Your search keyword '"MOUSE diseases"' showing total 20 results

1. Spleen atrophy related immune system changes attributed to infection of Angiostrongylus cantonensis in mouse model.

Author

Liu, Zhen, Wu, Yu, Feng, Ying, Wu, Feng, Liu, Rui-Feng, Wang, Li-Fu, Liang, Jin-Yi, Liu, Jia-Hua, Sun, Xi, and Wu, Zhong-Dao

Subjects

*SPLEEN, *IMMUNE response, *COMMUNICABLE diseases, *MOUSE diseases, *ANGIOSTRONGYLUS cantonensis, *ANIMAL models in research, *DIAGNOSIS

Abstract

The spleen is one of the most important peripheral immune organs, which is frequently affected in infectious diseases. Infectious diseases can induce splenic alterations including splenic atrophy and functional alteration, while splenic atrophy may in turn interferes with recovery of infectious diseases. Angiostrongyliasis is an infectious disease by Angiostrongylus cantonensis ( A. cantonensis), which invade non-permissive hosts, such as humans and mice, to cause severe damage to the central nervous system (CNS) and acute inflammatory response. A. cantonensis infection-induced CNS injury has been confirmed to be due to profound immunopathology derived from peripheral immune components. However, the mechanism of immunopathology remains largely unknown. Here, we found that A. cantonensis invaded non-permissive hosts such as mice in the brain, but not in the other peripheral organs. However, this infection induced severe spleen atrophy. We further recognized that this atrophy is associated with a decrease of total splenocyte number and disruption of splenic structure due to reduced proliferation and increased apoptotosis. These also resulted in deterioration of T cell profile in the periphery with a low CD4/CD8 ratio and B/T cell ratio, and increased ratio of CD4CD25Foxp3 Treg, CD8CD28 T, and CD38T lymphocyte of spleen. Albendazole treatment can alleviate spleen atrophy and set T cell immune reconstitution in some extend. Our data showed that A. cantonensis infection can cause splenic atrophy. These results are suggested to put more emphasis to improve the function of immune system. Meanwhile, infection and treatment model will be useful to evaluate new therapeutic approaches which can prevent or reverse immunosuppression and infectious complications. [ABSTRACT FROM AUTHOR]

Published

2017

2. Effects of Enterococcus faecalis CECT 7121 on Cryptosporidium parvum infection in mice.

Author

Del Coco, Valeria, Sparo, Mónica, Sidoti, Alicia, Santín, Mónica, Basualdo, Juan, and Córdoba, María

Subjects

*ENTEROCOCCUS faecalis, *CRYPTOSPORIDIUM parvum, *MOUSE diseases, *DIARRHEA, *PROBIOTICS

Abstract

Cryptosporidium is an opportunistic protozoan parasite of humans and animals worldwide and causes diarrheal disease that is typically self-limiting in immunocompetent hosts but often life threatening to immunocompromised individuals. However, there is a lack of completely efficient therapy available. Probiotics have attracted the attention as potential antiparasite compounds against protozoa involved in intestinal infections. This study investigated the effects of administration of probiotic Enterococcus faecalis CECT 7121 on Cryptosporidium parvum infection in immunosuppressed mice. Effects on C. parvum infection at the intestinal mucosa were studied and scored at each portion of the gut. It was demonstrated that Ef CECT 7121 interfered with C. parvum infection when both probiotic and parasite were present in the same intestinal location suggesting that Ef CECT 7121 supplementation can alleviate the negative effects of C. parvum infection. [ABSTRACT FROM AUTHOR]

Published

2016

3. Course of induced infection by Eimeria krijgsmannni in immunocompetent and immunodeficient mice.

Author

Ono, Yuina, Matsubayashi, Makoto, Kawaguchi, Hiroaki, Tsujio, Masashi, Mizuno, Masanobu, Tanaka, Tetsuya, Masatani, Tatsunori, Matsui, Toshihiro, and Matsuo, Tomohide

Subjects

*EIMERIA, *PARASITE life cycles, *MOUSE diseases, *IMMUNOCOMPETENT cells, *BIODIVERSITY

Abstract

Recently, we have demonstrated the utility of Eimeria krijgsmanni as a novel mouse eimerian parasite for elucidating the biological diversity. The parasite showed notable infectivity to mice with various levels of immune status and susceptibility to antimicrobial agents including coccidiostat. However, the detailed lifecycle of E. krijgsmanni had not yet been determined and this information was lacking in discussion of previous findings. In the present study, we clarified the morphological characteristics of E. krijgsmanni and its lifecycle in normal mice, and examined the effects in immunodeficient mice and lifecycle stage for challenge infections after the primary inoculation. In immunocompetent mice, the lifecycle consisted of four asexual stages and the sexual sages followed by formation of oocysts during the prepatent periods. Interestingly, the second-generation meronts were detected in all observation periods after the disappearance of the other stages. For the challenge infection of immunodeficient mice, all developmental stages except for the second generation meronts were temporarily vanished. This finding suggests a 'rest' or marked delay in development and a 'restart' of the promotion toward the next generations. The second generation meronts may play an important role in the lifecycle of E. krijgsmanni. [ABSTRACT FROM AUTHOR]

Published

2016

4. Immunomodulatory and antiparasitic effects of garlic extract on Eimeria vermiformis-infected mice.

Author

Khalil, Atef, Yasuda, Masahiro, Farid, Ayman, Desouky, Mohamed, Mohi-Eldin, Mouchira, Haridy, Mohie, and Horii, Yoichiro

Subjects

*MOUSE diseases, *THERAPEUTIC use of garlic, *ANTIPARASITIC agents, *IMMUNOREGULATION, *CYTOKINES, *T cells, *THERAPEUTICS

Abstract

We investigated the immunomodulatory and parasiticidal effects of garlic extract on coccidiosis caused by Eimeria vermiformis infection in male ICR mice. One group received garlic extract daily until the end of the experiment by the oral route from 10 days prior to oral infection with 300 sporulated E. vermiformis oocysts (infected-garlic). The other group served as a control positive with E. vermiformis infection alone (infected-garlic). In the infected-garlic group, garlic extract treatment induced a significant reduction in fecal oocyst output when compared with the infected-garlic group. Histopathological, immunohistochemical, and gene expression analysis for inflammatory cytokines in ileal tissues showed that the garlic extract treatment impaired intracellular development of E. vermiformis during the early stages by increasing the number of intraepithelial CD8 T cells and decreasing IL-10 expression. This induced cell cytotoxicity which was reflected by a decrease in oocyst numbers in the intestinal villi and the feces, indicating anticoccidial effects of the garlic extract. However, further studies to explore the precise mechanism of the observed effects of garlic treatment during Eimeria infection are needed to verify our results. [ABSTRACT FROM AUTHOR]

Published

2015

5. Besnoitia besnoiti infection in cattle and mice: ultrastructural pathology in acute and chronic besnoitiosis.

Author

Langenmayer, M., Gollnick, N., Scharr, J., Schares, G., Herrmann, D., Majzoub-Altweck, M., and Hermanns, W.

Subjects

*BESNOITIOSIS, *CATTLE infections, *CATTLE parasites, *MOUSE diseases, *VETERINARY parasitology, *LIMOUSIN cattle, *DISEASES

Abstract

Current knowledge on bovine besnoitiosis, caused by the emerging apicomplexan pathogen Besnoitia besnoiti, is still fragmentary. So far, studies dealing with ultrastructural pathology focused mainly on the easily accessible chronic stage, whereas ultrastructural investigations of tachyzoites were confined to in vitro studies. In the study presented here, the ultrastructural pathology of naturally B. besnoiti-infected cattle in the acute and chronic disease stages and experimentally B. besnoiti-infected mice was monitored. Further, the ultrastructure of tachyzoites and bradyzoites was investigated. Skin samples of two adult Limousin cows and one adult Limousin bull naturally infected with B. besnoiti and liver and skin samples of gamma-interferon knockout mice infected with B. besnoiti were examined in semithin sections stained with toluidine blue and safranin and in ultrathin sections contrasted with uranyl acetate and lead citrate. Samples of vessel walls of the bull and nasal mucosa of one cow were examined by scanning electron microscopy. Few tachyzoites-like endozoites were detected for the first time in bovine skin, and large numbers of tachyzoites were detected in murine skin and liver. Within tissue cysts in bovine skin, numerous bradyzoites were observed displaying signs of degeneration. Tachyzoites had apicomplexan endozoite ultrastructure. B. besnoiti tachyzoites and bradyzoites differed in shape and the number of amylopectin granules. Transmission and scanning electron microscopy confirmed the presence of two different cyst wall layers, and the present results on cyst wall ultrastructure were in accordance with those previously obtained by histological sections. [ABSTRACT FROM AUTHOR]

Published

2015

6. Alpha-tocopherol transfer protein gene inhibition enhances the acquired immune response during malaria infection in mice.

Author

Herbas, Maria, Natama, Magloire, and Suzuki, Hiroshi

Subjects

*PROTEIN genetics, *IMMUNE response, *MALARIA prevention, *MOUSE diseases, *PLASMODIUM yoelii, *PLASMODIUM berghei, *VITAMIN E

Abstract

Immune response to malaria infection is complex and seems to be regulated by innate and adaptive immune response as well as environmental factors such as host genetics and nutritional status. Previously, we have reported that α-tocopherol transfer protein knockout (α-ttp) mice, showing low concentrations of α-tocopherol in circulation, infected with Plasmodium berghei NK65 survived significantly longer as compared with the wild-type mice. In addition, Plasmodium yoelii XL-17, a lethal strain, showed non-lethal virulence in α-ttp mice. Thus, we hypothesized that the ability of the α-ttp mice to control P. yoelli XL-17 proliferation may allow them to build an efficient immune response against murine malaria infection. On 15 days after infection with P. yoelli XL-17, α-ttp mice were challenged to infection with P. berghei NK65. Results indicated that α-ttp mice infected with P. yoelli XL-17 built a protective immunity against P. berghei NK65 associated to extremely low levels of parasitemia, a controlled inflammatory response, and a robust antibody response. Moreover, the importance of α−tocopherol for parasite proliferation was remarkable. The results suggest that inhibition of α-tocopherol transfer protein activity is effective for the enhancement of acquired immunity in murine malaria infection. [ABSTRACT FROM AUTHOR]

Published

2014

7. Fusidic acid is an effective treatment against Toxoplasma gondii and Listeria monocytogenes in vitro, but not in mice.

Author

Payne, Amanda, Neal, Lori, and Knoll, Laura

Subjects

*MOUSE diseases, *ANTIBIOTICS, *TOXOPLASMA gondii, *LISTERIA monocytogenes, *INTRACELLULAR pathogens, *IN vitro studies, *THERAPEUTICS

Abstract

Fusidic acid is a bacteriostatic antibiotic that inhibits the growth of bacteria by preventing the release of translation elongation factor G (EF-G) from the ribosome. The apicomplexan parasite Toxoplasma gondii has an orthologue of bacterial EF-G that can complement bacteria and is necessary for parasite virulence. Fusidic acid has been shown to be effective in tissue culture against the related pathogen Plasmodium falciparum, and current drug treatments against T. gondii are limited. We therefore investigated the therapeutic value of fusidic acid for T. gondii and found that the drug was effective in tissue culture, but not in a mouse model of infection. To determine whether this trend would occur in another intracellular pathogen that elicits a T helper 1-type immune response, we tested the efficacy of fusidic acid for the bacterium Listeria monocytogenes. Similar to its effects on T. gondii, fusidic acid inhibits the growth of L. monocytogenes in vitro, but not in mice. These findings highlight the necessity of in vivo follow-up studies to validate in vitro drug investigations. [ABSTRACT FROM AUTHOR]

Published

2013

8. Antineoplastic drug, carboplatin, protects mice against visceral leishmaniasis.

Author

Kaur, Tejinder, Makkar, Prerna, Randhawa, Kulbir, and Kaur, Sukhbir

Subjects

*CARBOPLATIN, *LEISHMANIA donovani, *HEMATOLOGY, *ANTINEOPLASTIC agents, *MOUSE diseases, *VISCERAL leishmaniasis

Abstract

In the present study, the leishmanicidal effect of two doses (5 and 10 mg/kg body weight) of the carboplatin was studied in Leishmania donovani-infected BALB/c mice. Mice were infected intracardially with promastigotes of L. donovani, and a month after infection, they were treated intraperitoneally with the two doses of the drug (5 and 10 mg/kg body weight) for five continuous days. Animals were sacrificed on 1 and 15 posttreatment days. Hepatic parasite load was assessed on Geimsa-stained imprints. Immune responses were studied by measuring delayed-type hypersensitivity (DTH) responses, serum IgG isotype levels (IgG1 and IgG2a) and cytokine levels [γ-interferon (IFN-γ), interleukin (IL)-10 and IL-2] in spleen cell cultures by ELISA. To study the drug-induced side effects, various haematological (haemoglobin and total leukocyte count), biochemical (liver and kidney function tests) and histological investigations (kidney, liver and spleen) were carried out. The antileishmanial potential of the drug was revealed by significant reduction in the parasite burden. The infected and treated animals were also found to exhibit increased DTH responses, higher IgG2a levels, lower IgG1 levels and greater cytokine (IFN-γ, IL-10 and IL-2) concentrations pointing towards the generation of mixed Th1/Th2 response. Liver and kidney function tests and histological studies of kidney, liver and spleen of treated mice revealed no side effects. Carboplatin cures mice of visceral leishmaniasis without causing any serious side effects, and the drug was found be more effective at a dose of 10 mg/kg body weight as compared to 5 mg/kg body weight. [ABSTRACT FROM AUTHOR]

Published

2013

9. Cryopreservation of Toxoplasma gondii in infected murine tissues.

Author

Zheng, Huanqin, Chen, Ying, Lu, Fangli, Liu, Man, Yang, Xiaoyan, Fu, Xiaoyin, Zhao, Ying, Huang, Bo, Huang, Shiguang, and Kasper, Lloyd

Subjects

*CRYOPRESERVATION of organs, tissues, etc., *TOXOPLASMA gondii, *FIBROBLASTS, *MOUSE diseases, *SPLEEN

Abstract

Laboratory maintenance of the RH strain of Toxoplasma gondii is generally done by passage in mice, in vitro propagation in fibroblasts, or cryopreservation of peritoneal exudates from mice infected with T. gondii. To explore alternative techniques for preserving laboratory T. gondii tachyzoites, we propose a new method of freezing tissues from infected mice. The effect of storage of T. gondii tissue tachyzoites in two different cryoprotectant combinations and at two different temperatures was studied. The liver and spleen tissues, and peritoneal exudates from mice infected with RH-GFP strain of T. gondii, suspended in RPMI 1640 medium supplemented with 12 % glycerol plus 20 % calf serum, or 12 % dimethyl sulfoxide (DMSO) plus 20 % calf serum, were stored for 3 months at −20 °C in an ordinary refrigerator or at −80 °C in a deep freezer, respectively. The viability of tissue T. gondii tachyzoites was determined by animal inoculation method, which was assessed by monitoring survival and tissue parasitemia in recipient mice. Our data showed that toxoplasma tachyzoites in the above tissues remained viable after cryopreservation in 12 % DMSO plus 20 % calf serum at −80 °C, the infectivity of tachyzoites from the tissues and peritoneal fluids was demonstrated in inoculated murine tissues. Our data indicate that freezing infected murine tissues at −80 °C provides a simple and appropriate method for preservation of T. gondii tachyzoites in laboratory without the need for costly liquid nitrogen preservation procedures. [ABSTRACT FROM AUTHOR]

Published

2012

10. The potential role of Phoenix dactylifera on Eimeria papillata-induced infection in mice.

Author

Metwaly, Mahmoud, Dkhil, Mohamed, and Al-Quraishy, Saleh

Subjects

*DATE palm, *EIMERIA, *MOUSE diseases, *COCCIDIOSIS in animals, *FOOD additives

Abstract

Coccidiosis is a common infectious disease in poultry causing major economic losses. Here, we investigated the effect of Khodary date fruit aqueous extract (4 ml/kg) on the outcome of coccidiosis caused by Eimeria papillata in Swiss Albino mice. Date fruit extract was able to decrease the intracellular development by lowering the faecal output of E. papillata oocysts from 8.7 ± 0.5 × 10 to 6.6 ± 0.4 × 10 oocysts per gram faeces. Also, date extract caused a great diminish in body weight of infected mice from 19.3 to 3.2 %. The number of parasitic stages in the intestinal villi of the infected mice was reduced to about 52 % after treatment with date extract. The infection was associated with marked histopathological lesions of the murine jejunum in the form of inflammation, vacuolation of the epithelium, and destruction of some villi. Also, the number of goblet cells within the infected villi was significantly lowered ( P ≤ 0.05). These changes lead to an oxidative damage of the infected tissue. Moreover, infection induced a disturbance in both protein and carbohydrate content in the infected mice. Treatment of mice with date extract could improve the above-studied parameters. On the basis of the above results it can be hypothesized that date fruit can protect against coccidiosis-induced infection, this hypothesis can be revealed by the anti-inflammatory activity of date protecting host tissue from injuries induced by the parasite, and hence it is recommended to be used as an excellent food additive. [ABSTRACT FROM AUTHOR]

Published

2012

11. Cationic liposomes containing soluble Leishmania antigens (SLA) plus CpG ODNs induce protection against murine model of leishmaniasis.

Author

Heravi Shargh, Vahid, Jaafari, Mahmoud, Khamesipour, Ali, Jalali, Seyed, Firouzmand, Hengameh, Abbasi, Azam, and Badiee, Ali

Subjects

*LEISHMANIASIS treatment, *VETERINARY vaccines, *LIPOSOMES, *ANTIGENS, *LEISHMANIA, *MOUSE diseases

Abstract

Development of an effective vaccine against leishmaniasis is possible due to the fact that individuals cured from cutaneous leishmaniasis (CL) are protected from further infection. First generation Leishmania vaccines consisting of whole killed parasites reached to phase 3 clinical trials but failed to show enough efficacies mainly due to the lack of an appropriate adjuvant. In this study, an efficient liposomal protein-based vaccine against Leishmania major infection was developed using soluble Leishmania antigens (SLA) as a first generation vaccine and cytidine phosphate guanosine oligodeoxynucleotides (CpG ODNs) as an immunostimulatory adjuvant. 1, 2-Dioleoyl-3-trimethylammonium-propane was used as a cationic lipid to prepare the liposomes due to its intrinsic adjuvanticity. BALB/c mice were immunized subcutaneously (SC), three times in 2-week intervals, with Lip-SLA-CpG, Lip-SLA, SLA + CpG, SLA, or HEPES buffer. As criteria for protection, footpad swelling at the site of challenge and spleen parasite loads were assessed, and the immune responses were evaluated by determination of IFN-γ and IL-4 levels of cultured splenocytes, and IgG subtypes. The group of mice that received Lip-SLA-CpG showed a significantly smaller footpad swelling, lower spleen parasite burden, higher IgG2a antibody, and lower IL-4 level compared to the control groups. It is concluded that cationic liposomes containing SLA and CpG ODNs are appropriate to induce Th1 type of immune response and protection against leishmaniasis. [ABSTRACT FROM AUTHOR]

Published

2012

12. Structural changes of Schistosoma mansoni adult worms recovered from C57BL/6 mice treated with radiation-attenuated vaccine and/or praziquantel against infection.

Author

Reda, Enayat, Ouhtit, Allal, Abdeen, Sherif, and El-Shabasy, Eman

Subjects

*SCHISTOSOMA mansoni, *SCHISTOSOMA, *DRUG interactions, *MOUSE diseases, *PREVENTIVE medicine, *THERAPEUTICS, INFECTION treatment

Abstract

Although the current treatment of schistosomiasis relies largely on praziquantel (PZQ), it has not significantly reduced the overall number of disease cases, perhaps due to inevitable resistance to PZQ. Previous studies showed that radiation-attenuated vaccine gives protection levels for Schistosoma mansoni in host various species. In the present study, we evaluated the effect of various vaccination strategies in C57BL/6 mice, including single or multiple vaccination strategy, subcurative dose (20 mg/kg) of PZQ, and a combination of single vaccination with subcurative dose of PZQ. Groups of five mice were sacrificed postinfection in 42 days and schistosomes were collected by perfusion and examined by scanning electron microscopy. Treatment either with subcurative dose of PZQ or with a single vaccination of attenuated cercariae (500 per mouse), caused significant reduction in total worm burden, hepatic and intestinal ova counts 43.03%, 73.2%, 59.5% and 37.97%, 52.02%, 26.3%, respectively. Furthermore, tegumental changes were observed, including severe swelling, fusion of tegumental folds, vesicle formation, and loss or shortening of the spines on the tubercles. However, multiple vaccination strategy resulted in much higher reduction in total worm burden, hepatic and intestinal ova count. However, multiple vaccination strategy resulted in high reduction of worm burden, hepatic and intestinal ova counts 72.5%, 90.7%, 65.79%, respectively, and further causing swollen, disruption of tubercles teguments and erosion, extensive peeling, fusion of tegumental folds. Our findings suggest that multiple vaccination strategy is the most effective strategy to clear schistosomal infection, indicating its potential in guiding the design of appropriate therapeutic strategy against schistosomes. [ABSTRACT FROM AUTHOR]

Published

2012

13. Efficacy of Lasia spinosa leaf extract in treating mice infected with Trichinella spiralis.

Author

Yadav, Arun and Temjenmongla

Subjects

*TRICHINOSIS in animals, *MOUSE diseases, *ALBENDAZOLE, *TRICHINELLA spiralis, *LABORATORY mice, *MYALGIA, *THERAPEUTICS

Abstract

Trichinellosis is a widespread zoonoses for which no effective drug treatment is available at this time. Though anthelmintics such as mebendazole and albendazole are commonly used to treat human trichinellosis, none of these drugs are fully effective against the encysted or new-born larvae of Trichinella spiralis. In recent years, there has been a growing interest in developing newer anthelminthics from medicinal plants, particularly the ones used in traditional medicines in many parts of the world, due to the increasing spread of anthelminthic resistance and/or decreasing activity against encapsulated larval stages of parasites. The aim of the present study was to investigate the efficacy of leaf extract of Lasia spinosa (Araceae) against different life cycle stages of T. spiralis, i.e. adult (days 3 and 4 post-infection), migrating larvae (days 8, 9 and 10 post-infection) and encysted muscle larvae (days 31-37 post-infection). The study showed that L. spinosa leaf extract is effective against all the three life cycle stages of parasite. Against the adult stage, an oral administration of plant extract at 800 mg/kg dose revealed a 75.30% reduction in the number of adult worms, as compared to untreated controls at day 10 post-infection. Whereas against migrating larvae, the same dose of plant extract given for 3 days, reduced the number of larvae recovered from musculature of treated animals by 72.23%. However, in comparison of preceding two stages, the extract showed comparatively less efficacy against the encysted larvae of parasite. In this case, the 800 mg/kg dose of extract given for 7 days (after 30 day of post-infection) revealed only 64.84% reduction in the number of encysted larvae, as was evident from larval count on day 49 post-infection. Therefore, the results of this study indicate that leaf extract of L. spinosa possesses significant anthelminthic efficacy against the adult stages and migrating larvae of T. spiralis. On the other hand, the encysted muscle larvae of parasite are comparatively less sensitive to L. spinosa leaf extract treatment. [ABSTRACT FROM AUTHOR]

Published

2012

14. Toxocara canis larvae reinfecting BALB/c mice exhibit accelerated speed of migration to the host CNS.

Author

Kolbeková, Petra, Větvička, David, Svoboda, Jan, Skírnisson, Karl, Leissová, Markéta, Syrůček, Martin, Marečková, Helena, and Kolářová, Libuše

Subjects

*TOXOCARA, *LARVAE, *MOUSE diseases, *ENZYME-linked immunosorbent assay, *PARASITE antigens, *CENTRAL nervous system, *IMMUNOGLOBULIN G

Abstract

Using a small animal imaging system, migratory activity of Toxocara canis larvae stained by carboxyfluorescein succinimidyl ester (CFSE) was observed post primary infection (PPI) and post reinfection (PR) of BALB/c mice. Each infection was performed with 1,000 larvae per mouse. Primary infections were performed with labeled larvae, while for challenge infections the reinfecting larvae were stained by CFSE. The worm burden in mouse organs was determined during a period from 6 h to 21 days and 4 months PPI and PR. In comparison with primary infections that led to the first larvae appearance in the brain after 60 h, greatly accelerated migration of the parasites administered 3 weeks PPI to the CNS and eyes of challenged mice was noted-in both organs the larvae appeared 6 h PR. In all challenged mice, reinfecting larvae prevailed in the resident parasite population. Preliminary experiments with Toxocara cati larvae also revealed early brain involvement in primarily infected mice. Staining of T. canis larvae by CFSE had no effect on the development of a humoral antibody response against T. canis excretory-secretory antigens. In ELISA, elevated levels of specific IgG and IgG1 were noted on day 14 PPI and the levels of antibodies increased till the end of experiment. Reinfection induced an increase in the levels of both antibodies. In terms of optical density, IgG1 antibodies gave higher values in all sera examined. In ELISA for IgG antibodies, an increase in the avidity index of around 50% was detected 1 month PPI; higher-avidity antibodies were also detected in sera of reinfected animals. [ABSTRACT FROM AUTHOR]

Published

2011

15. Differential miRNA expression in the mouse jejunum during garlic treatment of Eimeria papillata infections.

Author

Al-Quraishy, Saleh, Delic, Denis, Sies, Helmult, Wunderlich, Frank, Abdel-Baki, Abdel Azeem S., and Dkhil, Mohamed Monam

Subjects

*THERAPEUTIC use of garlic, *MOUSE diseases, *NITRIC oxide, *MALONDIALDEHYDE, *MICROARRAY technology, *EIMERIA, *THERAPEUTICS

Abstract

umulating evidence indicates a critical role of microRNAs (miRNAs) in the outcome of diseases. Here, we investigate the effect of garlic on the intestinal miRNA signature of male Balb/c mice during infections with Eimeria papillata. Garlic decreases the intracellular development as evidenced by a lowered fecal output of E. papillata oocysts from 3,150 ± 410 to approximately 1,750 ± 390 oocysts per gram feces on day 4 postinoculation. This anti-coccidial activity of garlic is associated with an inhibition of the E. papillata-induced increases of interferon gamma, inducible nitric oxide synthase, nitrite/nitrate, and malondialdehyde and decrease in glutathione. Moreover, garlic downregulates the E. papillata-induced increases in the expression of the miRNAs miR-1959, miR-203, and miR-21, and it upregulates the expression of the 11 miRNA species miR-142-5P, miR-15A, miR-10A, miR-29B, miR-1902, miR-125A-5P, let-7E, miR-148A, miR-130A, miR-10B, and miR-93, respectively, as revealed by miRXplore microarray technology. Real-time PCR confirms these effects of garlic in the jejunum of E. papillata-infected mice. Our data indicate that the anti-coccidial activity of garlic is associated with specific changes in the miRNA signature of the mouse jejunum, the target site of E. papillata. These changes may reflect an involvement of miRNAs in garlic-activated pathways to reduce and/or to repair E. papillata-induced tissue injuries. [ABSTRACT FROM AUTHOR]

Published

2011

16. Serodiagnosis of experimental sparganum infections of mice and human sparganosis by ELISA using ES antigens of Spirometra mansoni spargana.

Author

Jing Cui, Nan Li, Zhong Wang, Peng Jiang, and Xi Lin

Subjects

*MOUSE diseases, *SERODIAGNOSIS, *ANTIGENS, *TOXOPLASMA gondii, *LABORATORY mice, *SERUM

Abstract

We conducted a study of serodiagnosis of experimental sparganum infections of mice and human sparganosis by enzyme-linked immunosorbent assay (ELISA) using excretory-secretory (ES) antigens of Spirometra mansoni spargana and compared the sensitivity and specificity of crude and ES antigens for detecting the specific anti-sparganum IgG antibodies. By crude antigen ELISA and ES antigen ELISA, anti-sparganum IgG was detected in all of 30 serum samples of the infected mice; no cross-reactions were observed in serum samples of the mice infected with Trichinella spiralis, Schistosoma japanicum, Toxoplasma gondii, and normal mice. Anti-sparganum IgG was detected by ES antigen ELISA in sera of mice infected with one, two, four, six, and eight spargana at 3 weeks post-infection (wpi), with a detection rate of 100%, and lasted to 18 wpi when the experiment was ended. The difference in anti-sparganum antibody levels among five groups of the infected mice was statistically significant ( F = 245.296, p < 0.05); the antibody levels were correlated with infecting doses of spargana ( r = 0.323, p < 0.05). The sensitivity of both ELISA in detecting the serum samples of patients with sparganosis was 100% (20/20), but 96.72% (59/61) of specificity of ES antigen ELISA in detecting serum samples of patients with cysticercosis, echinococcosis, paragonimiosis, clonorchiosis, and schistosomiasis, and healthy persons was significantly greater than 72.13% (44/61) of crude antigen ELISA ( χ = 14.027, p < 0.05). Our finding indicates that ELISA using ES antigens of S. mansoni spargana may be applied to the specific early serodiagnosis of sparganosis. [ABSTRACT FROM AUTHOR]

Published

2011

17. Effect of mefloquine administered orally at single, multiple, or combined with artemether, artesunate, or praziquantel in treatment of mice infected with Schistosoma japonicum.

Author

Shu-hua Xiao, Jing-yan Mei, and Pei-ying Jiao

Subjects

*MOUSE diseases, *MEFLOQUINE, *SCHISTOSOMA japonicum, *INFECTION, *WORMS, *THERAPEUTICS

Abstract

The purpose of the study is to explore the efficacy of mefloquine administered orally at single, multiple doses, or in combination with artesuante, artemether, or praziquantel in mouse- Schistosoma japonicum model. A total of 205 mice were divided into 4 batches and each batch of mice was infected percutaneously with 40 S. japonicum cercariae for 35 days. The infected mice were treated orally with mefloquine at single doses, multiple daily doses, or combined with artesunate, artemether, or praziquantel, while infected but untreated mice served as control. All treated animals were killed 4 weeks post-treatment for assessment of effect. When infected mice were treated orally with mefloquine at single or multiple daily doses under the same total dose levels, the tendency to decrease the efficacy was seen. Particularly, when a lower single dose of 100 mg/kg was divided equally into five daily doses of 20 mg/kg, the efficacy decreased statistically significant ( P < 0.05), i.e., the total worm and female worm reductions of 67.9% and 73.4% decreased to 31.3% and 30.3%, respectively. In infected mice treated with mefloquine or artesuante at a single dose of 100 mg/kg, a moderate effect against schistosomes was observed. No further significant reduction of total and female worm burdens was seen, when the two drugs combined together at the same dose level. On the other hand, administration of mefloquine combined with artesunate at single dose of 50 mg/kg, which exhibited no effect against schistosomes, resulted in significant reduction of total and female worm burdens in comparison with the groups treated with mefloquine and artesunate alone at the same dose level. Similar results were observed in treatment of infected mice with mefloquine in combination with artemether at the smaller dose of 50 mg/kg. The total worm burden was significantly lower than that of control and the female worm burden was also significant lower than that of groups treated with mefloquine and artemether alone. Interestingly, in administration of mefloquine 100 mg/kg combined with artemether 100 mg/kg to the infected mice, all female worms were killed and the total worm burden was also statistically significant lower than that of groups treated with either drug alone. Finally, when infected mice were treated with mefloquine combined with prazqiuatel at single dose of 50 mg/kg, no apparent improvement in efficacy was seen. Administration of mefloquine 100 mg/kg combined with praziquantel 100 mg/kg, only the difference of female worm burdens between praziquantel group and combined treatment group was statistically significant. The results indicate that under the same dose level of mefloquine, the efficacy of single dose is superior to that of multiple daily doses; mefloquine combined with artesunate or artemether at an invalid or moderate effective dose may show synergistic effect, especially the effect against female worms; no prominent synergistic effect is observed, when the similar dose level of mefloquine in combination with praziquantel. [ABSTRACT FROM AUTHOR]

Published

2011

18. Murine schistosomiasis as a model for human schistosomiasis mansoni: similarities and discrepancies.

Author

Abdul-Ghani, Rashad A. and Hassan, Azza A.

Subjects

*SCHISTOSOMIASIS, *MOUSE diseases, *ANIMAL models of immunology, *DRUG therapy, *ANIMAL models in research

Abstract

Human schistosomiasis has been studied extensively since its discovery by Theodore Bilharz in 1851. Because of its medical importance as a chronic debilitating disease in the tropics and subtropics, continuing research efforts are still going on. The use of animal models still represents a major cornerstone in this field, with murine hosts, especially mice, as the most preferable experimental units. Murine schistosomiasis has been employed as a model for studying various aspects of human schistosomiasis, including biology, pathogenesis, immunology, chemotherapy screening, and vaccine development. However, there may be differences between murine and human schistosomiasis. The present article tries to explore some of these aspects that may help researchers in the field of schistosomiasis. [ABSTRACT FROM AUTHOR]

Published

2010

19. Evaluation of effects of albendazole on the kinetics of cytosolic glutathione transferase in skeletal muscles during experimental trichinellosis in mice.

Author

Agnieszka Wojtkowiak, Krystyna Boczo?, El?bieta Wandurska-Nowak, and Monika Derda

Subjects

*ALBENDAZOLE, *GLUTATHIONE transferase, *TRICHINOSIS, *MOUSE diseases

Abstract

Abstract??In this study, the effect of trichinellosis as well as the effect of albendazole treatment on the kinetics of substrate saturation of cytosolic glutathione transferase (GST) in the skeletal muscles from infected mice was examined because the idea of multifunctional mode of action of anthelmintic drugs was considered. Our results pointed out to the influence of trichinellosis and albendazole treatment on the quaternary structure of GST in mouse muscles. A double reciprocal plot of GST saturation in control mice was biphasic with apparent low and highKmvalues equal to 0.54 and 1.0?mM, respectively. Infection withTrichinella spiralisin the third week postinfection caused a 2.3-fold increase in the highKmvalue and at the same time a 2.8-fold decrease in the lowKm. In the sixth week postinfection, the highKmvalue was unchanged, but the lowKmvalue increased 2.3 times. Calculated from the double reciprocal plot of GST substrate saturation in muscles from infected and treated mice (measured in the third week postinfection only), the highKmvalue increased 1.4 times relative to the respective controls. The normal substrate saturation plot of GST in treated mice has a clearly ?double sigmoid? character. Our results suggest that despite the complicated character of the GST saturation curve, albendazole seems to act as an allosteric activator for cytosolic GST in infected mouse muscles. [ABSTRACT FROM AUTHOR]

Published

2007

20. N -acetyl-<span style="font-variant:small-caps">l</span> -cysteine reduces the parasitism of BALB/c mice infected with Leishmania amazonensis.

Author

Marta Monteiro, Fúlvia Marques, Renê Blazius, Onilda Santos da Silva, Fernando de Queiroz Cunha, Diana Bento, and Pedro Torres Romão

Subjects

*CYSTEINE proteinases, *PARASITISM, *MOUSE diseases, *LEISHMANIA

Abstract

Abstract   Leishmania amazonensis infection leads to progressive diseases in a majority of inbred strains of mice. Glutathione (GSH) participates in a large number of cellular phenomena and seems to be essential for several immune functions, including host defense during leishmaniasis. In this study, we evaluated the effects of N-acetyl-l-cysteine (NAC), as GSH supplement, on the course of L. amazonensis infection in susceptible BALB/c mice. The treatment with NAC (200 mg/kg daily) was effective in raising GSH levels in both lymph node and spleen cells. Although this treatment did not change the footpad swelling development in L. amazonensis-infected mice, it caused a significant decrease in the number of parasites recovered from the footpad lesion and draining popliteal lymph node. Our data suggest that intracellular Leishmania killing in vivo was improved by the augment of GSH levels through NAC administration. [ABSTRACT FROM AUTHOR]

Published

2008