Spelling suggestions: "subject:"rhesus monkey""
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Sexually Differentiated Object Preference in Rhesus Monkeys (Macaca mulatta)Berkowitz, Jamie 01 January 2009 (has links) (PDF)
Children have strong preferences for sex-typed toys; boys prefer trucks, whereas girls prefer dolls. These preferences appear to be driven by complex interactions of hormones and the socio-cultural environment. The relative contribution of each of these factors in children is impossible to isolate given ethical limitations. Non-human primate species afford the opportunity to examine preferences in the absence of societal values and influences that children experience. In two previous studies with non-human primates, one with vervet monkeys and one with rhesus monkeys, monkeys showed sex-typed object preferences that paralleled those of children. However, several uncontrolled variables could have influenced these preferences. Our study considered object characteristics and we controlled for possible color preferences. We also tested monkeys individually to eliminate the effects of social facilitation and dominance rank. In experiment 1, monkeys were given a choice between similar objects of different colors (Phase A) and moving vs. non-moving objects (Phase B). In experiment 2, monkeys were given a choice between dolls and trucks (Phase A) and subsequent phases looked at the influence of moving wheels (Phase B) and hardness (Phase C). Contrary to previous findings, monkeys did not show sex-typed object preferences. Instead, the monkeys preferred blue objects, hard PVC objects such as trucks and hard dolls, and dolls with wheels. The influence of previous reward based cognitive testing, familiarity of substrate materials, and rearing condition are considered as possible explanations for these findings.
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Clonal Analysis of Mucosal SIV-Specific CD8+ T Cell ResponsesSircar, Piya January 2011 (has links)
CD8+ T cells responses are critical in the immune defense against human immunodeficiency virus (HIV) and simian immunodeficiency virus (SIV) infection. A major challenge for vaccine development is that HIV/SIV can rapidly mutate to escape containment by the CD8+ T cell response. Therefore, optimal virus control by a vaccine will likely require clonally diverse CD8+ T cells capable of recognizing mutant viruses. Mucosal tissues play a fundamental role in early HIV/SIV pathogenesis by serving as the site for viral entry, CD4+ T cell depletion, and a reservoir for viral replication. Vaccine strategies that induce effective mucosal immunity will likely be critical for protection against HIV/SIV. We examined the SIV Gag p11C-specific CD8+ T cell responses in peripheral blood, gastrointestinal (GI) mucosal and lung mucosal tissues of rhesus monkeys expressing the MHC class I molecule Mamu-A*01. We first investigated the clonal composition of this cell population during the acute and chronic phases of SIVmac infection. We showed that there is a narrowing of the clonal repertoire from acute to chronic infection and the same clonal populations of virus-specific CD8+ T cells are present in the systemic and mucosal compartments of chronically SIV-infected animals. These data indicated that virus-specific CD8+ T cells establish broadly distributed immune responses. Next, we examined the clonal diversity of systemic and mucosal p11C-specific CD8+ T cells induced by prime-boost vaccination. We found that systemic prime-boost vaccination induced clonally diverse p11C-specific populations in mucosal tissues. There were high levels of clonal sharing between systemic and mucosal compartments soon after vaccination. However, later following vaccination there was decreased clonal sharing between the GI mucosa and the systemic circulation. We showed that this was due to limited trafficking of p11C-specific CD8+ T cells to the GI mucosa following vaccination. Overall, these studies indicate that following SIV infection and systemic vaccination the same p11C-specific clones are present in mucosal and systemic compartments. Moreover, the apparent immune compartmentalization is a consequence of differences in cell trafficking between systemic and mucosal CD8+ T cells. These observations have important implications for the design of HIV vaccines that generate effective mucosal immunity.
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Developmental Predictors of Adolescent Alcohol Intake: A Nonhuman Primate ModelWood, Elizabeth Katherine 12 June 2020 (has links)
Alcohol abuse is one of the costliest human health problems in the United States. Studies assessing the etiology of alcohol use disorders (AUDs) in adulthood suggest that these disorders are predicted by trait-like differences, such as low or impaired central serotonin or temperamental anxiety. Few studies, however, have assessed neonatal, infant, and adolescent characteristics that lead to alcohol abuse in adolescence. Given that the expression of AUDs is rooted in biological processes, the set of studies presented in this work investigate the early origins of excessive alcohol use in adolescence, with an overall goal of identifying risk factors that may aid in prevention or intervention efforts to deter future alcohol abuse. Due to their evolutionary similarities, as well as similarities in their patterns of alcohol consumption, these studies utilize a nonhuman primate model (Macaca mulatta). A series of three studies investigating neonatal, infant, and adolescent predictors of adolescent alcohol intake were conducted. In study one, we assessed the relationship between neurobehavioral measures at two weeks of life and voluntary alcohol intake in adolescence. In study two, we assessed the relationship between behaviors that reflect an anxiety-like temperament in the first six months of life and excessive alcohol intake in adolescence. In study three, we investigated the relationship between infant and adolescent trait-like stress-induced cortisol and adolescent anxiety-like behaviors and alcohol intake in adolescence. The findings from this set of studies lends itself to an increased understanding of early-life, biologically-based predictors of excessive alcohol intake in adolescence and provides critical information to establishing early interventions for individuals at risk for the development of later AUDs.
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Bedeutung der mikrobiellen Transmission im SIV-Rhesusaffen-Tiermodell für die HIV/AIDS-Pathogenese / Microbial translocation in the SIV rhesus monkey model for HIV/AIDS pathogenesisLeinert, Christoph Alexander 21 February 2011 (has links)
No description available.
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Evaluating The Kinetics Of Proinflammatory Immune Responses To Simian Immunodeficiency Virus Infection In Rhesus Macaques By Transcriptional AnalysisUnknown Date (has links)
Understanding the host response immediately following mucosal HIV-1
infection will be pivotal in determining whether the immune response induced by
a vaccine will successfully sense and control viral replication. In order for
effective vaccine strategies and modalities to be developed, these earliest
immunological events must be fully assessed in a non-biased manner.
Nonhuman primates (NHP), specifically Rhesus macaques (RM), serve as a
model to investigate the immunological landscape immediately post-challenge
and to define the spatiotemporal path of simian immunodeficiency virus (SIV).
SIV infection of RM serves as a model of human HIV infection as it recapitulates
many of the virological, immunological, and pathological features of HIV infection in the human host. In this thesis I will test the hypothesis whether
transcriptional analysis will allow a sensitive measure of the early innate immune
responses that accompany detection of the SIV virus in the periphery. I have
determined that an early inflammatory profile arises early in tissues proximal to
the challenge site that precedes widespread immune activation and the systemic
antiviral interferon response. This study defines in detail the spatiotemporal
relationship between virus and host immune response and may be a valuable
resource in guiding future vaccine design strategies. / Includes bibliography. / Thesis (M.S.)--Florida Atlantic University, 2016. / FAU Electronic Theses and Dissertations Collection
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Metagenomics in One Health — from standardization to targeted applicationHallmaier-Wacker, Luisa 10 May 2019 (has links)
No description available.
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Charakterisierung der angeborenen Immunantwort in SIV-infizierten Rhesusaffen / Characterization of the innate immune response in SIV-infected rhesus monkeysMußil, Bianka 30 June 2009 (has links)
No description available.
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