Your search keyword '"*GIARDIASIS treatment"' showing total 139 results

1. Leaky Gut and Giardia duodenalis Infection Associated Serum Zonulin Levels Among Calves: Randomized Clinical Study.

Author

ALIÇ URAL, Deniz

Subjects

GIARDIA, BLOOD serum analysis, GIARDIASIS treatment, PARASITIC diseases, DYSBIOSIS, CLINICAL trials

Abstract

Copyright of Türkiye Klinikleri Journal of Veterinary Sciences is the property of Turkiye Klinikleri and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

2. Technical Notes on High-Frequency Ultrasound Duodenography and Colonography Imaging of Giardial Lesions.

Author

Njemanze, Philip C., Njemanze, Josephine T., Ofoegbu, Clara C., Nneke, Esther, Onweni, Ijeoma A., Ejiogu, Uchechi V., Mgbenu, Chinenye U., Ukeje, Nneoma E., Amadi, Anthonia C., and Amaefule, Doris C.

Subjects

GIARDIASIS treatment, DIAGNOSIS of diarrhea, ULTRASONIC imaging, WATERBORNE infection, INTESTINAL parasites, IMMUNOCOMPROMISED patients

Abstract

Background: Worldwide G. lamblia is the third most common agent of diarrheal disease with over 300 million cases annually. Simple technical notes for clinicians are presented on use of high-frequency ultrasound imaging for duodenography and colonography in patients with Giardia lamblia infection. Methods: Ultrasound images were obtained from 100 consecutive patients with symptomatic giardiasis and 40 healthy controls. High-frequency annular array transducer of 7.5 MHz was used to obtain B-mode ultrasound grayscale and color images of the duodenum and colon with and without water contrast. The diagnosis of G. lamblia was based on clinical presentation, serial stool microscopy, and finding of flagellates in duodenal aspirates. Results: We demonstrated normal duodenum and colon echoanatomy in control subjects. In patients with giardiasis, the lesions of the duodenum and colon were associated with increased dimensions and wall thickness compared to healthy controls (P < 0.05). The ultrasound features of giardial lesions were characterized by increased wall echogenicity, flattening or loss of duodenal folds and/or colonic haustration, hyperechoic floating foci demonstrating chaotic motility, increased perilesional tissue echogenicity, and altered colonic peristalsis. Conclusion: In conclusion, high-frequency B-mode ultrasound imaging with and without water contrast demonstrated the details of duodenal and colonic echoanatomy in normal subjects and patients with giardiasis. The technique could be applied in the clinical setting of rural practitioners. [ABSTRACT FROM AUTHOR]

Published

2021

3. Molecular genotyping of Giardia lamblia assemblages by conventional polymerase chain reaction in rural and urban areas in Egypt.

Author

Abozahra, Rania, Mokhles, Moustafa, and Baraka, Kholoud

Subjects

MOLECULAR genetics, GIARDIA lamblia, POLYMERASE chain reaction, GIARDIASIS treatment, DISEASE prevalence, TRIOSE phosphates

Abstract

Background: Giardiasis is one of the most important parasitic gastro-intestinal infections that affect humans worldwide. Children are the most affected age group either in developing or developed countries. Genotyping of Giardia lamblia by molecular techniques classified it into eight assemblages; of which, assemblages A and B are potentially zoonotic pathogens. This study was done to investigate the prevalence of different Giardia lamblia genotypes by conventional polymerse chain reaction (PCR), and to explore the environmental and patients' sociodemographic factors that may affect the disease prevalence. Methods: Two hundreds fecal samples were collected at Damanhour General Hospital from patients with gastrointestinal diseases. All samples were examined microscopically, and the positive ones were investigated by conventional PCR. Results: Giardiasis was detected in 92 (46%) samples. Eighty-eight samples gave positive results by PCR, 18% of which were assemblage A, 70.5% were assemblage B, and 11.5% were mixed infection of both assemblages. The infection was more prevalent in males, rural patients and the highly educated ones. Conclusion: This study presents critical and demonstrative data regarding public health in Egypt. The results reveal that the prevalence of giardiasis is high among both rural and urban patients, particularly in children. It also prevails in patients of all education levels, and patients dealing and not dealing with animals. Moreover, we recommend PCR amplifying the triose phosphate isomerase (tpi) gene in fresh fecal samples as a very effective method for the diagnosis and genotyping. [ABSTRACT FROM AUTHOR]

Published

2021

4. COMPARISON OF SIDE EFFECTS OF SOME DRUGS USED FOR THE GIARDIASIS TREATMENT.

Author

Al-Qazwini, Yarub Modhar, Haddawee, Riyadh Hatim, and Abbas, Jabbar Ashour

Subjects

DRUG side effects, ADVERSE health care events, GIARDIASIS treatment, NITROIMIDAZOLES, ALBENDAZOLE

Abstract

Our current research includes a comparative study between a set of samples for patients with giardiasis in some medical clinics, when two types of the common drug are used as a treatment to cure infection with the giardia parasite, namely (Nitroimidazole and Albendazole). The comparison included two aspects, the first; aspect is knowing the most important side effects that arise after up taking these two treatments independently (dose, adverse effects, pharmacokinetics, interactions), while the second; aspect of the comparison included studying the most important significant differences between the two treatments that were counted by some through statistical tests, this is when counting the patients who used these two drugs for treatment in a single clinic according to the data recorded by the medical clinics for patients with giardia in Babylon. After microscopic examination of samples taken from infected patients, in the laboratory the giardiasis is clearly seen in the maturity stage in addition to the cystic phase. The total of the samples studied is (93 samples), of which (40 samples) were used with (Nitroimidazole) as a drug for treatment of giardiasis, while (53 samples) were used with (Albendazole) as a drug for treatment. [ABSTRACT FROM AUTHOR]

Published

2021

5. Update on Giardia: Highlights from the seventh International Giardia and Cryptosporidium Conference.

Author

Buret, André G., Cacciò, Simone M., Favennec, Loïc, and Svärd, Staffan

Subjects

GIARDIA, EPIDEMIOLOGY, GENOMICS, CYTOLOGY, DIARRHEA, GIARDIASIS treatment

Abstract

Copyright of Parasite (1252607X) is the property of EDP Sciences and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2020

6. Piqueria trinervia as a source of metabolites against Giardia intestinalis

Author

Yadira Rufino-González, Martha Ponce-Macotela, Manuel Jiménez-Estrada, Candy N. Jiménez-Fragoso, Guadalupe Palencia, Gabriel Sansón-Romero, Anahi Anzo-Osorio, and Mario N. Martínez-Gordillo

Subjects

piquerol, trinervinol, giardiasis treatment, Therapeutics. Pharmacology, RM1-950

Abstract

Context: Piqueria trinervia Cav. (Asteraceae) is a plant species with a long history in traditional medicine to cure diarrhoea and other digestive disorders. Objective: The study investigates the antigiardial activity of piquerol, trinervinol, red oil and two fractions (F1 and F2) from P. trinervia. Materials and methods: P. trinervia was collected in the Ajusco in Mexico City. Aerial parts were ground and mixed with water to obtain the extract, which was treated with dichloromethane to isolate piquerol and trinervinol (P & T). Remnants were the red oil, fractions 1 and 2 (RO, F1 & F2). Trophozoites of Giardia intestinalis were treated with P, T, RO, F1 and F2 at different concentrations (0.78–200 μg/mL) for 48 h. Antigiardial activity was measured using the methylene blue reduction, and the cytotoxicity assayed on human fibroblasts and Vero cells by reduction of tetrazolium salts. Results: Trinervinol and piquerol showed antigiardial activity with an IC50 = 2.03 and 2.42 μg/mL, and IC90 = 13.03 and 8.74 μg/mL, respectively. The concentrations of trinervinol (CC50 = 590 μg/mL) and piquerol (CC50 = 501 μg/mL) were not cytotoxic to human fibroblasts. Conclusions: Compounds from P. trinervia showed antigiardial activity; to enhance this activity, piquerol and trinervinol can be chemically modified.

Published

2017

7. STUDY OF SOME PATHOGENESIS ASPECTS IN PUPPIES AFTER EXPERIMENTAL INFECTION OF PUPPIES WITH GIARDIA DUODENALIS.

Author

Swadi, Hisham A. and Zenad, Mohammad M.

Subjects

GIARDIASIS treatment, DOG diseases, TUMOR necrosis factors, GLUTATHIONE, SUPEROXIDE dismutase

Abstract

The purpose of this study was to investigate some pathogenesis aspects in puppies after experimental infection with G. duodenalis of 10 local breed dogs, age 4 months as experimental infected dogs and 5 dogs as control.A clinical signs of experimental infection of puppies showed mild increased in the temperature and respiratory rate after one week of infection.The results of biochemical tests showed significant increas in the levels of blood sugar and decreased in the insulin and amylase level; significant decreased in the levels of serum cholesterol, triglycerides, VLDL, LDL and HDL, while alkaline phosphatase showed significant increased.The measurement of antibodies concentration revealed that the significant decreased in the concentration of the IgA was found in the experimental infected dogs compared with control dogs, while no significant differences was found in the concentration of the IgG. The measurement of antioxidant concentration demonstrated a significant decreased in the levels of glutathione and superoxide dismutase in the duodenum, liver, gall bladder and pancreas in infected dogs compared with non infected dogs.A different histopathological changes was found induodenum, Pancreas, gall baldder and liver. Internal tissue (duodenum, pancreas, liver and gall bladde) were Immunohistchemically evaluated for two receptors, which were tumor nectosis factor – alpha ( TNF-alpha) and interluken- 6 (IL-6). Tumor nectosis factor – alpha receptor was positive in 80% of doudenum, 60% of pancreas, 50% of gall bladder and 30% of liver of the expermintal infected dogs. Duodenum postive (70%) for IL-6 more frequent than of the panceas, liver and gall bladder (60%, 20% and 60% respectivly). [ABSTRACT FROM AUTHOR]

Published

2019

8. EFFECT OF BERBERINE ON GIARDIASIS.

Author

Mohammad, Fatima Ibrahim, Muhammed Ridh, Doaa Abd Alabas, and Kokaz, OsamahFaisal

Subjects

BERBERINE, GIARDIASIS treatment, PROTOZOAN diseases, HERBS, WEIGHT loss

Abstract

Giardia is one of a protozoal parasites that infect the upper small intestine of mammals and causes intestinal symptoms such as abdominal pains, chronic diarrhea, malabsorption of the fats and weight loss, this parasite spread in world wide and infect all ages especially poor communites. There are many herbs that use to treat Giardia such as berberineis a plant alkaloid use in traditional Chinese and indigenous Indian medicine dating back at least 3,000 years, it's produced by herbs Coptis chinensis, Berberisa quifolium, Hydrastis canadensis, Berberis aristata, Berberis vulgaris. Berberine has proved antimicrobial activity against protozoan. [ABSTRACT FROM AUTHOR]

Published

2019

9. A natural zoonotic giardiasis: Infection of a child via Giardia cysts in pet chinchilla droppings.

Author

Tůmová, P., Mazánek, L., Lecová, L., Dluhošová, J., Typovská, H., Kotrašová, V., Ticháčková, V., and Nohýnková, E.

Subjects

*GIARDIASIS, *GIARDIASIS treatment, *CHINCHILLA rabbits, *GIARDIA lamblia, *JUVENILE diseases, *INFECTIOUS disease transmission

Abstract

Abstract Here, we report a case of direct zoonotic transmission of giardiasis between a pet chinchilla and a human. Microscopic and molecular examinations of stool samples from a child and samples of chinchilla droppings revealed cysts/DNA of Giardia intestinalis. The transmission from the chinchilla to the child has been confirmed as coprophagous after the 1-year-old toddler ingested pet chinchilla droppings. Molecular analysis of the gdh gene from both hosts classified the G. intestinalis cysts into the assemblage B genetic group, which has been previously shown to be characteristic of both human and chinchilla giardiasis. Both Giardia sub-assemblages BIII and BIV were present in the chinchilla droppings, whereas only the sub-assemblage BIV was isolated from the child's stool sample. To the best of our knowledge, this is the first report of a true zoonotic transmission of giardiasis, supporting the zoonotic potential of assemblage B. Highlights • Giardiasis is a significant public health concern because of its high prevalence and propensity to cause outbreaks. • Our study is the first to confirm the natural zoonotic transmission of Giardia intestinalis between a pet chinchilla and a child. • This case report is indicative of the hypothesized zoonotic potential of the G. intestinalis genetic group assemblage B. [ABSTRACT FROM AUTHOR]

Published

2018

10. Cellular immune responses in peripheral blood lymphocytes of Giardia infected squirrel monkey (Saimiri boliviensis boliviensis) treated with Fenbendazole.

Author

Nehete, Pramod N., Wilkerson, Gregory, Nehete, Bharti P., Chitta, Sriram, Ruiz, Julio C., Scholtzova, Henrieta, Williams, Lawrence E., Abee, Christian R., and Vanchiere, John A.

Subjects

*CELLULAR immunity, *LYMPHOCYTES, *GIARDIA, *GIARDIASIS treatment, *SQUIRREL monkeys, *FENBENDAZOLE

Abstract

Cellular immune responses were tested to determine the effect of fenbendazole on the function of lymphocytes from Bolivian squirrel monkeys (Samiri boliviensis boliviensis). Giardia-infected squirrel monkeys were treated with commercially available fenbendazole (FBZ)-medicated monkey chow. Immune responses were compared between historical controls (Giardia naïve, untreated with FBZ (control animals)) and Giardia-infected, FBZ-treated squirrel monkeys (study animals). Peripheral blood lymphocytes from study monkeys had significantly lower stimulation indices compared to control animals when cultured in vitro with concanavalin A (Con A) (p<0.0001), phytohaemagglutinin (PHA) (p<0.0001) and lipopolysaccharide (LPS) (p<0.0001). PBMCs were also analyzed for IFN-γ producing cells in response to stimulation with Con A, PHA, PWM, and LPS by the cytokine ELISPOT assay. Significantly higher responses to Con A- (p<0.0001), and PHA- (p<0.001) stimulated cultures from Giardia-infected and fenbendazole treated compared to controls. Flow cytometric analysis for expression of cell surface markers revealed a significant increase in B- and NKT-lymphocytes and significant decrease in CD14+CD16+ monocytes after FBZ treatment. Also, circulating plasma cytokines IFN-γ, TNF-α, IL-12p40, IL-1β, IL-10, IL-13, IL-1ra, IL-6 and IL-4 were significantly decreased after FBZ treatment. Comparison of hematologic parameters between controls and FBZ-treated squirrel monkeys revealed significantly lower numbers of total leukocytes, neutrophils, monocytes, and eosinophils compared to controls. However, erythrocyte indices (red cell count, hemoglobin and hematocrit were significantly higher in FBZ-treated monkeys. Our findings suggest that fenbendazole treatment may alter sensitive immune and molecular measures of inflammation. Postponing the experimental use of squirrel monkeys until at least 6 weeks after FBZ treatment should be considered. [ABSTRACT FROM AUTHOR]

Published

2018

11. Longitudinal cohort study of serum antibody responses towards Giardia lamblia variant-specific surface proteins in a non-endemic area.

Author

Hjøllo, Torunn, Bratland, Eirik, Steinsland, Hans, Radunovic, Matej, Langeland, Nina, and Hanevik, Kurt

Subjects

*HUMORAL immunity, *ANTIBODY formation, *GIARDIA lamblia, *GIARDIASIS treatment, *SERUM, *COHORT analysis

Abstract

Introduction/Aims The long-term humoral immune response after a natural giardiasis infection is not well understood. The aim of this study was to evaluate longitudinal serum IgA and IgG/M responses towards conserved regions of two Giardia variant-specific surface proteins (VSP) and whether these responses differ between Giardia assemblages and durations of infection. Methods We recruited thirty Giardia -positive patients, mainly returning travellers, and eighteen healthy adults presumed to be Giardia unexposed. Blood samples were collected before treatment, and at 6 weeks, 6 months and 12 months after the infection cleared. We used a multiplex bead-based flow cytometry immunoassay to measure Giardia specific IgA and IgG/M responses targeting two recombinant antigens from G. lamblia VSP proteins 3 and 5 (VSP3 and VSP5). Results Serum levels of anti-VSP5 and anti-VSP3 IgA decreased rapidly to low levels after treatment but continued to be substantially higher than that of presumed unexposed controls even after 6 and 12 months. The IgG/M response decreased more gradually but remained significantly higher than presumed unexposed controls at all time points, except for anti-VSP3 at 12 months. There were no significant difference in responses for infections with assemblage A and assemblage B Giardia lamblia . Chronic infections (>8 weeks) were associated with a significantly lower anti-VSP5 IgG/M response. Conclusion This study describes the kinetics of the humoral immune response against two Giardia VSP proteins over one year, and the considerable cross reactivity between the two human infective Giardia assemblages. Persons with chronic Giardia infection seem to have lower levels of VSP antibodies. [ABSTRACT FROM AUTHOR]

Published

2018

12. Detecting endomysial and tissue transglutaminase antibodies in patients with giardiasis.

Author

Hajialiani, Fateme, Tabatabaie, Fatemeh, Akhlaghi, Lame, and Damercheli, Mahlegha

Subjects

*TRANSGLUTAMINASES, *IMMUNOGLOBULINS, *CELIAC disease diagnosis, *CELIAC disease, *GIARDIASIS, *GIARDIASIS treatment

Abstract

Celiac disease is a genetic disease diagnosed to be associated with chronic intestinal inflammation. Endomysial and tissue transglutaminase antibodies are the best serum markers for celiac disease (CD) diagnosis. This research aimed to determine the levels of endomysial and tissue transglutaminase antibodies in patients with giardiasis. Forty cases of giardiasis were selected among the referees to Milad Hospital in Tehran, as well as a children’s hospital and some health centers in Karaj. Euro-immune IgA immunofluorescence and ELISA were utilized to measure their titers of endomysial and tissue transglutaminase antibodies, respectively. Twenty random serum samples of negative Giardia and 16 serum samples of positive anti-(tissue transglutaminase) tTG antibodies were evaluated by using ELISA and endomysium antibody through immunofluorescence techniques. Among the 40 cases of giardiasis, 16 positive endomysial and transglutaminase antibodies (40%) were detected. Sixteen positive samples of endomysial antibody (EMA) were also positive for anti-tTG, and 20 random negative samples were negative for EMA and anti-tTG. The chi-square test revealed a significant association between antibodies and giardiasis (P = 0.001). Atrophy of the intestinal villi can arise after giardia infection by mimicking the behavioral patterns of anti-EMA and anti-tTG antibodies. Due to low specificity, anti-gliadin antibody test is not helpful in detecting CD in patients with giardiasis. In the present study on anti-EMA and anti-tTG in patients with giardiasis, these antibodies were positive in giardiasis. Thus, the best and most reliable way to diagnose CD and treat giardiasis is intestinal biopsy as the gold standard method. [ABSTRACT FROM AUTHOR]

Published

2018

13. Comparative efficacy of drugs for treating giardiasis: a systematic update of the literature and network meta-analysis of randomized clinical trials.

Author

Ordóñez-Mena, José M., McCarthy, Noel D., and Fanshawe, Thomas R.

Subjects

*DRUG efficacy, *GIARDIASIS treatment, *CLINICAL trials, *META-analysis, *RANDOMIZED controlled trials, *ANTHELMINTICS, *COMPARATIVE studies, *GIARDIASIS, *IMIDAZOLES, *METRONIDAZOLE, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *SYSTEMATIC reviews, *EVALUATION research, *TREATMENT effectiveness, *ANTIPROTOZOAL agents, *THERAPEUTICS

Abstract

Background: Giardiasis is the commonest intestinal protozoal infection worldwide. The current first-choice therapy is metronidazole. Recently, other drugs with potentially higher efficacy or with fewer and milder side effects have increased in popularity, but evidence is limited by a scarcity of randomized controlled trials (RCTs) comparing the many treatment options available. Network meta-analysis (NMA) is a useful tool to compare multiple treatments when there is limited or no direct evidence available.Objectives: To compare the efficacy and side effects of all available drugs for the treatment of giardiasis.Methods: We selected all RCTs included in systematic reviews and expert reviews of all treatments for giardiasis published until 2014, extended the systematic literature search until 2016, and identified new studies by scanning reference lists for relevant studies. We then conducted an NMA of all available treatments for giardiasis by comparing parasitological cure (efficacy) and side effects.Results: We identified 60 RCTs from 58 reports (46 from published systematic reviews, 8 from reference lists and 4 from the updated systematic search). Data from 6714 patients, 18 treatments and 42 treatment comparisons were available. Tinidazole was associated with higher parasitological cure than metronidazole [relative risk (RR) 1.23, 95% CI 1.12-1.35] and albendazole (RR 1.35, 95% CI 1.21-1.50). Taking into consideration clinical efficacy, side effects and amount of the evidence, tinidazole was found to be the most effective drug.Conclusions: We provide additional evidence that single-dose tinidazole is the best available treatment for giardiasis in symptomatic and asymptomatic children and adults. [ABSTRACT FROM AUTHOR]

Published

2018

14. Bile Salt Hydrolase Activities: A Novel Target to Screen Anti-Giardia Lactobacilli?

Author

Allain, Thibault, Chaouch, Soraya, Thomas, Myriam, Travers, Marie-Agnès, Valle, Isabelle, Langella, Philippe, Grellier, Philippe, Polack, Bruno, Florent, Isabelle, and Bermúdez-Humarán, Luis G.

Subjects

BILE salts, HYDROLASES, GIARDIASIS treatment, GIARDIA, PARASITIC diseases

Abstract

Giardia duodenalis is a protozoan parasite responsible for giardiasis, a disease characterized by intestinal malabsorption, diarrhea and abdominal pain in a large number of mammal species. Giardiasis is one of the most common intestinal parasitic diseases in the world and thus a high veterinary, and public health concern. It is wellestablished that some probiotic bacteria may confer protection against this parasite in vitro and in vivo and we recently documented the implication of bile-salt hydrolase (BSH)-like activities from strain La1 of Lactobacillus johnsonii as mediators of these effects in vitro. We showed that these activities were able to generate deconjugated bile salts that were toxic to the parasite. In the present study, a wide collection of lactobacilli strains from different ecological origins was screened to assay their antigiardial effects. Our results revealed that the anti-parasitic effects of some of the strains tested were well-correlated with the expression of BSH-like activities. The two most active strains in vitro, La1 and Lactobacillus gasseri CNCM I-4884, were then tested for their capacity to influence G. duodenalis infection in a suckling mice model. Strikingly, only L. gasseri CNCM I-4884 strain was able to significantly antagonize parasite growth with a dramatic reduction of the trophozoites load in the small intestine. Moreover, this strain also significantly reduced the fecal excretion of Giardia cysts after 5 days of treatment, which could contribute to blocking the transmission of the parasite, in contrast of La1 where no effect was observed. This study represents a step toward the development of new prophylactic strategies to combat G. duodenalis infection in both humans and animals. [ABSTRACT FROM AUTHOR]

Published

2018

15. Bile-Salt-Hydrolases from the Probiotic Strain Lactobacillus johnsonii La1 Mediate Anti-giardial Activity in Vitro and in Vivo.

Author

Allain, Thibault, Chaouch, Soraya, Thomas, Myriam, Vallée, Isabelle, Buret, André G., Langella, Philippe, Grellier, Philippe, Polack, Bruno, Bermúdez-Humarán, Luis G., and Florent, Isabelle

Subjects

GIARDIASIS treatment, THERAPEUTIC use of probiotics, LACTOBACILLUS

Abstract

Giardia duodenalis (syn. G. lamblia, G. intestinalis) is the protozoan parasite responsible for giardiasis, themost common and widely spread intestinal parasitic disease worldwide, affecting both humans and animals. After cysts ingestion (through either contaminated food or water), Giardia excysts in the upper intestinal tract to release replicating trophozoites that are responsible for the production of symptoms. In the gut, Giardia cohabits with the host's microbiota, and several studies have revealed the importance of this gut ecosystem and/or some probiotic bacteria in providing protection against G. duodenalis infection through mechanisms that remain incompletely understood. Recent findings suggest that Bile-Salt-Hydrolase (BSH)-like activities from the probiotic strain of Lactobacillus johnsonii La1 may contribute to the anti-giardial activity displayed by this strain. Here, we cloned and expressed each of the three bsh genes present in the L. johnsonii La1 genome to study their enzymatic and biological properties. While BSH47 and BSH56 were expressed as recombinant active enzymes, no significant enzymatic activity was detected with BSH12. In vitro assays allowed determining the substrate specificities of both BSH47 and BSH56, which were different. Modeling of these BSHs indicated a strong conservation of their 3-D structures despite low conservation of their primary structures. Both recombinant enzymes were able tomediate anti-giardial biological activity against Giardia trophozoites in vitro. Moreover, BSH47 exerted significant anti-giardial effects when tested in a murine model of giardiasis. These results shed new light on the mechanism, whereby active BSH derived from the probiotic strain Lactobacillus johnsonii La1 may yield anti-giardial effects in vitro and in vivo. These findings pave the way toward novel approaches for the treatment of this widely spread but neglected infectious disease, both in human and in veterinary medicine. [ABSTRACT FROM AUTHOR]

Published

2018

16. Effect of Piper betle on Giardia intestinalis infection in vivo.

Author

Pecková, Radka, Doležal, Karel, Sak, Bohumil, Květoňová, Dana, Kváč, Martin, Nurcahyo, Wisnu, and Foitová, Ivona

Subjects

*GIARDIASIS treatment, *PIPER betle, *METRONIDAZOLE, *HISTOLOGY, *SCANNING electron microscopy

Abstract

Piper betle has been used as a medicinal plant in traditional medical systems throughout South and South East Asia. Experimental studies have revealed its wide and diverse biological and pharmacological effects. In this study, antigiardial activity of Piper betle was tested using experimental infections of Giardia intestinalis , the most common cause of protozoal diarrhoea worldwide, in Mongolian gerbils. Plants were extracted in water, methanol and methanol:tetrahydrofuran. Gerbils were treated for ten days intragastrically twice a day, with the dose of 40 mg of the extract per 100 g of body weight. Drug metronidazole was used as a negative control. Gerbils' faeces were taken every day and examined by flotation method, the number of shed cysts were counted using a haemocytometer. After gerbils' sacrifice and dissection, their duodena were then processed for examination using histological sectioning and scanning electron microscopy. The antigiardial activity was evaluated by the course of cyst shedding throughout the entire experiment. A significant decline in cyst shedding, evaluated by linear regression was found in gerbils treated with the aqueous extract. Our results indicate that the aqueous extract of P. betle shows giardicidal effects. [ABSTRACT FROM AUTHOR]

Published

2018

17. Nitroimidazole-refractory giardiasis: a growing problem requiring rational solutions.

Author

Carter, E.R., Nabarro, L.E., Hedley, L., and Chiodini, P.L.

Subjects

*ALBENDAZOLE, *COMBINATION drug therapy, *GIARDIA lamblia, *GIARDIASIS treatment, *QUINACRINE, *METRONIDAZOLE, *NITROIMIDAZOLES, *DRUG resistance in bacteria

Abstract

Background Giardia intestinalis is microaerophilic diarrhoea-causing protozoan common in countries with suboptimal sanitation. Standard treatment is with nitroimidazoles, but a growing number of refractory cases is being reported. Treatment failure has become increasingly prevalent in travellers who contract giardiasis in Asia. Clinicians are increasingly falling back on second-line and less well-known drugs to treat giardiasis. Aims To review nitroimidazole-refractory G. intestinalis infection, examine the current efficacy of standard therapeutic agents, consider potential resistance mechanisms which could cause treatment failure and describe the practical aspects of managing this emerging clinical problem. Sources A PubMed search was conducted using combinations of the following terms: refractory, Giardia, giardiasis, resistance and treatment. Articles on the pharmacotherapy, drug resistance mechanisms and use of alternative agents in nitroimidazole-refractory giardiasis were reviewed. Content We review the standard drugs for giardiasis, including their efficacy in initial treatment, mode of action and documented in vitro and in vivo drug resistance. We assess the efficacy of alternative drugs in nitroimidazole-refractory disease. Existing data suggest a potential advantage of combination treatment. Implications An optimal treatment strategy for refractory giardiasis has still to be determined, so there is no standard treatment regimen for nitroimidazole-refractory giardiasis. Further work on drug resistance mechanisms and the use of drug combinations in this condition is a priority. [ABSTRACT FROM AUTHOR]

Published

2018

18. Piqueria trinervia as a source of metabolites against Giardia intestinalis.

Author

Rufino-González, Yadira, Ponce-Macotela, Martha, Jiménez-Estrada, Manuel, Jiménez-Fragoso, Candy N., Palencia, Guadalupe, Sansón-Romero, Gabriel, Anzo-Osorio, Anahi, and Martínez-Gordillo, Mario N.

Subjects

*ASTERACEAE, *METABOLITES, *TROPHOZOITES, *TRADITIONAL medicine, *THERAPEUTICS, *DIARRHEA

Abstract

Context:Piqueria trinerviaCav. (Asteraceae) is a plant species with a long history in traditional medicine to cure diarrhoea and other digestive disorders. Objective:The study investigates the antigiardial activity of piquerol, trinervinol, red oil and two fractions (F1 and F2) fromP. trinervia. Materials and methods:P. trinerviawas collected in the Ajusco in Mexico City. Aerial parts were ground and mixed with water to obtain the extract, which was treated with dichloromethane to isolate piquerol and trinervinol (P & T). Remnants were the red oil, fractions 1 and 2 (RO, F1 & F2). Trophozoites ofGiardia intestinaliswere treated with P, T, RO, F1 and F2 at different concentrations (0.78–200 μg/mL) for 48 h. Antigiardial activity was measured using the methylene blue reduction, and the cytotoxicity assayed on human fibroblasts and Vero cells by reduction of tetrazolium salts. Results:Trinervinol and piquerol showed antigiardial activity with an IC50 = 2.03 and 2.42 μg/mL, and IC90 = 13.03 and 8.74 μg/mL, respectively. The concentrations of trinervinol (CC50 = 590 μg/mL) and piquerol (CC50 = 501 μg/mL) were not cytotoxic to human fibroblasts. Conclusions:Compounds fromP. trinerviashowed antigiardial activity; to enhance this activity, piquerol and trinervinol can be chemically modified. [ABSTRACT FROM PUBLISHER]

Published

2017

19. Human Leukocyte Antigen Class II Alleles in Children with Giardiasis.

Author

El-Belehy, Ayat Abd El-Aziz

Subjects

GIARDIASIS treatment, PROTOZOAN diseases, HLA histocompatibility antigens, JUVENILE diseases, FOODBORNE diseases

Abstract

Copyright of Journal of Plant Production is the property of Egyptian National Agricultural Library (ENAL) and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2017

20. Curcumin alters the cytoskeleton and microtubule organization on trophozoites of Giardia lamblia.

Author

Gutiérrez-Gutiérrez, Filiberto, Palomo-Ligas, Lissethe, Hernández-Hernández, José Manuel, Pérez-Rangel, Armando, Aguayo-Ortiz, Rodrigo, Hernández-Campos, Alicia, Castillo, Rafael, González-Pozos, Sirenia, Cortés-Zárate, Rafael, Ramírez-Herrera, Mario Alberto, Mendoza-Magaña, María Luisa, and Castillo-Romero, Araceli

Subjects

*GIARDIASIS treatment, *CURCUMIN, *CYTOSKELETON, *MICROTUBULES, *TROPHOZOITES, *GIARDIA lamblia, *THERAPEUTICS

Abstract

Giardia lamblia is a worldwide protozoan responsible for a significant number of intestinal infections. There are several drugs for the treatment of giardiasis, but they often cause side effects. Curcumin, a component of turmeric, has antigiardial activity; however, the molecular target and mechanism of antiproliferative activity are not clear. The effects of curcumin on cellular microtubules have been widely investigated. Since tubulin is the most abundant protein in the cytoskeleton of Giardia , to elucidate whether curcumin has activity against the microtubules of this parasite, we treated trophozoites with curcumin and the cells were analyzed by scanning electron microscopy and confocal microscopy. Curcumin inhibited Giardia proliferation and adhesion in a time-concentration-dependent mode. The higher inhibitory concentrations of curcumin (3 and 15 μM) disrupted the cytoskeletal structures of trophozoites; the damage was evident on the ventral disk, flagella and in the caudal region, also the membrane was affected. The immunofluorescence images showed altered distribution of tubulin staining on ventral disk and flagella. Additionally, we found that curcumin caused a clear reduction of tubulin expression. By docking analysis and molecular dynamics we showed that curcumin has a high probability to bind at the interface of the tubulin dimer close to the vinblastine binding site. All the data presented indicate that curcumin may inhibit Giardia proliferation by perturbing microtubules. [ABSTRACT FROM AUTHOR]

Published

2017

21. Structural characterization of Giardia duodenalis thioredoxin reductase (gTrxR) and computational analysis of its interaction with NBDHEX.

Author

Brogi, Simone, Fiorillo, Annarita, Chemi, Giulia, Butini, Stefania, Lalle, Marco, Ilari, Andrea, Gemma, Sandra, and Campiani, Giuseppe

Subjects

*METRONIDAZOLE, *GIARDIASIS treatment, *THIOREDOXIN reductase (NADPH), *ANTIPARASITIC agents, *DRUG efficacy, *THERAPEUTICS

Abstract

Giardia duodenalis is a microaerophilic parasite that colonizes the upper portions of the small intestine of humans. Giardia infection is a major contributor to diarrheal disease worldwide. Nitroheterocycles (e.g. metronidazole) or benzimidazoles (e.g. albendazole) are the most commonly used therapeutic agents. Unfortunately, their efficacy is reduced by low compliance or resistance phenomena. We recently discovered that the antitumoral drug 6-(7-nitro-2,1,3-benzoxadiazol-4-ylthio)hexanol (NBDHEX) is active against G. duodenalis trophozoites and its mode of action is linked to inhibition of thioredoxin reductase ( g TrxR), a key component of Giardia redox system: g TrxR provides efficient defenses against reactive oxygen species (ROS), it is a target of 5-nitroimidazoles antiparasitic drugs and also contributes to their metabolism. However, the exact mechanism responsible for the g TrxR inhibition mediated by this chemical class of antigiardial compounds is yet to be defined. The definition of the structural determinants of activity against g TrxR could be important for the identification of novel drugs endowed with an innovative mode of action. With this aim, we solved the crystal structure of g TrxR and we analyzed in silico the binding mode of NBDHEX. The data presented herein could guide the development of NBDHEX derivatives tailored for selective inhibition of g TrxR as antigiardial agents. [ABSTRACT FROM AUTHOR]

Published

2017

22. A survey for potentially zoonotic gastrointestinal parasites in domestic cavies in Cameroon (Central Africa).

Author

Meutchieye, Felix, Kouam, Marc K., Miegoué, Emile, Nguafack, Terence T., Tchoumboué, Joseph, Téguia, Alexis, and Théodoropoulos, Georgios

Subjects

*ZOONOSES, *GIARDIASIS treatment, *CRYPTOSPORIDIUM, *DOMESTIC animals, *GASTROINTESTINAL disease treatment

Abstract

Background: Farm animals are usually suspected to transmit infections to humans. Domestic cavies (Cavia porcellus) are hosts to a variety of pathogens, some of which are zoonotic. Several parasites including the protozoa Giardia spp. and Cryptosporidium spp. may be causative agents of gastrointestinal disorders in domestic cavies and humans. The aim of the study was to investigate the occurrence of potentially zoonotic protozoa as well as any potential zoonotic gastrointestinal parasite in domestic cavies raised under a semi extensive system in the rural areas of Cameroon. Results: Giardia/Cryptosporidium antigens were detected in 12.90% of cavies. Helminthe eggs were found in 1.52% of animals. The prevalence of Paraspidodera uncinata, Heligmosomoides polygyrus (also known as Nematospiroides dubius) and Trichuris sp. was 1% (4/397), 0.3% (1/397), and 0.3% (1/397), respectively. Presence of Giardia/Cryptosporidium was unrelated to the occurrence of diarrhea, as none of the positive samples was from a diarrheic individual. Conclusion: Domestic cavies are hosts of Giardia/Cryptosporidium and appear as potential source of human giardiasis, cryptosporidiosis and infection with H. polygyrus in Cameroon. In keeping with the One Health Initiative, veterinarians and medical doctors should collaborate to address the problem of Giardia and Cryptosporidium infection in cavies and cavy breeders both in Cameroon and other countries with a similar cavy breeding system. Follow-up studies are required to further taxonomically characterize these cavy parasites and to determine their routes of transmission to humans. [ABSTRACT FROM AUTHOR]

Published

2017

23. Giardiasis Diagnosis and Treatment Practices Among Commercially Insured Persons in the United States.

Author

Beer, Karlyn D., Collier, Sarah A., Fan Du, and Gargano, Julia W.

Subjects

*GIARDIASIS, *GIARDIASIS treatment, *PARASITIC disease treatment, *NOSOLOGY, *INSURANCE claims, *PUBLIC health, *DIAGNOSIS

Abstract

Background. Giardiasis, the most common enteric parasitic infection in the United States, causes an estimated 1.2 million episodes of illness annually. Published clinical recommendations include readily available Giardia-specific diagnostic testing and antiparasitic drugs. We investigated sequences of giardiasis diagnostic and treatment events using MarketScan, a large health insurance claims database. Methods. We created a longitudinal cohort of 2995 persons diagnosed with giardiasis (International Classification of Diseases, Ninth Revision, Clinical Modification [ICD-9-CM] code 007.1) from 2006 to 2010, and analyzed claims occurring 90 days before to 90 days after initial diagnosis. We evaluated differences in number and sequence of visits, diagnostic tests, and prescriptions by age group (children 1-17 years, adults 18-64 years) using Χ2 tests and data visualization software. Results. Among 2995 patients (212 433 claims), 18% had a Giardia-specific test followed by or concurrent with an effective antiparasitic drug, without ineffective antibiotics. Almost two-thirds of patients had an antiparasitic and 27% had an antibiotic during the study window. Compared with children, adults more often had ≥3 visits before diagnosis (19% vs 15%; P = .02). Adults were also less likely to have a Giardia-specific diagnostic test (48% vs 58%; P < .001) and more likely to have an antibiotic prescription (28% vs 25%; P = .04). When Giardia-specific tests and antiparasitic and antibiotic prescriptions were examined, pediatric clinical event sequences most frequently began with a Giardia-specific test, whereas adult sequences most frequently began with an antiparasitic prescription. Conclusions. Giardiasis care infrequently follows all aspects of clinical recommendations. Multiple differences between pediatric and adult care, despite age-agnostic recommendations, suggest opportunities for provider education or tailored guidance. [ABSTRACT FROM AUTHOR]

Published

2017

24. Synergistic effects of fenbendazole and metronidazole against Giardia muris in Swiss mice naturally infected.

Author

Bezagio, Renata, Colli, Cristiane, Romera, Liara, Ferreira, Érika, Falavigna-Guilherme, Ana, and Gomes, Mônica

Subjects

*DRUG synergism, *FENBENDAZOLE, *METRONIDAZOLE, *GIARDIA, *LABORATORY mice, *PROBIOTICS, *GIARDIASIS treatment

Abstract

In this study were proposed different protocols for the treatment of mice naturally infected with Giardia muris. Male Swiss mice were divided into seven groups, with five animals each, in a blind, controlled, randomized by drawing lots and once-repeated experiment. Parasite detection and cure control were performed using the Faust method and search by trophozoites in the intestinal mucosa. Clinical parameters (weight, water and feed consumption, elimination of excreta, aspect of the fur and feces) were also evaluated. All animals were treated with metronidazole (M), fenbendazole (F), and probiotics (P), administered intragastrically, during 7 days. M1, FM1, and F1 groups were treated 1×/day; M3, FM3, and PM3 groups 3×/day; and ST (control group) received only water. After the 5th and 7th days of treatment, the animals in FM1/FM3 and PM3/M3 groups presented, respectively, negative results and remained negative in the following 10 days. Animals in F1 group consumed less water ( p = 0.00010) compared with FM1/FM3/PM3. The animals in M1 group compared with FM3/M3, F1 compared with M3, and ST compared with FM1/FM3/M3/PM3 consumed a larger amount of feed ( p = 0.00001). The animals in F1 group compared with FM3/M1/M3/PM3, FM1 compared with FM3, and ST compared with FM3/M1/M3/PM3 eliminated lower volume of excreta ( p = 0.00001). The results show that the association between F and M potentiates the effects, indicating a synergistic action of these two drugs, and FM1 is the best protocol due to early negativity in the animals, lower concentrations of the drugs, lower risk of toxicity and stress, and less alterations in clinical parameters. [ABSTRACT FROM AUTHOR]

Published

2017

25. Giardiasis and Subsequent Irritable Bowel Syndrome: A Longitudinal Cohort Study Using Health Insurance Data.

Author

Nakao, Jolene H., Collier, Sarah A., and Gargano, Julia W.

Subjects

*GIARDIASIS, *IRRITABLE colon, *HEALTH insurance, *GIARDIASIS treatment, *PATHOLOGICAL physiology, *ANXIETY, *DIAGNOSIS, *DATABASES, *EPIDEMICS, *LONGITUDINAL method, *DISEASE incidence, *PROPORTIONAL hazards models, *DISEASE complications

Abstract

Background: Giardia intestinalis is the most commonly reported human intestinal parasite in the United States. Increased incidence of chronic gastrointestinal complaints has been reported after some giardiasis outbreaks. We examined the relationship between giardiasis diagnosis and irritable bowel syndrome (IBS) diagnosis.Methods: We used the 2006-2010 MarketScan commercial insurance database. Persons with at least 1 giardiasis diagnosis were individually matched on age group, sex, and enrollment length in months to 5 persons without a giardiasis diagnosis. Persons diagnosed with IBS before the date of study entry were excluded. We calculated crude incidence rates (IRs) and developed Cox proportional hazards models.Results: The matched cohort included 3935 persons with giardiasis and 19663 persons without giardiasis. One-year incidence of IBS was higher in persons with giardiasis (IR = 37.7/1000 person-years vs 4.4/1000 person-years). The unadjusted hazard ratio was 4.8 (95% confidence interval [CI] = 3.6-6.4), attenuated slightly to 3.9 (95% CI = 2.9-5.4) after adjusting for anxiety, depression, and healthcare utilization.Conclusions: In a large insurance database, individuals diagnosed with giardiasis were more likely to have a subsequent IBS diagnosis, despite accounting for confounders. Future research on risk factors for IBS among giardiasis patients and the pathophysiology of postinfectious IBS is needed. [ABSTRACT FROM AUTHOR]

Published

2017

26. Efficacy of nitazoxanide to treat natural Giardia infections in dogs.

Author

Moron-Soto, Mario, Gutierrez, Lilia, Sumano, Héctor, Tapia, Graciela, and Alcala-Canto, Yazmin

Subjects

*DRUG efficacy, *DRUG side effects, *VETERINARY medicine, *GIARDIASIS treatment, *VETERINARY therapeutics, *DOG diseases

Abstract

Background: Giardia parasites cause gastrointestinal disease in humans, dogs, and many other animals worldwide. The treatment of dogs for giardiasis requires further investigation to ascertain levels of drug efficacy and the possibility of adverse side effects. Nitazoxanide (NTZ) has shown good clinical anti-Giardia activity in humans, yet it has not been evaluated for the treatment of giardiasis in dogs. Methods: Thirty-five dogs, naturally infected with Giardia were divided into five groups (n = 7): dogs in group NTZ1, NTZ2, and NTZ3 were treated with a single oral dose of 37.5 mg/kg, 75 mg/kg, and 150 mg/kg, respectively, of NTZ on days 0 and 14. The fourth group was treated with a commercially available regimen that includes a combination of pyrantel, praziquantel, and febantel (FEB) administered orally for three consecutive days. Additionally, an untreated control group was established. Giardia cysts from the stool of each dog were quantified on days -3, 0, 5, 7, 9, 11, 14, 18, 25, and 28. Biochemical parameters were evaluated in all dogs, before the first treatment and after concluding the experiment. Results: Shedding of Giardia cysts was reduced in all treated groups when compared to untreated controls (P < 0.01). However, NTZ2, NTZ3, and FEB had a lower risk during the study. Furthermore, NTZ was also effective against another protozoan, Cryptosporidium spp. at doses of 75 mg/kg and 150 mg/kg, in contrast to the combination of febantel + pyrantel + praziquantel. Biochemical parameters of treated animals, namely, aspartate transaminase and alanine transaminase enzymes, remained within physiological ranges. Conclusions: Based on these results, the implementation of NTZ as a treatment for giardiasis in dogs is proposed. The administration of a single dose is an important advantage of NTZ because it reduces workload, particularly in animals placed in shelters and kennels, where handling of large numbers of animals is required, and personnel is frequently scarce. [ABSTRACT FROM AUTHOR]

Published

2017

27. Identification and Validation of Small-Gatekeeper Kinases as Drug Targets in Giardia lamblia.

Author

Hennessey, Kelly M., Smith, Tess R., Xu, Jennifer W., Alas, Germain C. M., Ojo, Kayode K., Merritt, Ethan A., and Paredez, Alexander R.

Subjects

*GIARDIASIS treatment, *DRUG target, *KINASES, *PROTOZOA genetics, *KINASE inhibitors, *GIARDIA lamblia

Abstract

Giardiasis is widely acknowledged to be a neglected disease in need of new therapeutics to address toxicity and resistance issues associated with the limited available treatment options. We examined seven protein kinases in the Giardia lamblia genome that are predicted to share an unusual structural feature in their active site. This feature, an expanded active site pocket resulting from an atypically small gatekeeper residue, confers sensitivity to “bumped” kinase inhibitors (BKIs), a class of compounds that has previously shown good pharmacological properties and minimal toxicity. An initial phenotypic screen for biological activity using a subset of an in-house BKI library found that 5 of the 36 compounds tested reduced trophozoite growth by at least 50% at a concentration of 5 μM. The cellular localization and the relative expression levels of the seven protein kinases of interest were determined after endogenously tagging the kinases. Essentiality of these kinases for parasite growth and infectivity were evaluated genetically using morpholino knockdown of protein expression to establish those that could be attractive targets for drug design. Two of the kinases were critical for trophozoite growth and attachment. Therefore, recombinant enzymes were expressed, purified and screened against a BKI library of >400 compounds in thermal stability assays in order to identify high affinity compounds. Compounds with substantial thermal stabilization effects on recombinant protein were shown to have good inhibition of cell growth in wild-type G. lamblia and metronidazole-resistant strains of G. lamblia. Our data suggest that BKIs are a promising starting point for the development of new anti-giardiasis therapeutics that do not overlap in mechanism with current drugs. [ABSTRACT FROM AUTHOR]

Published

2016

28. The efficacy of chloroquine treatment of Giardia duodenalis infection in calves.

Author

Gultekin, M., Ural, K., Aysul, N., Ayan, A., Balikci, C., and Akyildiz, G.

Subjects

CALF disease treatment, GIARDIASIS treatment, CHLOROQUINE, POLYMERASE chain reaction, CYSTS (Pathology), THERAPEUTICS

Abstract

Copyright of Vlaams Diergeneeskundig Tijdschrift is the property of Ghent University, Faculty of Veterinary Medicine and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2016

29. Combination therapy in the management of giardiasis: What laboratory and clinical studies tell us, so far.

Author

Escobedo, Angel A., Lalle, Marco, Hrastnik, Nana I., Rodríguez-Morales, Alfonso J., Castro-Sánchez, Enrique, Cimerman, Sérgio, Almirall, Pedro, and Jones, Jony

Subjects

*GIARDIASIS treatment, *COMBINATION drug therapy, *DRUG tolerance, *CLINICAL trials, *ALBENDAZOLE, *THERAPEUTICS

Abstract

Treatment failures in patients suffering from giardiasis are not uncommon feature. The most frequent approach in these cases is to treat these patients with longer repeated courses and/or higher doses of the primary therapy, or using drugs from a different class to avoid potential cross-resistance. However, a higher rate of adverse events may limit this strategy. In this context, combination therapy (CT) is emerging as a valuable option against refractory giardiasis. In the attempt to evaluate the benefits of CT, a number of experimental studies, clinical series, and randomized clinical trials (RCTs), as well as several veterinary studies have been performed, with varying results. Here, we present a critical analysis of the available information regarding CT for the treatment of Giardia infection, as well as the authors’ opinion with respect to its use. RCTs of combination therapy are limited and the optimal combinations and administration strategies need yet to be clarified. Analyses of the cost-effectiveness and RCTs of CTs for Giardia infection are required to assess the role of these drugs for the control of giardiasis, mainly in the case of treatment failures linked to suspected drug tolerance are the case. [ABSTRACT FROM AUTHOR]

Published

2016

30. Deconjugated Bile Salts Produced by Extracellular Bile-Salt Hydrolase-Like Activities from the Probiotic Lactobacillus johnsonii La1 Inhibit Giardia duodenalis In vitro Growth.

Author

Travers, Marie-Agnès, Sow, Cissé, Zirah, Séverine, Deregnaucourt, Christiane, Chaouch, Soraya, Queiroz, Rayner M. L., Charneau, Sébastien, Allain, Thibault, Florent, Isabelle, and Grellier, Philippe

Subjects

GIARDIASIS treatment, PROBIOTICS, PARASITIC protozoa

Abstract

Giardiasis, currently considered a neglected disease, is caused by the intestinal protozoan parasite Giardia duodenalis and is widely spread in human as well as domestic and wild animals. The lack of appropriate medications and the spread of resistant parasite strains urgently call for the development of novel therapeutic strategies. Host microbiota or certain probiotic strains have the capacity to provide some protection against giardiasis. By combining biological and biochemical approaches, we have been able to decipher a molecular mechanism used by the probiotic strain Lactobacillus johnsonii La1 to prevent Giardia growth in vitro. We provide evidence that the supernatant of this strain contains active principle(s) not directly toxic to Giardia but able to convert non-toxic components of bile into components highly toxic to Giardia. By using bile acid profiling, these components were identified as deconjugated bile-salts. A bacterial bile-salt-hydrolase of commercial origin was able to mimic the properties of the supernatant. Mass spectrometric analysis of the bacterial supernatant identified two of the three bile-salt-hydrolases encoded in the genome of this probiotic strain. These observations document a possiblemechanismby which L. johnsonii La1, by secreting, or releasing BSH-like activity(ies) in the vicinity of replicating Giardia in an environment where bile is present and abundant, can fight this parasite. This discovery has both fundamental and applied outcomes to fight giardiasis, based on local delivery of deconjugated bile salts, enzyme deconjugation of bile components, or natural or recombinant probiotic strains that secrete or release such deconjugating activities in a compartment where both bile salts and Giardia are present. [ABSTRACT FROM AUTHOR]

Published

2016

31. Occurrence and multilocus genotyping of Giardia intestinalis assemblage C and D in farmed raccoon dogs, Nyctereutes procyonoides, in China.

Author

Xiao-Xuan Zhang, Wen-Bin Zheng, Jian-Gang Ma, Qiu-Xia Yao, Yang Zou, Cai-Jia Bubu, Quan Zhao, and Xing-Quan Zhu

Subjects

*GIARDIA lamblia, *GIARDIASIS treatment, *RACCOON, *GENOTYPES, *NUCLEOTIDE sequence, *DISEASES

Abstract

Background: Giardia intestinalis, the only causative agent of human giardiasis, can infect a wide range of animals. As no information concerning the prevalence and genotyping of G. intestinalis in raccoon dogs in China is available, examination of 305 faecal samples from raccoon dogs in Jilin Province (n = 110), Heilongjiang Province (n = 40), Liaoning Province (n = 72), Hebei Province (n = 54) and Shandong Province (n = 29) was conducted to estimate the prevalence of G. intestinalis in raccoon dogs in northern China and identify their genotypes using a genetic approach. Findings: Of 305 faecal samples from farmed raccoon dogs, 22 (7.21 %) were detected G. intestinalis-positive by nested PCR amplification of the triosephosphate isomerase (tpi) gene. The prevalence of G. intestinalis was strongly related to the region and season of sampling. All 22 samples were analysed at the tpi, the glutamate dehydrogenase (gdh) and the beta giardin (bg) gene loci, showing 13, 3, 2 subtypes, respectively. The results also demonstrated that two raccoon dogs harboured mixed infections of assemblage C and assemblage D (or mixed C/D), whereas only assemblage C was detected in the remaining 20 samples. Moreover, five new multilocus genotypes, named as MLGs C1-C5, were observed in the assemblage C in the present study. Conclusions: This is the first report of G. intestinalis infection in raccoon dogs in China. DNA sequence analysis of the tpi, gdh and bg gene indicated that 13, 3, 2 subtypes were found at these loci, respectively. Furthermore, this is also the first report of five new multilocus genotypes (MLGs C1-C5) in farmed raccoon dogs, which provides baseline data for further studies of the distribution of G. duodenalis in different hosts. [ABSTRACT FROM AUTHOR]

Published

2016

32. Molecular Characterization of Giardia lamblia: First Report of Assemblage B in Human Isolates from Rio de Janeiro (Brazil).

Author

Faria, Clarissa Perez, Zanini, Graziela Maria, Dias, Gisele Silva, da Silva, Sidnei, and Sousa, Maria do Céu

Subjects

*GIARDIASIS treatment, *DISEASE prevalence, *GIARDIA lamblia, *MOLECULAR epidemiology

Abstract

Background: Despite the high prevalence of giardiasis, the genetic characterization of Giardia lamblia has been poorly documented in Brazil and molecular epidemiology research has only been conducted in the last few years. The aim of this study was to determine the prevalence of different G. lamblia assemblages and detect mixed infections among patients with giardiasis. Methods and Principal Findings: The cross-section survey was conducted among patients attending the FIOCRUZ in Rio de Janeiro. In order to discriminate the genetic assemblages/sub-assemblages, G. lamblia isolates were characterized by PCR-RFLP and qPCR using four loci genes (bg, gdh, tpi and orfC4). Of the 65 positive samples, 41 (63.1%) were successfully amplified by nested-PCR of bg and gdh genes. Among them, 16 were typed as sub-assemblage AII, 7 as BIII, 4 as BIV and 8 as a mixture of BIII and BIV. After the analysis by qPCR assay, a total of 55 (84.6%) samples were amplified using at least one locus: bg gene was amplified in 38 (58.5%) samples, gdh in 41 (63.1%), tpi in 39 (60%), and orfC4 in 39 (60%). Multilocus genotyping results showed that 29 (52.7%) samples belonged to Assemblage A and 26 (47.3%) samples belonged to Assemblage B. In 2011 and 2012, 20 (74.1%) samples belonged to Assemblage A and 7 (25.9%) belonged to Assemblage B. In subsequent years (2013–2015) there was a predominance of Assemblage B, 19 (67.9%) versus 9 (32.1%) Assemblage A. Conclusions: This is the first time that Assemblage B of G. lamblia was reported in human clinical samples from Rio de Janeiro (Brazil) and is the first report about genetic characterization using four genes. The qPCR assemblage-specific showed no mixed infections by Assemblages A and B. A switch in genetic profile over the years was observed, firstly predominance of Assemblage A and lastly of Assemblage B. [ABSTRACT FROM AUTHOR]

Published

2016

33. Spatial and Molecular Epidemiology of Giardia intestinalis Deep in the Amazon, Brazil.

Author

Coronato Nunes, Beatriz, Pavan, Márcio G., Jaeger, Lauren H., Monteiro, Kerla J. L., Xavier, Samanta C. C., Monteiro, Fernando A., Bóia, Márcio N., and Carvalho-Costa, Filipe A.

Subjects

*GIARDIA lamblia, *GIARDIASIS treatment, *GIARDIASIS, *MOLECULAR epidemiology, *HELMINTHS, *SOIL microbiology, *DIAGNOSIS, *INFECTIOUS disease transmission

Abstract

Background: Current control policies for intestinal parasitosis focuses on soil-transmitted helminths, being ineffective against Giardia intestinalis, a highly prevalent protozoon that impacts children’s nutritional status in developing countries. The objective of this study was to explore spatial and molecular epidemiology of Giardia intestinalis in children of Amerindian descent in the Brazilian Amazon. Methodology/Principal Findings: A cross sectional survey was performed in the Brazilian Amazon with 433 children aged 1 to 14 years. Fecal samples were processed through parasitological techniques and molecular characterization. Prevalence of G. intestinalis infection was 16.9% (73/433), reaching 22.2% (35/158) among children aged 2–5 years, and a wide distribution throughout the city with some hot spots. Positivity-rate was similar among children living in distinct socioeconomic strata (48/280 [17.1%] and 19/116 [16.4%] below and above the poverty line, respectively). Sequencing of the β-giardin gene revealed 52.2% (n = 12) of assemblage A and 47.8% (n = 11) of assemblage B with high haplotype diversity for the latter. The isolates clustered into two well-supported G. intestinalis clades. A total of 38 haplotypes were obtained, with the following subassemblages distribution: 5.3% (n = 2) AII, 26.3% (n = 10) AIII, 7.9% (n = 3) BIII, and 60.5% (n = 23) new B genotypes not previously described. Conclusions/Significance: Giardia intestinalis infection presents a high prevalence rate among Amerindian descended children living in Santa Isabel do Rio Negro/Amazon. The wide distribution observed in a small city suggests the presence of multiple sources of infection, which could be related to environmental contamination with feces, possibly of human and animal origin, highlighting the need of improving sanitation, safe water supply and access to diagnosis and adequate treatment of infections. [ABSTRACT FROM AUTHOR]

Published

2016

34. Establishment of Canine-Derived Giardia duodenalis Isolates in Culture.

Author

Tysnes, Kristoffer R. and Robertson, Lucy J.

Subjects

TROPHOZOITES, PARASITES, GIARDIASIS treatment, ZOONOSES, DOG diseases

Abstract

Researchers continue to rely on axenic cultivation of Giardia duodenalis trophozoites in vitro to study the life cycle and host-parasite interactions of G. duodenalis and to develop vaccines and drugs to prevent and treat giardiasis. The majority of in vitro studies of G. duodenalis have used a small subset of isolates, mostly of assemblage A, and these isolates are usually originally isolated from humans. The most commonly used isolate for lab studies is known as WB. Canine giardiasis is a disease of veterinary importance, but it may also be of relevance in zoonotic transmission. Few G. duodenalis isolates from dogs have been adapted to in vitro culture, probably because the methods used are not suitable for the canine-specific genotypes that tend to dominate in most dog populations. In the current study, an experimental approach to cultivating canine-derived isolates of G. duodenalis was attempted by modification of the standard protocol based on physiological differences between the human and canine digestive system. An adapted method is described for improving the rate of in vitro excystation of cysts isolated from dogs by chemically weakening the cyst wall. A new canine-derived assemblage A G. duodenalis isolate was successfully adapted to axenic culture by using this method; the dog apparently had a mixed infection of assemblages A and D, but the assemblage A successfully outcompeted the assemblage D under conditions of in vitro culture. Based on the results, reasons regarding why humans do not seem to be suitable hosts for G. duodenalis in assemblages C and D are discussed. [ABSTRACT FROM AUTHOR]

Published

2016

35. The efficacy of chloroquine treatment against naturally occuring Giardia duodenalis infection in lambs.

Author

Karademir, Umit, Ural, Kerem, Aysul, Nuran, Ayan, Adnan, Toplu, Songul, Ortlek, Onur, Balıkci, Canberk, Kunyeli, Ahmet, and Erdogan, Hasan

Subjects

*GIARDIASIS treatment, *CHLOROQUINE, *LAMBS, *SHEEP diseases, *DRUG efficacy, *GIARDIASIS, *TROPHOZOITES, *DIAGNOSIS, *THERAPEUTICS

Abstract

Objective. The aim of the present study was to determine the efficacy of Chloroquine (Cq), an antimalarial medicine, administered at a dose of 2.5 mg/kg, orally, during 5 consecutive days, in Sakiz and Merino lambs naturally infected with Giardia duodenalis. Materials and methods. To this extent weaned 10 weeks of aged lambs were enrolled and randomly assigned into two groups based on treatment (group C, n=18 lambs treated with Cq) and placebo (group P, n=8 untreated control animals). Diagnosis was based on detection of trophozoit and/or cysts on fecal flotation. Cyst count per gram feces (days 0, 3, 7 and 10) was analyzed among groups. Results. During the trial, regarding the efficacy of Cq on days 3., 7., and 10. There was significant (p<0.01) reduction in cyst excretion; whereas evaluation of mean geometric cyst excretion revealed 100% reduction. Conclusions. There was a very high (100%) reduction in cyst excretion in the Cq treatment group compared to the positive untreated control group on days 3, 7 and 10, resulting in a significant (p<0.001) reduction, making Cq, safety, and thus highly effective treatment option of lambs with naturally occuring giardiasis. [ABSTRACT FROM AUTHOR]

Published

2016

36. Proton pump inhibitors drastically modify triosephosphate isomerase from Giardia lamblia at functional and structural levels, providing molecular leads in the design of new antigiardiasic drugs.

Author

García-Torres, Itzhel, de la Mora-de la Mora, Ignacio, Marcial-Quino, Jaime, Gómez-Manzo, Saúl, Vanoye-Carlo, América, Navarrete-Vázquez, Gabriel, Colín-Lozano, Blanca, Gutiérrez-Castrellón, Pedro, Sierra-Palacios, Edgar, López-Velázquez, Gabriel, and Enríquez-Flores, Sergio

Subjects

*PROTON pump inhibitors, *TRIOSE-phosphate isomerase, *GIARDIA lamblia, *HYDROPHOBIC surfaces, *GIARDIASIS treatment, *OMEPRAZOLE

Abstract

Background Proton pump inhibitors (PPIs) are extensively used in clinical practice because of their effectiveness and safety. Omeprazole is one of the best-selling drugs worldwide and, with other PPIs, has been proposed to be potential drugs for the treatment of several diseases. We demonstrated that omeprazole shows cytotoxic effects in Giardia and concomitantly inactivates giardial triosephosphate isomerase (GlTIM). Therefore, we evaluated the efficiency of commercially available PPIs to inactivate this enzyme. Methods We assayed the effect of PPIs on the GlTIM WT, single Cys mutants, and the human counterpart, following enzyme activity, thermal stability, exposure of hydrophobic regions, and susceptibility to limited proteolysis. Results PPIs efficiently inactivated GlTIM; however, rabeprazole was the best inactivating drug and was nearly ten times more effective. The mechanism of inactivation by PPIs was through the modification of the Cys 222 residue. Moreover, there are important changes at the structural level, the thermal stability of inactivated-GlTIM was drastically diminished and the structural rigidity was lost, as observed by the exposure of hydrophobic regions and their susceptibility to limited proteolysis. Conclusions Our results demonstrate that rabeprazole is the most potent PPI for GlTIM inactivation and that all PPIs tested have substantial abilities to alter GITIM at the structural level, causing serious damage. General significance. This is the first report demonstrating the effectiveness of commercial PPIs on a glycolytic parasitic enzyme, with structural features well known. This study is a step forward in the use and understanding the implicated mechanisms of new antigiardiasic drugs safe in humans. [ABSTRACT FROM AUTHOR]

Published

2016

37. An update on handling patients with chronic enteropathies: When it comes to chronic gastrointestinal cases, it's time to throw out your outdated terms and diagnoses.

Author

Wooten, Sarah

Subjects

INTESTINAL disease diagnosis, INTESTINAL disease treatment, ANIMAL diseases, PETS, GIARDIASIS treatment, INFLAMMATORY bowel diseases, VITAMIN B12

Abstract

The article presents an update on handling patients with chronic enteropathies by STOP IT. Fetch dvm3360 conference speaker Craig Ruaux. Topics discussed include diagnosis of inflammatory bowel diseases (IBD) or idiopathic inflammatory bowel disease (IIBD), serum cobalamin and folate concentrations to help in determining the extent of the disease and treatment of giardiasis using protein diet over a hydrolyzed diet.

Published

2017

38. Giardia duodenalis mouse model for the development of novel antigiardial agents.

Author

Abraham, Rebecca J., O'Dea, Mark, Rusdi, Bertha, Page, Stephen W., O'Handley, Ryan, and Abraham, Sam

Subjects

*GIARDIASIS treatment, *DRUG development, *DRUG efficacy, *ANTIPROTOZOAL agents, *ANIMAL models in research, *THERAPEUTICS

Abstract

This study describes a neonatal mouse model of Giardia infection for development of novel antigiardials. Mice were infected with the axenically cultured Assemblage A BAH2c2 strain, with 10 5 trophozoites per animal recovered. This model proved to be robust and consistent for use in preliminary drug efficacy trials and drug development. [ABSTRACT FROM AUTHOR]

Published

2018

39. Terminalia ferdinandiana extracts as inhibitors of Giardia duodenalis proliferation: a new treatment for giardiasis.

Author

Rayan, P., Matthews, B., McDonnell, P., and Cock, I.

Subjects

*GIARDIASIS treatment, *TERMINALIA, *INTESTINAL parasites, *GIARDIA, *BIOLOGICAL assay

Abstract

Giardisis is a debilitating disease caused by gastrointestinal parasites of the genus Giardia. High-antioxidant T. ferdinandiana fruit extracts were investigated for the ability to block Giardia duodenalis growth. Methanolic and aqueous extracts had the most potent growth inhibitory activity (IC50 values of approximately 700 and 140 μg/ml, respectively). Ethyl acetate and chloroform extracts also inhibited G. duodenalis growth, albeit with lower potency. The hexane extract was completely devoid of G. duodenalis growth inhibitory activity. All extracts were nontoxic in the Artemia fransiscana bioassay. Nontargeted HPLC-quadrupole time-of-flight (QTOF) mass spectroscopy (with screening against three compound databases) putatively identified 17 compounds in all of the inhibitory extracts but not in the inactive hexane extract. The low toxicity of the Terminalia ferdinandiana fruit extracts and their potent G. duodenalis growth inhibitory bioactivity indicate their potential as medicinal agents in the treatment and prevention of this disease. [ABSTRACT FROM AUTHOR]

Published

2015

40. Giardia fatty acyl-CoA synthetases as potential drug targets.

Author

Fengguang Guo, Ortega-Pierres, Guadalupe, Argüello-García, Raúl, Haili Zhang, Guan Zhu, Sriramulu, Dinesh, and Podust, Larissa M.

Subjects

GIARDIASIS treatment, ACYL coenzyme A, DRUG target

Abstract

Giardiasis caused by Giardia intestinalis (syn. G. lamblia, G. duodenalis) is one of the leading causes of diarrheal parasitic diseases worldwide. Although limited drugs to treat giardiasis are available, there are concerns regarding toxicity in some patients and the emerging drug resistance. By data-mining genome sequences, we observed that G. intestinalis is incapable of synthesizing fatty acids (FA) de novo. However, this parasite has five long-chain fatty acyl-CoA synthetases (GiACS1 to GiACS5) to activate FA scavenged from the host. ACS is an essential enzyme because FA need to be activated to form acyl-CoA thioesters before they can enter subsequent metabolism. In the present study, we performed experiments to explore whether some GiACS enzymes could serve as drug targets in Giardia. Based on the high-throughput datasets and protein modeling analyses, we initially studied the GiACS1 and GiACS2, because genes encoding these two enzymes were found to be more consistently expressed in varied parasite life cycle stages and when interacting with host cells based on previously reported transcriptome data. These two proteins were cloned and expressed as recombinant proteins. Biochemical analysis revealed that both had apparent substrate preference toward palmitic acid (C16:0) and myristic acid (C14:0), and allosteric or Michaelis-Menten kinetics on palmitic acid or ATP. The ACS inhibitor triacsin C inhibited the activity of both enzymes (IC50 = 1.56 μM, Ki = 0.18 μM for GiACS1, and IC50 2.28 μM, Ki = 0.23 μM for GiACS2, respectively) and the growth of G. intestinalis in vitro (IC50 = 0.8 μM). As expected from giardial evolutionary characteristics, both GiACSs displayed differences in overall folding structure as compared with their human counterparts. These observations support the notion that some of the GiACS enzymes may be explored as drug targets in this parasite. [ABSTRACT FROM AUTHOR]

Published

2015

41. Antigiardial activity of novel triazolyl-quinolone-based chalcone derivatives: when oxygen makes the difference.

Author

Bahadur, Vijay, Mastronicola, Daniela, Singh, Amit K., Tiwari, Hemandra K., Pucillo, Leopoldo P., Sarti, Paolo, Singh, Brajendra K., and Giuffrè, Alessandro

Subjects

GIARDIASIS treatment, QUINOLONE antibacterial agents, CHALCONE, ANTIPARASITIC agents, METRONIDAZOLE, ANAEROBIC protozoa, THERAPEUTICS

Abstract

Giardiasis is a common diarrheal disease worldwide caused by the protozoan parasite Giardia intestinalis. It is urgent to develop novel drugs to treat giardiasis, due to increasing clinical resistance to the gold standard drug metronidazole (MTZ). New potential antiparasitic compounds are usually tested for their killing efficacy against G. intestinalis under anaerobic conditions, in which MTZ is maximally effective. On the other hand, though commonly regarded as an 'anaerobic pathogen,' G. intestinalis is exposed to relatively high O2 levels in vivo, living attached to the mucosa of the proximal small intestine. It is thus important to test the effect of O2 when searching for novel potential antigiardial agents, as outlined in a previous study [Bahadur et al. (2014) Antimicrob. Agents Chemother. 58, 543]. Here, 45 novel chalcone derivatives with triazolyl-quinolone scaffold were synthesized, purified, and characterized by high resolution mass spectrometry, 1H and 13C nuclear magnetic resonance and infrared spectroscopy. Efficacy of the compounds against G. intestinalis trophozoites was tested under both anaerobic and microaerobic conditions, and selectivity was assessed in a counter-screen on human epithelial colorectal adenocarcinoma cells. MTZ was used as a positive control in the assays. All the tested compounds proved to be more effective against the parasite in the presence of O2, with the exception of MTZ that was less effective. Under anaerobiosis eighteen compounds were found to be as effective as MTZ or more (up to three to fourfold); the same compounds proved to be up to >100- fold more effective than MTZ under microaerobic conditions. Four of them represent potential candidates for the design of novel antigiardial drugs, being highly selective against Giardia trophozoites. This study further underlines the importance of taking O2 into account when testing novel potential antigiardial compounds. [ABSTRACT FROM AUTHOR]

Published

2015

42. The effect of metronidazole on the cell cycle and DNA in metronidazole-susceptible and -resistant Giardia cell lines.

Author

Uzlikova, Magdalena and Nohynkova, Eva

Subjects

*GIARDIASIS treatment, *METRONIDAZOLE, *DNA damage, *CELL cycle, *PHOSPHORYLATION, *CELL death, *FLOW cytometry, *THERAPEUTICS

Abstract

Metronidazole (MTZ) is used as the drug of choice to treat Giardia infections. It is believed that the prodrug is transformed intracellularly into toxic intermediates that interact with cellular components, leading to cell death. The present study aimed to describe the effects of MTZ treatment on DNA and cell cycle progression in MTZ-sensitive and in vitro -derived MTZ-resistant cell lines. Detection of the phosphorylated form of histone H2A in cell nuclei together with electrophoresis of genomic DNA, flow cytometry analysis and incubation of cells with other drugs (albendazole or neomycin) demonstrated that DNA damage in MTZ-treated cells is clearly conditioned by the presence of this drug. The flow cytometry analysis and a BrdU labeling assay showed that the sublethal drug concentration affects the replication phase of the cell cycle. Cells incubated with lethal drug concentration exhibit unchanged DNA profile, only about 50% of cells are positive for γH2A and lose an ability to attach to a surface after few hours of incubation. It is likely that the early reaction of cells to lethal concentration of MTZ is not primarily initiated by the reaction to DNA damage but rather by the immediate interaction of MTZ with biomolecules where activated MTZ is generated. Interestingly, in MTZ-resistant lines incubated in the presence of the drug, about 40% of cells remain permanently positive for γH2A without any effects on the cell cycle progression suggesting that DNA damage caused by MTZ treatment persists in these cells. Accelerated mutagenesis caused by MTZ-induced DNA damage may therefore be a new factor contributing to the development of natural resistance. [ABSTRACT FROM AUTHOR]

Published

2014

43. Ginger and Cinnamon: Can This Household Remedy Treat Giardiasis? Parasitological and Histopathological Studies.

Author

MAHMOUD, Abeer, ATTIA, Rasha, SAID, Safaa, and IBRAHEIM, Zedan

Subjects

*GINGER, *CINNAMON, *GIARDIASIS treatment, *GIARDIA lamblia, *METRONIDAZOLE, *HISTOPATHOLOGY, *THERAPEUTICS

Abstract

Background: Giardia lamblia is one of the most common protozoal infections in human especially children. Metronidazol (MTZ) is the drug of choice for treatment of giardiasis; its chemical composition possesses major threats and is becoming less sensitive. This study aimed to search for natural extracts alternative to MTZ. Methods: In-vivo effects of dichloromethane extracts of ginger and cinnamon in doses of 10 and 20 mg/kg/day separately were studied on 30 experimentally infected albino rats divided into 6 groups (5 rats each). Plant extracts were started on the 6th day post infection for 7 successive days. The study was evaluated by fecal cyst and intestinal trophozoite counts, histopathology, scanning and transmission electron microscopic examinations of the small intestinal mucosa. Results: Ginger and cinnamon caused reduction of fecal cyst and trophozoites counts. Histopathology, scanning electron microscopy (SEM) and transmission electron microscopy (TEM) after exposure to each extract revealed evident improvement of intestinal mucosal damage produced by G. lamblia infection and direct structural injury to the trophozoites. However, these results were more obvious after exposure to cinnamon extracts. Conclusion: We confirmed the potential therapeutic effects of ginger and cinnamon extracts on G. lamblia infection in albino rats as a promising alternative therapy to the commonly used antigiardial drugs. [ABSTRACT FROM AUTHOR]

Published

2014

44. Efficacy of 5-Nitroimidazoles for the Treatment of Giardiasis: A Systematic Review of Randomized Controlled Trials.

Author

Pasupuleti, Vinay, Escobedo, Angel Arturo, Deshpande, Abhishek, Thota, Priyaleela, Roman, Yuani, and Hernandez, Adrian V.

Subjects

*NITROIMIDAZOLES, *DRUG efficacy, *GIARDIASIS treatment, *RANDOMIZED controlled trials, *META-analysis

Abstract

Background: Giardiasis is one of the most common causes of diarrheal disease worldwide and 5-nitroimidazoles (5-NI) are the most commonly prescribed drugs for the treatment of giardiasis. We evaluated the efficacy of 5-nitroimidazoles (5-NI) in the treatment of giardiasis in a systematic review of randomized controlled trials (RCTs). Methodology/Principal Findings: We conducted a comprehensive literature search in PubMed-Medline, Scopus, Web of Science and Cochrane Library for RCTs evaluating the efficacy of 5-NI vs. control (placebo or active treatment) on parasitological cure in patients with parasitologically-demonstrated giardiasis. The search was performed in May 2013 with no language restriction by two authors independently. The efficacy outcome was parasitological cure, and harmful outcomes were abdominal pain, bitter or metallic taste, and headache. We included 30 RCTs (n = 3,930). There was a significant and slightly higher response rate with 5-NI in giardiasis treatment (RR 1.06, 95%CI 1.02–1.11, p = 0.005). There was high heterogeneity among studies (I2 = 72%). The response rates for metronidazole, tinidazole and secnidazole were similar (RR 1.05, 95%CI 1.01–1.09, p = 0.01; RR 1.32 95%CI 1.10–1.59, p = 0.003; and RR 1.18 95%CI 0.93–1.449, p = 0.18, respectively). On subgroup analyses, the response rates did not vary substantially and high heterogeneity persisted (I2 = 57%–80%). Harmful outcomes were uncommon, and 5-NIs were associated with lower risk of abdominal pain, and higher risk of both bitter or metallic taste and headache. Conclusions: Studies investigating the efficacy of 5-NI in giardiasis treatment are highly heterogeneous. 5-NIs have a slightly better efficacy and worse profile for mild harmful outcomes in the treatment of giardiasis in comparison to controls. Larger high quality RCTs are needed to further assess efficacy and safety profiles of 5-NI. [ABSTRACT FROM AUTHOR]

Published

2014

45. High Sensitivity of Giardia duodenalis to Tetrahydrolipstatin (Orlistat) In Vitro.

Author

Hahn, Juliane, Seeber, Frank, Kolodziej, Herbert, Ignatius, Ralf, Laue, Michael, Aebischer, Toni, and Klotz, Christian

Subjects

*GIARDIASIS treatment, *GIARDIA, *ORLISTAT, *ETIOLOGY of diseases, *GASTROINTESTINAL diseases, *PHARMACEUTICAL research, *ALTERNATIVE medicine, *IN vitro studies

Abstract

Giardiasis, a gastrointestinal disease caused by Giardia duodenalis, is currently treated mainly with nitroimidazoles, primarily metronidazole (MTZ). Treatment failure rates of up to 20 percent reflect the compelling need for alternative treatment options. Here, we investigated whether orlistat, a drug approved to treat obesity, represents a potential therapeutic agent against giardiasis. We compared the growth inhibitory effects of orlistat and MTZ on a long-term in vitro culture adapted G. duodenalis strain, WB-C6, and on a new isolate, 14-03/F7, from a patient refractory to MTZ treatment using a resazurin assay. The giardiacidal concentration of the drugs and their combined in vitro efficacy was determined by median-effect analysis. Morphological changes after treatment were analysed by light and electron microscopy. Orlistat inhibited the in vitro growth of G. duodenalis at low micromolar concentrations, with isolate 14-03/F7 (IC5024h = 2.8 µM) being more sensitive than WB-C6 (IC5024h = 6.2 µM). The effect was significantly more potent compared to MTZ (IC5024h = 4.3 µM and 11.0 µM, respectively) and led to specific undulated morphological alterations on the parasite surface. The giardiacidal concentration of orlistat was >14 µM for 14-03/F7 and >43 µM for WB-C6, respectively. Importantly, the combination of both drugs revealed no interaction on their inhibitory effects. We demonstrate that orlistat is a potent inhibitor of G. duodenalis growth in vitro and kills parasites at concentrations achievable in the gut by approved treatment regimens for obesity. We therefore propose to investigate orlistat in controlled clinical studies as a new drug in giardiasis. [ABSTRACT FROM AUTHOR]

Published

2013

46. High Sensitivity of Giardia duodenalis to Tetrahydrolipstatin (Orlistat) In Vitro.

Author

Hahn, Juliane, Seeber, Frank, Kolodziej, Herbert, Ignatius, Ralf, Laue, Michael, Aebischer, Toni, and Klotz, Christian

Subjects

GIARDIASIS treatment, GIARDIA, ORLISTAT, ETIOLOGY of diseases, GASTROINTESTINAL diseases, PHARMACEUTICAL research, ALTERNATIVE medicine, IN vitro studies

Abstract

Giardiasis, a gastrointestinal disease caused by Giardia duodenalis, is currently treated mainly with nitroimidazoles, primarily metronidazole (MTZ). Treatment failure rates of up to 20 percent reflect the compelling need for alternative treatment options. Here, we investigated whether orlistat, a drug approved to treat obesity, represents a potential therapeutic agent against giardiasis. We compared the growth inhibitory effects of orlistat and MTZ on a long-term in vitro culture adapted G. duodenalis strain, WB-C6, and on a new isolate, 14-03/F7, from a patient refractory to MTZ treatment using a resazurin assay. The giardiacidal concentration of the drugs and their combined in vitro efficacy was determined by median-effect analysis. Morphological changes after treatment were analysed by light and electron microscopy. Orlistat inhibited the in vitro growth of G. duodenalis at low micromolar concentrations, with isolate 14-03/F7 (IC5024h = 2.8 µM) being more sensitive than WB-C6 (IC5024h = 6.2 µM). The effect was significantly more potent compared to MTZ (IC5024h = 4.3 µM and 11.0 µM, respectively) and led to specific undulated morphological alterations on the parasite surface. The giardiacidal concentration of orlistat was >14 µM for 14-03/F7 and >43 µM for WB-C6, respectively. Importantly, the combination of both drugs revealed no interaction on their inhibitory effects. We demonstrate that orlistat is a potent inhibitor of G. duodenalis growth in vitro and kills parasites at concentrations achievable in the gut by approved treatment regimens for obesity. We therefore propose to investigate orlistat in controlled clinical studies as a new drug in giardiasis. [ABSTRACT FROM AUTHOR]

Published

2013

47. Effects of metronidazole analogues on Giardia lamblia: experimental infection and cell organization

Author

Busatti, Haendel G.N.O., Alves, Ricardo J., Santana-Anjos, Karla G., Gil, Frederico F., Cury, Marcia C., Vannier-Santos, Marcos A., and Gomes, Maria A.

Subjects

*METRONIDAZOLE, *GIARDIASIS treatment, *DRUG side effects, *GIARDIA lamblia, *CELL physiology, *TRANSMISSION electron microscopy, *ULTRASTRUCTURE (Biology), *AUTOPHAGY

Abstract

Abstract: The chemotherapeutic agents used for the treatment of giardiasis are often associated with adverse side effects and are refractory cases, due to the development of resistant parasites. Therefore the search for new drugs is required. We have previously reported the giardicidal effects of metronidazole (MTZ) and its analogues (MTZ-Ms, MTZ-Br, MTZ-N3, and MTZ-I) on the trophozoites of Giardia lamblia. Now we evaluated the activity of some giardicidal MTZ analogues in experimental infections in gerbils and its effects on the morphology and ultrastructural organization of Giardia. The giardicidal activity in experimental infections showed ED50 values significantly lower for MTZ-I and MTZ-Br when compared to MTZ. Transmission electron microscopy was employed to approach the mechanism(s) of action of MTZ analogues upon the protozoan. MTZ analogues were more active than MTZ in changing significantly the morphology and ultrastructure of the parasite. The analogues affected parasite cell vesicle trafficking, autophagy, and triggered differentiation into cysts. These results coupled with the excellent giardicidal activity and lower toxicity demonstrate that these nitroimidazole derivates may be important therapeutic alternatives for combating giardiasis. In addition, our results suggest a therapeutic advantage in obtaining synthetic metronidazole analogues for screening of activities against other infectious agents. [Copyright &y& Elsevier]

Published

2013

48. Enantioseparation of Secnidazole by High-Performance Liquid Chromatography using Amylose-based Stationary Phase.

Author

Nascimento, Ana C., Perna, Rafael F., Cremasco, Marco A., and Santana, Cesar C.

Subjects

*NITROIMIDAZOLES, *SEPARATION (Technology), *HIGH performance liquid chromatography, *AMYLOSE, *AMEBIASIS treatment, *GIARDIASIS treatment, *BACTERIAL vaginitis treatment, *THERMODYNAMICS

Abstract

The secnidazole, a drug used in hepatic amebiasis, giardiasis and bacterial vaginosis, was enantioseparated on a semi-preparative scale by high performance liquid chromatography (HPLC), using chiral stationary phase (CSP) containing amylose tris (3, 5-dimethylphenyl) carbamate on silica gel (Chiralpak® AD). The experiments were carried out under normal phase conditions and the separation method exhibited very high selectivity and resolutions. The chromatographic parameters and the effects of column temperature on the retention time and selectivity were evaluated. Thermodynamic parameters were obtained from van't Hoff plots, and the elution order of the enantiomers was determined by circular dichorism. The enantiomers of secnidazole were separated under overloaded conditions with a good performance. [ABSTRACT FROM AUTHOR]

Published

2012

49. Validity of silver, chitosan, and curcumin nanoparticles as anti- Giardia agents.

Author

Said, D., ElSamad, L., and Gohar, Y.

Subjects

*CHITOSAN, *SILVER nanoparticles, *CURCUMIN, *GIARDIASIS treatment, *ANTIPARASITIC agents

Abstract

This study was carried out to evaluate the anti parasitic potential of silver, chitosan, and curcumin nanoparticles as anti- Giardia agents. Non-treated infected control rats were inoculated with Giardia lamblia cysts in a dose of 2 × 10 cysts/rat. Experimental group was infected then treated with curcumin, curcumin nanoparticles, chitosan, chitosan nanoparticles, and silver nanoparticles as single or combined therapy. The number of Giardia cysts in stools and trophozoites in intestinal sections were detected. Toxicity of nanoparticles was evaluated by comparing hematological and histopathological parameters of the normal control group and treated non-infected control group. The amount of silver was also measured in the liver, kidney, small intestine, lung, and brain of rats treated with silver nanoparticles. The number of the parasites in stool and small intestinal sections decreased in treated infected rats compared with infected non-treated ones. The effect in the single therapy was better with nanoparticles, and the best effect was detected in nano-silver. The combined therapy gave better results than single. Combination between nanoparticles was better than the combination of nano-forms and native chitosan and curcumin. The best effect was detected in combinations of nano-silver and nano -chitosan but with no full eradication. In conclusion, the highest effect and complete cure was gained by combining the three nano-forms. The parasite was successfully eradicated from stool and intestine. None of the treatments exhibited any toxicity. Accumulated silver in different organs was within the safe limits. [ABSTRACT FROM AUTHOR]

Published

2012

50. Giardia lamblia: A new target for miltefosine

Author

Eissa, Maha M. and Amer, Eglal I.

Subjects

*GIARDIA lamblia, *LEISHMANIASIS treatment, *PARASITES, *GIARDIASIS treatment, *INTESTINAL infections, *DISEASE prevalence

Abstract

Abstract: Giardia lamblia, the causative agent of giardiasis, is an intestinal infection with worldwide distribution and high rates of prevalence. Increased resistance of the parasite and the side effects of the reference drugs employed in the treatment of giardiasis make it necessary to seek new therapeutic agents. Therefore, the aim of this study was to examine the activity of hexadecylphosphocholine (miltefosine), a membrane active alkylphospholipid, that is licensed as an antileishmanial agent against giardiasis. The efficacy of miltefosine was evaluated both in vitro and in vivo in Swiss albino mice. Results of the in vitro testing revealed susceptibility of G. lamblia trophozoites to miltefosine with the following effective concentrations: EC50s of between 20 and 40μM, and EC90s of between 20 and 80μM. Immediate total lysis of the organisms was achieved by 100μM. In vivo testing showed that oral administration of miltefosine, in a daily dose regimen course of 20mg/kg for three successive days, to infected mice resulted in total elimination of the parasite from the intestine and amelioration of intestinal pathology. Scanning and transmission electron microscopy studies revealed that miltefosine induced severe morphological alterations to G. lamblia trophozoites, mainly at the level of cell membrane and adhesive disc. In conclusion, we believe that this is the first study highlighting G. lamblia as a possible new target for miltefosine. [Copyright &y& Elsevier]

Published

2012