Viral Chemokine Alteration of Neutrophil Functions

病毒趋化因子改变中性粒细胞功能

• 批准号: 7940295
• 负责人: TIMOTHY E SPARER
• 金额: $ 2.27万
• 依托单位: UNIVERSITY OF TENNESSEE KNOXVILLE
• 依托单位国家: 美国
• 财政年份: 2008
• 资助国家: 美国
• 起止时间: 2008-03-01 至 2013-02-28
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7940295
• 关键词: Acquired Immunodeficiency Syndrome; Address; Adhesions; Apoptosis; Attenuated; Binding; Biological Process; Biological Response Modifiers; Body part; CXC Chemokines; Cell Adhesion Molecules; Cell physiology; Characteristics; Clinical; Collaborations; Complex; Cytomegalovirus; Cytomegalovirus Infections; Disease; Exocytosis; Family; Genes; Genome; Human; IL8 gene; IL8RA gene; IL8RB gene; Immune response; Immune system; Immunocompromised Host; In Vitro; Inbred BALB C Mice; Infection; Inflammatory; Inflammatory Response; Interleukin-8B Receptor; Knock-in Mouse; Letters; Leukocyte Trafficking; Libraries; Life Cycle Stages; Longevity; Mental Retardation; Mission; Modeling; Morbidity - disease rate; Mus; Neutrophil Activation; Normal Cell; Pathogenesis; Pathology; Patients; Pattern; Phagocytosis; Play; Porifera; Proteins; Public Health; Recombinants; Role; Signal Transduction; Site; Site-Directed Mutagenesis; Specificity; Swelling; Transgenic Organisms; Transplant Recipients; United States; United States National Institutes of Health; Variant; Viral; Viral Genes; Viral Pathogenesis; Virulence; Virulence Factors; Virulent; cell type; chemokine; chemokine receptor; combat; cytokine; fighting; fitness; flexibility; functional outcomes; hearing impairment; homologous recombination; in utero; in vivo; migration; monolayer; mouse model; neutrophil; novel; receptor; release of sequestered calcium ion into cytoplasm; response; uptake

DESCRIPTION (provided by applicant): Neutrophils provide the body's first line of defense against infection. They fight infections by, among other things, releasing chemokines or cytokines which initiate cascades of other immune mediators and cell types. Neutrophils themselves are first signaled to move to the site of infection via chemokines. Once they arrive at the infection site, the neutrophils are activated. This activation can take many forms: increased exocytosis and phagocytosis, extension of their life span, and alteration of adhesion molecules for enhancing their specificity and mobility. Although the rapid response and flexibility of neutrophils make them an integral part of the body's immune system, human cytomegalovirus (HCMV), ironically, may use neutrophil activation for its own evolutionary advantage. HCMV may use neutrophils for dissemination or for attracting other cell types within which HCMV can remain latent. Virulent HCMV produces a functional chemokine, vCXCL-1Tol, that can mimic the body's normal immune response by attracting and activating neutrophils, yet this chemokine is only 22% identical to the host ELR-CXC chemokine, Gro1. The gene for this viral chemokine is one of the most variable in the HCMV genome with the vCXCL-1 proteins from different isolates having as little as 32% identity with each other. Using viral chemokines from a transplant patient and AIDS patients, we will compare these viral chemokines to chemokines from virulent and attenuated CMV strains. The questions that we will address are: 1) Do these viral chemokines have unique binding and functional outcomes? 2) Do these differences relate to viral pathogenesis in vivo? We have expressed and isolated the vCXCL-1 proteins from four different clinical isolates representing divergence in the vCXCL-1 family. Our next step will be to assess the differences in viral chemokine receptor usage, binding and signaling characteristics, and cellular processes. Initially we will focus on the variant chemokine from the C956 strain, which has the least homology to vCXCL-1Tol and the chemokine from the avirulent Towne strain. We will then relate these in vitro differences to the role that these proteins play in viral dissemination and pathogenesis using murine CMV as a surrogate for the HCMV chemokine genes. By understanding how these novel viral chemokines function in vitro and in vivo, we will begin to understand more about the complex relationship between the CMV life cycle, its impact on neutrophil functions, and disease. Narrative: This proposal supports the NIH mission by contributing to better public health within the United States. HCMV infection/reactivation is a leading cause of morbidity in immunocompromised hosts as well as hearing loss and mental retardation following in utero infection. Understanding an additional mechanism that HCMV exploits for dissemination/survival will provide a new avenue for exploration of novel anti-virals to combat HCMV disease in immunocompromised hosts.

描述（由申请人提供）：中性粒细胞提供了人体抵抗感染的第一道防线。它们通过释放趋化因子或细胞因子来对抗感染，这些趋化因子或细胞因子启动其他免疫介质和细胞类型的级联反应。中性粒细胞本身首先通过趋化因子被告知移动到感染部位。一旦它们到达感染部位，中性粒细胞就会被激活。这种激活可以采取多种形式：增加胞吐作用和吞噬作用，延长其寿命，以及改变粘附分子以增强其特异性和流动性。尽管中性粒细胞的快速反应和灵活性使其成为人体免疫系统的组成部分，但具有讽刺意味的是，人类巨细胞病毒（HCMV）可能利用中性粒细胞活化来获得自身的进化优势。HCMV可以利用中性粒细胞进行传播或吸引其他细胞类型，其中HCMV可以保持潜伏。强毒HCMV产生一种功能性趋化因子vCXCL-1 Tol，它可以通过吸引和激活中性粒细胞来模拟人体的正常免疫反应，但这种趋化因子与宿主ELR-CXC趋化因子Gro 1只有22%相同。这种病毒趋化因子的基因是HCMV基因组中最可变的基因之一，来自不同分离株的vCXCL-1蛋白彼此具有低至32%的同一性。使用来自移植患者和艾滋病患者的病毒趋化因子，我们将这些病毒趋化因子与来自强毒和减毒CMV株的趋化因子进行比较。我们将解决的问题是：1）这些病毒趋化因子是否具有独特的结合和功能结果？2)这些差异是否与体内病毒发病机制有关？我们已经表达并分离了来自四种不同临床分离株的vCXCL-1蛋白，这些分离株代表vCXCL-1家族中的分歧。我们的下一步将是评估病毒趋化因子受体的使用，结合和信号特征，以及细胞过程的差异。最初，我们将集中在C956株的变体趋化因子，它与vCXCL-1 Tol和无毒Towne株的趋化因子具有最小的同源性。然后，我们将这些在体外的差异，这些蛋白质在病毒传播和发病机制中发挥的作用，使用鼠CMV作为HCMV趋化因子基因的替代品。通过了解这些新的病毒趋化因子如何在体外和体内发挥作用，我们将开始了解更多关于CMV生命周期，其对中性粒细胞功能的影响和疾病之间的复杂关系。叙述：该提案通过促进美国境内更好的公共卫生来支持NIH的使命。HCMV感染/再活化是免疫功能低下宿主发病以及子宫内感染后听力损失和智力迟钝的主要原因。了解HCMV传播/存活的另一种机制将为探索新的抗病毒药物以对抗免疫功能低下宿主中的HCMV疾病提供新的途径。