kg) by 7 consecutive days, and it was not effective against cysts. Some pigs treated with nitazoxanide developed prostatic hypertrophy and bladder distention[11]. In this experiment, single doses of 30 mg/kg of either OFZ or TCBZ did not produce any adverse effects in pigs. They were apparently normal and did not show any signs of toxicity during and after treatment.

    Flubendazole and fenbendazole have show efficacy against porcine cysticercosis when used in multiple doses, 40 mg/kg for 10 d and 5 mg/kg for 7 d, respectively, without secondary effects. Furthermore,praziquantel has been shown to have efficacy against cysticerci using daily doses of 50 mg / kg for 15 consecutive days[11,21]. However, animal treatments using multiple doses are impractical in field conditions and not suitable for mass chemotherapy campaigns in endemic zones. In summary our findings do not support the use of TCBZ for porcine cysticercosis, and confirm the efficacy of a single dose of OFZ for muscle cysticercosis cysts.

    Conflict of interest statement

    We declare that we have no conflict of interest.

    Acknowledgements

    Partial support from the Fogarty International Center/NIH (training grants D43 TW008273-03 and D43 TW001140) is acknowledged. Luis A. Gomez-Puerta’s PhD study, Ana Vargas Calla’s MSc study, and Juan Calcina’s MSc study are supported by the Fogarty International Center/NIH (D43 TW008273-03). Hector H. Garcia is supported by a Wellcome Trust Senior International Research Fellowship in Public Health and Tropical Medicine. Many thanks are also due to Dr. Narry Tiao for the comments and critique of the manuscript.

    References

    [1]Flisser A. State of the art of Taenia solium as compared to Taenia asiatica. Korean J Parasitol 2013; 51(1): 43-49.

    [2]Gilman RH, Gonzalez AE, Llanos-Zavalaga F, Tsang VC, Garcia HH, Cysticercosis Working Group in Peru. Prevention and control of Taenia solium taeniasis/cysticercosis in Peru. Pathog Glob Health 2012; 106(5): 312-318.

    [3]Del Brutto OH, Garcia HH. Neurocysticercosis. Handbook Clin Neurol 2013; 114: 313-325.

    [4]Handali S, Pawitan Y. Verifying elimination programs with a special emphasis on cysticercosis endpoints and postelimination surveillance. J Parasitol Res 2012; 2012: 974950.

    [5]Nash TE, Garcia HH. Diagnosis and treatment of neurocysticercosis. Nature Reviews Neurol 2011; 7(10): 584-594.

    [6]Flisser A, Rodriguez-Canul R, Willingham AL, 3rd. Control of the taeniosis/cysticercosis complex: future developments. Vet Parasitol 2006; 139(4): 283-292.

    [7]Gauci CG, Jayashi CM, Gonzalez AE, Lackenby J, Lightowlers MW. Protection of pigs against Taenia solium cysticercosis by immunization with novel recombinant antigens. Vaccine 2012; 30(26): 3824-3828.

    [8]Lightowlers MW. Control of Taenia solium taeniasis/cysticercosis: past practices and new possibilities. Parasitology 2013; 140(13): 1566-1577.

    [9]O'Neal S, Winthrop K, Gonzalez A. Cysticercosis control: bringing advances to the field. J Glob Infect Dis 2011; 3(2): 156-160.

    [10]Mkupasi EM, Sikasunge CS, Ngowi HA, Johansen MV. Efficacy and safety of anthelmintics tested against Taenia solium cysticercosis in pigs. PLoS Negl Trop Dis 2013; 7(7): e2200.

    [11]Gonzalez AE, Bustos JA, Jimenez JA, Rodriguez ML, Ramirez MG, Gilman RH, et al. Efficacy of diverse antiparasitic treatments for cysticercosis in the pig model. Am J Trop Med Hyg 2012; 87(2): 292-296.

    [12]Gonzales AE, Garcia HH, Gilman RH, Gavidia CM, Tsang VC, Bernal T, et al. Effective, single-dose treatment or porcine cysticercosis with oxfendazole. Am J Trop Med Hyg 1996; 54(4): 391-394.

    [13]Coles GC. Anthelmintic activity of triclabendazole. J Helminthol 1986; 60(3): 210-212.

    [14]Keiser J, Engels D, Buscher G, Utzinger J. Triclabendazole for the treatment of fascioliasis and paragonimiasis. Expert Opin Investig Drugs 2005; 14(12): 1513-1526.

    [15]Garcia HH, Gilman RH, Gonzalez AE, Verastegui M, Rodriguez S, Gavidia C, et al. Hyperendemic human and porcine Taenia solium infection in Peru. Am J Trop Med Hyg 2003; 68(3): 268-275.

    [16]Tsang VC, Brand JA, Boyer AE. An enzyme-linked immunoelectrotransfer blot assay and glycoprotein antigens for diagnosing human cysticercosis (Taenia solium). J Infect Dis 1989; 159(1): 50-59.

    [17]Gonzalez AE, Cama V, Gilman RH, Tsang VC, Pilcher JB, Chavera A, et al. Prevalence and comparison of serologic assays, necropsy, and tongue examination for the diagnosis of porcine cysticercosis in Peru. Am J Trop Med Hyg 1990; 43(2):194-199.

    [18]Coles TB, Lynn RC. Antiparasitic drugs. In: Bowman DD, editor. Georgis' parasitology for veterinarians. 10th ed. Missouri: Elsevier; 2014, p. 264 - 325.

    [19]Gonzalez AE, Bustos JA, Jimenez JA, Rodriguez ML, Ramirez MG, Gilman RH, et al. Efficacy of diverse antiparasitic treatments for cysticercosis in the pig model. Am J Trop Med Hyg 2012; 87(2): 292-296.

    [20]Richter D, Richter J, Gruner B, Kranz K, Franz J, Kern P. In vitro efficacy of triclabendazole and clorsulon against the larval stage of Echinococcus multilocularis. Parasitol Res 2013; 112(4): 1655-1660.

    [21]Flisser A, Gonzalez D, Shkurovich M, Madrazo I, Correa D, Rodriguez-Carbajal J, et al. Praziquantel treatment of porcine brain and muscle Taenia solium cysticercosis. 1. radiological, physiological and histopathological studies. Parasitol Res 1990; 76(3): 263-269.

    Contents lists available at ScienceDirect IF: 1.062
    Asian Pacific Journal of Tropical Medicine
    journal homepage:www.elsevier.com/locate/apjtm

    doi:Document heading 10.1016/j.apjtm.2015.12.005

    *Corresponding author:Luis A. Gomez-Puerta, Department of Veterinary Epidemiology and Economics, School of Veterinary Medicine, Universidad Nacional Mayor de San Marcos, Lima 41, Peru.

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