Exploring female mice interstrain differences relevant for models of depression

Depression is an extremely heterogeneous disorder. Diverse molecular mechanisms have been suggested to underlie its etiology. To understand the molecular mechanisms responsible for this complex disorder, researchers have been using animal models extensively, namely mice from various genetic backgrounds and harboring distinct genetic modifications. The use of numerous mouse models has contributed to enrich our knowledge on depression. However, accumulating data also revealed that the intrinsic characteristics of each mouse strain might influence the experimental outcomes, which may justify some conflicting evidence reported in the literature. To further understand the impact of the genetic background, we performed a multimodal comparative study encompassing the most relevant parameters commonly addressed in depression, in three of the most widely used mouse strains: Balb/c, C57BL/6, and CD-1. Moreover, female mice were selected for this study taken into account the higher prevalence of depression in women and the fewer animal studies using this gender. Our results show that Balb/c mice have a more pronounced anxious-like behavior than CD-1 and C57BL/6 mice, whereas C57BL/6 animals present the strongest depressive-like trait. Furthermore, C57BL/6 mice display the highest rate of proliferating cells and brain-derived neurotrophic factor (Bdnf) expression levels in the hippocampus, while hippocampal dentate granular neurons of Balb/c mice show smaller dendritic lengths and fewer ramifications. Of notice, the expression levels of inducible nitric oxide synthase (iNos) predict 39.5% of the depressive-like behavior index, which suggests a key role of hippocampal iNOS in depression. Overall, this study reveals important interstrain differences in several behavioral dimensions and molecular and cellular parameters that should be considered when preparing and analyzing experiments addressing depression using mouse models. It further contributes to the literature by revealing the predictive value of hippocampal iNos expression levels in depressive-like behavior, irrespectively of the mouse strain.

An efficient chronic unpredictable stress protocol to induce stress-related responses in C57BL/6 mice

Exposure to chronic stress can have broad effects on health ranging from increased predisposition for neuropsychiatric disorders to deregulation of immune responses. The chronic unpredictable stress (CUS) protocol has been widely used to study the impact of stress exposure in several animal models and consists in the random, intermittent, and unpredictable exposure to a variety of stressors during several weeks. CUS has consistently been shown to induce behavioral and immunological alterations typical of the chronic stress-response. Unfortunately C57BL/6 mice, one of the most widely used mouse strains, due to the great variety of genetically modified lines, seem to be resistant to the commonly used 4-week-long CUS protocol. The definition of an alternative CUS protocol allowing the use of C57BL/6 mice in chronic stress experiments is a need. Here, we show that by extending the CUS protocol to 8?weeks is possible to induce a chronic stress-response in C57BL/6 mice, as revealed by abrogated body weight gain, increased adrenals weight, and an overactive hypothalamic-pituitary-adrenal axis with increased levels of serum corticosterone. Moreover, we also observed stress-associated behavioral alterations, including the potentiation of anxious-like and depressive-like behaviors and a reduction of exploratory behavior, as well as subtle stress-related changes in the cell population of the thymus and of the spleen. The present protocol for C57BL/6 mice consistently triggers the spectrum of CUS-induced changes observed in rats and, thus, will be highly useful to researchers that need to use this particular mouse strain as an animal model of neuropsychiatric disorders and/or immune deregulation related to CUS.

Hind limb ischemia in type 1 diabetic mice as useful tool to evaluate the neovascularization of tissue engineering constructs

Hind-limb ischemia has been used in type 1 diabetic mice to evaluate treatments for peripheral arterial disease or mechanisms of vascular impairment in diabetes [1]. Vascular deficiency is not only a pathophysiological condition, but also an obvious circumstance in tissue regeneration and in tissue engineering and regenerative medicine (TERM) strategies. We performed a pilot experiment of hind-limb ischemia in streptozotocin(STZ)-induced type 1 diabetic mice to hypothesise whether diabetes influences neovascularization induced by biomaterials. The dependent variables included blood flow and markers of arteriogenesis and angiogenesis. Type 1 diabetes was induced in 8-week-old C57BL/6 mice by an i.p. injection of STZ (50 mg/kg daily for 5 days). Hind-limb ischemia was created under deep anaesthesia and the left femoral artery and vein were isolated, ligated, and excised. The contralateral hind limb served as an internal control within each mouse. Non-diabetic ischaemic mice were used as experiment controls. At the hind-limb ischemia surgical procedure, different types of biomaterials were placed in the blood vessels gap. Blood flow was estimated by Laser Doppler perfusion imager, right after surgery and then weekly. After 28 days of implantation, surrounding muscle was excised and evaluated by histological analysis for arteriogenesis and angiogenesis. The results showed that implanted biomaterials were promote faster restoration of blood flow in the ischemic limbs and improved neovascularization in the diabetic mice. Therefore, we herein demonstrate that the combined model of hind-limb ischemia in type 1 diabetes mice is suitable to evaluate the neovascularization potential of biomaterials and eventually tissue engineering constructs.  

Vacunación en la Enfermedad de Chagas experimental: estudio de mediadores involucrados en la protección en ratones y aplicación de la vacuna en perros. Vaccination in experimental Chagas'disease: study of intermediates involved in the protection of mice and application of the vaccine in dogs.

La Enfermedad de Chagas es una de las principales endemias de América Latina donde existen cerca de 18 millones de infectados y 90 millones en riesgo. Entre el 25 y el 30 por ciento desarrolla patología cardíaca o digestiva en el período crónico. Se ha postulado que mecanismos autoinmunes, sumados a la acción directa del parásito, podrían estar involucrados en la patogenia de la enfermedad. El desarrollo de vacunas tradicionales en Enfermedad de Chagas es una meta difícil de alcanzar, por lo cual parece más factible abordar estrategias basadas en la inmunomodulación, para disminuir la carga parasitaria, minimizar las acciones deletéreas en el periodo agudo y prevenir el desarrollo de patología en la etapa crónica. Para ello es necesario avanzar en el conocimiento de los mecanismos involucrados en la protección y en la patogenia. Si se acepta la hipótesis autoinmune, una estrategia de vacunación con un tripanosoma antigénicamente similar al T. cruzi pero no patógeno podría evitar posibles mecanismos autoagresivos. En nuestro Laboratorio se ha empleado un modelo de vacunación en ratones utilizando como inmunógeno el Trypanosoma rangeli, no patógeno en humanos. Los ratones vacunados, infectados con T. cruzi, mostraron buena respuesta inmune celular y humoral, bajas parasitemias, ausencia de lesiones histológicas, y sobrevida cercana al 100 por ciento. Los controles no vacunados tuvieron una elevada mortalidad. Debido al ciclo biológico del parásito, la defensa efectiva contra el T. cruzi requiere una potente respuesta de anticuerpos contra las formas extracelulares y una eficaz respuesta celular contra los amastigotes intracelulares. En el modelo desarrollado en nuestro laboratorio la protección se asocia con un adecuado equilibrio entre respuesta TH1 y TH2, con leve predominio TH1, disminución de citoquinas (Ck) proinflamatorias e incremento de receptores solubles de Ck. El esquema de inmunización demostró asimismo su eficacia en cobayos y en perros mantenidos en el Laboratorio. Hipótesis de trabajo: - La vacunación con T. rangeli desencadena mecanismos inmunomodulatorios que protegen de la infección con T. cruzi, entre los cuales se encuentran eventos que actúan tempranamente en el sitio de inoculación y en los que están involucradas células y moléculas del sistema inmune innato. - La vacunación a perros constituye una nueva herramienta en la lucha contra la Enfermedad de Chagas. Objetivos: i) profundizar el estudio tendiente a dilucidar los mecanismos involucrados en la resistencia inducida por la inmunización con T. rangeli en ratones; ii) estudiar el efecto que tiene el estrés físico de los ratones sobre la eficacia de la vacunación y iii) analizar la inmunogenicidad de la vacuna en perros de zonas endémicas para Enfermedad de Chagas. Material y metodos: Los ratones y perros serán vacunados con tres dosis de epimastigotes de T. rangeli, fijados con glutaraldehido y los controles solo recibirán PBS. Los ratones seran desafiados con T. cruzi. Se estudiará en liquido peritoneal: a) poblaciones celulares por Citometria de flujo; b) cuantificación de los distintos tipos de inmunoglobulinas, de citoquinas y sus receptores solubles, por ELISA, c) ON y arginasa, por técnicas colorimetricas; d) est.udio de la interacción macrófago-parásito y de receptores celulares por Inmunofluorescencia. e) En perros, se realizarán estudios parasitológicos (xenodiagnostico) y serológicos en vacunados y controles, 12 y 24 meses post vacunación. Resultados esperados e importancia del proyecto: se espera conocer los principales eventos tempranos que participan en la eliminación de los parásitos en los animales vacunados, el efecto del stress sobre la vacunación y asimismo, la inmunogenicidad de la vacuna en perros de campo. Todo ello permitirá obtener información sobre la eficacia de la vacunación experimental y podría aportar una herramienta adicional contra la Enfermedad de Chagas, interfiriendo en la cadena epidemiológica en áreas endémicas.

Intravital visualization of hematopoietic stem cell and neutrophil behavior in long bones of mice

Magdeburg, Univ., Fak. für Naturwiss., Diss., 2011

"Morphologic, genetic, and biochemical characterisation of novel Heliobacter isolates from laboratory mice and tigers"

Magdeburg, Univ., Fak. für Naturwiss., Diss., 2012

Effects of neural nitric oxide synthase gene inactivation on the neurodocrine stress response in mice

Neural nitric oxide synthase, neuroendocrine stress response, forced swimming, nNOS KO mice, hypothalamus, adrenal gland

Analyse der translatorischen Probleme anhand des Originals „Of Mice and Men“ von John Steinbeck und den deutschen Übersetzungen von Elisabeth Rotten, Georg Hofer und Mirjam Pressler

Die Ziel- und Aufgabenstellung dieser Arbeit ist es, die Originalfassung des Romans „Of Mice and Men“ von John Steinbeck und die deutschen Übersetzungen von Elisabeth Rotten, Georg Hofer und Mirjam Pressler zu analysieren. Anschließend werden die literarischen Übersetzungen im Hinblick auf die damit verbundenen translatorischen Probleme und auf die jeweils gewählte Übersetzungsstrategie miteinander verglichen. Zum Schluss wird beurteilt, welche der verschiedenen Lösungsansätze für den deutschsprachigen Leser am adäquatesten sind.

Systematics of mice of the subgenus Akodon (Rodentia, Cricetidae) in southern South America, with the description of a new species / Bruce D. Patterson, Milton H. Gallardo, Kathy E. Freas.

n.s. no.23(1984)

The South American mice referred to Microryzomys and Thallomyscus, by Wilfred H. Osgood.

v.20:no.1(1933)

Mice of the Akodon boliviensis size class (Sigmodontinae, Cricetidae), with the description of two new species from Brazil / Philip Hershovitz.

n.s. no.57(1990)

The interaction of Gram negative bacteria and S. mansoni in mice with experimental Schistosomiasis

Animals (122 mice) were infected each with eighty cercariae of S. mansoni and subsequently challenged intravenously eight weeks later with the following gram-negative organisms. S. typhi, E. coli, Klebsiella-enterobacter species, Proteus mirabilis and Pseudomonas aeruginosa. Enumeration of bacteria in the liver, spleen and blood and S. mansoni from the portal sistem was performed from one to four weeks later in infected animals. A significant difference between infection produced by S. typhi and other gram negative organisms was observed: S. typhi persisted longer in the spleen and liver and could be recovered from S. mansoni worms up to three weeks following bacterial infection. Other gram negative bacteria disappeared from S. mansoni worms after two weeks of initial challenge. Additional animals (51 mice) infected with S. mansoni were given S. typhi, E. coli or sterile saline. After two weeks, animals were sacrificed and the recovery rate of worms from the portal system, and the mesenteric and hepatic oogram were determined. in animals infected with E. coli a significant decrease in the number of worms was observed compared to the saline control group; thirty worms were recovered in the control group compared to two worms in e. coli infected animals. In addition, the patterns of oviposition was significantly different in these latter animals suggesting complete inhibition of this process. Following S. typhi infection the difference in recovery of worms and pattern of oviposition was minimal. These findings suggest a difference in the interaction of various gram negative bacteria and S. mansoni and are consistent with the clinical observation of prolonged salmonella bacteremia in patients with schistosomiasis.

Hematological changes in mice experimentally infected with Trypanosoma Cruzi

Mice inoculated with trypanosoma cruzi display an intense thrombocytopenia which is more severe in animals infected with the Y than CL strain. In animals inoculated with a T. cruzi strain which induces chronic infection (Colombiana), the number of platelets decreases as parasitemia ascends, and then reverts to normal values as soon as the acute infection merges into the chronic phase. The mechanisms involved in the thrombocytopenia are still obscure and are likely to be related to more general phenomena affecting the host rather than to direct damage of platelets or precursor cells by parasitism. Anemia and leukopenia are also present in T. cruzi infected mice.