Inter-stain interactions of a vector-borne parasite over its life cycle, "Borrelia afzelii", "Mus musculus", "Ixodes ricinus" model

Many pathogens consist of genetically distinct strains. When hosts are simultaneously infected with multiple strains the phenomenon is known as a mixed infection or a co-infection. In mixed infections, strains can interact with each other and these interactions between strains can have important consequences for their transmission and frequency in the pathogen population. Vector-borne pathogens have a complex life cycle that includes both a vertebrate host and an arthropod vector. As a result of this complexity, interactions between strains can occur in both the host and the vector. Interactions between strains in the vertebrate host are expected to influence transmission from the co-infected host to uninfected vectors. Conversely, interactions between strains in the arthropod vector are expected to influence transmission from the co-infected vector to the uninfected host. This thesis used the tick-borne bacterium, Borrelia afzelii, as a model system to investigate how co-infection and interactions between strains influence their transmission and lifetime fitness over the course of the tick-borne life cycle. B. afzelii is a common cause of Lyme disease in Europe, it is transmitted by the castor bean tick (Ixodes ricinus) and it uses small mammals (e.g. rodents) as a reservoir host. An experimental approach with two genetically distinct strains of B. afzelii (one Swiss stain, one Finnish strain) was used to investigate the effects of co-infection in both the host and the vector. In Chapter 1, lab mice were experimentally infected via tick bite with either 1 or 2 strains of B. afzelii. The infected mice were then fed upon by I. ricinus ticks from a laboratory colony to quantify host-to-tick transmission. qPCR was used to determine the presence and abundance of each strain in the ticks. Chapter 1 found that co-infection in the mice reduced the host-to-tick transmission success of the strains. This chapter also found that co-infection reduced the abundance of each strain in the tick. This is one of the first studies to show that co-infection is important for determining the abundance of the pathogen strains in the vector. In the lifecycle of B. afzelii, the bacterium is acquired by larval ticks that blood feed on an infected host. These larvae subsequently moult into nymphs that are responsible for transmitting the bacterium to the next generation of hosts. The bacterium has to persist inside the midgut of the nymph for a long time (8 – 12 months). Chapter 2 investigated whether nymphal ageing (1-month-old vs 4-month-old nymphs) under different environmental conditions (summer vs winter) influenced the interactions between strains in co-infected ticks. The spirochete abundance inside the nymph decreased with nymphal age, but there was no effect of the environmental conditions investigated. In Chapter 3, the presence and abundance of the two strains of B. afzelii were quantified in the tissues of 6 different organs (bladder, left ear, right ear, heart, ankle joint, and dorsal skin) that were harvested from the co-infected and singly infected mice. This study showed that co-infection in the mouse host reduced the prevalence of the Finnish strain in the host tissues (but the Swiss strain was not affected by co-infection). Chapter 3 found a positive relationship between the prevalence (or abundance) of each strain in the mouse tissues and the host-to-tick transmission of each strain. External tissues (e.g. ears) were more important for host-to-tick transmission than internal organs (e.g. bladder). Chapter 3 enhances our understanding of the biology of mixed infections by showing the causal links between co-infection in the host, the distribution and abundance of the strains in host tissues and the subsequent host-to-tick transmission success of the strains. Chapter 4 investigated how co-infection in the arthropod vector influences vector-to-host transmission success. A second infection experiment was performed, where naïve mice were exposed to nymphs that were either co-infected or infected with one of the two strains (i.e., using the nymphs generated in Chapters 1 and 2). The infection status of the mice was then tested using the same qPCR-based methods. Importantly, Chapter 4 confirmed that the negative effect of co-infection in the mouse on host-to-tick transmission (observed in Chapters 1, 2, and 3) had real fitness consequences for subsequent tick-to-host transmission. Ticks that had fed on co-infected mice were much less likely to transmit their strains to the host because these strains were less common inside these co-infected ticks. Chapter 4 did not find evidence that co-infection in the nymph influenced the nymph-to-host transmission success of each strain. This Chapter did find that there was a two-fold difference in nymph-to-host transmission success between the two strains. This work provides evidence for the idea that vector-borne pathogen strains can exhibit trade-offs across the different steps of their complex life cycles. In the co-infected mice, the Swiss strain had higher host-to-tick transmission success than the Finnish strain. Conversely, the Finnish strains had higher spirochete loads in the tick vector and had tick-to-host transmission success. Thus, the Swiss and Finnish strains are specialized on the host versus the vector, respectively.

Complete Genome Sequence of Mycoplasma feriruminatoris Strain IVB14/OD_0535, Isolated from an Alpine Ibex in a Swiss Zoo

Mycoplasma feriruminatoris is a fast-growing and genetically tractable mycoplasma species. We sequenced the Swiss strain IVB14/OD_0535, isolated from an Alpine ibex. This strain has a circular genome of 1,027,435 bp with a G+C content of 24.3%. It encodes 835 open reading frames (ORFs), 2 rRNA operons, and 30 tRNAs.

ANALGETICACTIVITY TEST OF ETHANOL EXTRACT OFTAMARIND LEAVES (TamarindusIndica L.) TO MALEMICE OF SWISS STRAIN

Tamarind is a medicinal plant that has benefits as an antiseptic, antipyretic and analgetic (anti-pain). Pain is an unpleasant sensory and emotional experience due to actual or potential damage.The purpose thisstudy to determine the optimal analgetic and dosage activity of tamarind leaf ethanol extract on male mice swiss strain induced by acetic acid. The method used is analysis of results by observing the amount of stretching of mice every five minutes for an hour. The cumulative amount of stretching in mice to calculate the analgetic activity was obtained from the amount of stretching of mice induced by acetid acid intraperitoneally within 30 minutes after orally induced. Statistical analgetic data using kolmogorov-smirnov normality test, test of homogenity of variances followed by Anova test and post hoc tests using SPSS 24.0 for windows. Percentanalgesic activity of ethanol extract of leaves tamarind dosage 5%, 10%, 20%wererespectively (9,81 ± 2,24)%, (24,68 ± 2,10)% and (36,39 ± 3,06)%. Ethanol extract of leaves tamarind dosage 20% provide the most optimal activity analgesic

Uji Efek Analgetik Infusa Daun Beluntas (Pluchea indica L.) Pada Mencit Jantan Galur Swiss

Beluntas leaves (Pluchea indica L.) have been known as analgetic reducer. The study about this research has been going on right now. The goal of this research is to study the analgesic effect of beluntas (P. indica) leaf infused into male mice of swiss strain. The method used is the stretching chemical stimuli using acetic acid as an inducer of pain. Healthy male mice of Swiss strain were divided into five groups, and each group consisted of 5 mice. Group I was given paracetamol at a dose of 65 mg/kg of body weight, group II were given distilled water , the group III-V were given beluntas leaf infuse in the variation of 10 %, 20 % and 40 %. Thirty minutes after test substance application, acetic acid of 100 mg/kg of body weight were given intraperitoneally in all groups and stretching of mice was observed every 5 minutes for 1 hour. The data was analyzed by using normality test of Kolmogorov-Smirnov; the test of homogeneity of variance was analyzed by ANOVA and post hoc tests were to differenciate the percentage analgetic of every group. Statistical test showed normal distributed and homogeneous data; there are significant differences of percentage analgesic between paracetamol and beluntas leaf infuse of 10, 20, and 40 % (p < 0.05). There was significant differences between infuse of beluntas leaves with positive control (parasetamol) in mice. Key words: Analgetic, leave of beluntas (P. indica), infuse, mice.

Nephroprotective Effect of Pentoxyphylline Through Improvement in the Expression of TGF-beta1, Collagen Type-1, and Renal Interstitial Fibrosis in Swiss Strain Mice After Being Induced by Doxorubicin

BACKGROUND: Use of doxorubicin (DXR) in the treatment of cancer has been increasing along with the increase in cancer morbidity. Nephrotoxic effects of DXR are still a problem. Pentoxyphylline (PTX) as an electron-donor material can be nephroprotective, so the combination of DXR and PTX might reduce the nephrotoxic effects of DXR. The aim of this study was to prove the nephroprotective effect of PTX and DXR nephrotoxicity through the improvement of TGF-β1, collage type-1, and renal interstitial fibrosis.METHODS: Twenty-four males Swiss strain mice, divided into three groups namely Control (C) injected with NaCl 0.9%; DXR induced nephrotoxicity (D); and effect of PTX on D (P/D) by intraperitoneally, respectively, each group consisted of 8 mice. Injections were given once a week for three consecutive weeks. At 8th week post-treatment, all eight mice of each group were sacrificed. Examination of TGF-β1 and collagen type-I expression was done by immunohistochemistry with monoclonal antibody. Renal interstitial fibrosis examination was done by a histopathologist, using Verheoff van Giesen staining. The statistic analysis was carried out using one-way ANOVA.RESULTS: TGF-β1 expression increased from C to D and subsequently decreased in P/D (4.50±3.89 vs. 177.88±68.78 vs. 36.88±9.51). Collagen type-I expression increased from C to D and subsequently decreased in P/D (12.00±14.32 vs. 186.25±125.62 vs. 36.00±29.14). Renal interstitial fibrosis expression increased from C to D and subsequently decreased in P/D (16.75±6.14 vs. 85.00±7.33 vs. 60.50±11.40). The expression of TGF-β1, collagen type-1, and renal interstitial fibrosis were higher significantly in D group as compared to C group (p<0,001). The expression of TGF-β1, collagen type-1, and renal interstitial fibrosis were lower significantly in P/D group as compared to D group (p<0.005).CONCLUSIONS: PTX was proved to be nephroprotector inducing by DXR.KEYWORDS: PTX, nephroprotector, TGF-β1, collagen type-I, renal interstitial fibrosis

Model of induction of thyroid dysfunctions in adult female mice

It is described the elaboration of a protocol to induce hyperthyroidism and hypothyroidism in mice by administrating thyroxin and propylthiouracil, respectively, in the drinking water. The drugs were administered to adult female mice of the Swiss strain for 30 days in order to obtain a systemic status of thyroid dysfunction. The induction of hyperthyroidism and hypothyroidism in the animals was confirmed by the histomorphological analysis of the thyroid in the end of the experiment, when the state of gland dysfunction in the animals submitted to the treatment was observed.

Uptake of Labelled Tallysomycin by Solid Ehrlich Ascites Tumors in Mice

Tumor and normal tissue uptake of 51Cror 57Co-labelled bleomycin (BLEO) and tallysomycin (TLM) was compared in female solid Ehrlich ascites tumor mice of Swiss strain. The complexes were administered intraperitoneally: 30-50 μ§ of each complex with an activity of 40-120 μCi. Activity distribution factors (ADF) and tumor/non-tumor ratios for blood, bone, skeletal muscles, kidneys and liver were determined. The ratios were generally higher for complexes labelled with 57Co than for the 51Cr-labelled ones; bleomycin appears equivalent or superior to tallysomycin.