UMD Theses and Dissertations

Permanent URI for this collectionhttp://hdl.handle.net/1903/3

New submissions to the thesis/dissertation collections are added automatically as they are received from the Graduate School. Currently, the Graduate School deposits all theses and dissertations from a given semester after the official graduation date. This means that there may be up to a 4 month delay in the appearance of a given thesis/dissertation in DRUM.

More information is available at Theses and Dissertations at University of Maryland Libraries.

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2013 - 20173

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Subject: search.filters.subject.Innate Immunity

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    CHARACTERIZING THE INHIBITION OF INNATE IMMUNE SIGNALING BY MYCOBACTERIUM TUBERCULOSIS
    (2017) Ahlbrand, Sarah; Briken, Volker; Molecular and Cell Biology; Digital Repository at the University of Maryland; University of Maryland (College Park, Md.)
    Numerous cytokines are induced as a consequence of infection by Mycobacterium tuberculosis (Mtb), an intracellular pathogen that is responsible for millions of deaths each year. These cytokines play varied roles in eliciting and regulating the innate and adaptive immune responses against Mtb and often determine disease outcome. The pro-inflammatory cytokine interleukin 1β (IL-1β) is required for Mtb maintenance and clearance, as mice lacking the ability to produce IL-1β succumb very quickly to infection compared to infected wildtype mice. In contrast, interferon β (IFNβ) is largely thought to be detrimental to the host during Mtb infection based on collective studies in patients and mouse models. Both IL-1β and IFNβ are induced during Mtb infection, but here we demonstrate that Mtb has also evolved mechanisms to reduce their production and/or signaling. Previously, we’ve shown that Mtb can inhibit IL-1β production induced by the Absent in Melanoma 2 (AIM2) inflammasome. These findings were expanded upon by investigating the mechanisms by which Mtb inhibits AIM2 activation. A gain-of-function screen was also utilized in the non-pathogenic mycobacterial species Msmeg to identify Mtb genomic regions contributing to this phenomenon. In addition, we demonstrate that Mtb inhibits IFNβ signaling by inhibiting IFNβ-induced JAK1 and Tyk2 phosphorylation, leading to changes in the host type I interferon transcriptional profile. These studies provide insight into two previously undescribed mechanisms Mtb utilizes to manipulate the host immune response.
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    Interferense of Host Innate Immune Response by Hepatitis E Virus
    (2014) Nan, Yuchen; Zhang, Yanjin; Veterinary Medical Science; Digital Repository at the University of Maryland; University of Maryland (College Park, Md.)
    The host antiviral innate immunity mainly relies on host pattern recognition receptors (PRR) and downstream interferon (IFN) signaling. Host PRR for RNA viruses include Toll-like receptors (TLR) and Retinoic acid-inducible gene I (RIG-I) like receptors (RLR). Activation of both TLR and RLR pathways can eventually lead to the secretion of type I IFNs, which can modulate both innate and adaptive immune responses against viral pathogens, including hepatitis E virus (HEV). HEV causes acute hepatitis in humans and has been responsible for several outbreaks of hepatitis across the world. Currently, no commercial vaccine is available for the prevention of HEV infection in any country except China. HEV biology and pathogenesis as well as its responses to host innate immunity are poorly understood, though other hepatitis viruses, including the hepatitis A, B and C viruses, have been much better studied. In this study, how HEV interferes with IFN induction and IFN-activated signaling had been examined. Results showed that the protein encoded by HEV ORF1 can inhibit type I IFN synthesis and downstream JAK/STAT signaling pathway. However, the HEV ORF3 product is able to enhance RIG-I-mediated signaling to a certain extent. These data suggest that HEV proteins interfere with the host innate immune response and may exert the diverse roles depending on the stage and/or context of infection. These studies contribute to a better understanding of HEV pathogenesis and may facilitate a strategy development for the prevention and control of HEV infection.
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    Characterization of the West Nile virus pathogen associated molecular patterns
    (2013) German, Jennifer; Fredericksen, Brenda L; Cell Biology & Molecular Genetics; Digital Repository at the University of Maryland; University of Maryland (College Park, Md.)
    The recent emergence of West Nile virus (WNV) in the western hemisphere has been marked by an increase in severe neurological disease. The factors that contribute to this increase in pathogenicity are poorly understood, however, there is evidence that the host antiviral response plays a significant role in controlling WNV mediated disease. The innate antiviral response is mediated by a variety of pathogen recognition receptors, including RIG-I. Here, we analyzed the RIG-I mediated antiviral response to WNV infection. We identified multiple regions of the pathogenic WNV-NY genome and antigenome that act as pathogen associated molecular patterns (PAMPs) capable of stimulating the RIG-I response. Additionally, preliminary examination of the related, non-pathogenic WNV-MAD78 genome has revealed stimulatory regions that differ from those found in the WNV-NY genome. One of PAMP region, the 5'UTR, was analyzed further to elucidate the secondary structural elements present in the RNA, which may be contributing to the antiviral response. Similar, equally stimulatory structures were found in the 5'UTR of both the WNV-NY strain WNV-MAD78, indicating similar structures may be recognized for RIG-I activation. We also examined the role of DDX3, a DExD/H box helicase similar to RIG-I, in WNV infection. DDX3 appeared to co-localize with WNV protein and DDX3 expression was reduced at late points in infection, but DDX3 overexpression had no effect on viral replication or protein expression. Therefore, the exact role that DDX3 plays during the course of WNV infection remains unresolved. Taken together, our data suggests a specific structural requirement to activate the RIG-I mediated antiviral response.