Literature DB >> 12224512

Fatal attraction: cytomegalovirus-encoded chemokine homologs.

N Saederup1, E S Mocarski.   

Abstract

Members of the cytomegalovirus (CMV) subfamily of betaherpesviruses infecting primates and rodents encode divergent proteins with sequence characteristics and activities of chemokines, a class of small, secreted proteins that control leukocyte migration and trafficking behavior. Human CMV genes UL146 and UL147 encode proteins with sequence characteristics of CXC chemokines, whereas, murine CMV encodes a CC chemokine homolog (MCK-2). Human CMV UL146 encodes a neutrophil-attracting chemokine denoted viral CXC chemokine-1 (vCXCL1) that is as potent as host IL-8 and functions via the CXCR2 receptor, one of two human IL-8 receptors. Murine CMV MCK-2 is composed of a chemokine domain derived from open reading frame (ORF) m131 (and denoted MCK-1) as well as a domain derived from m129 that does not have sequence similarity to any known class of proteins. A synthetic version of murine CMV m131 (MCK-1) protein carries out many of the activities of a positive-acting chemokine, including transient release of intracellular calcium stores and cell adhesion of peritoneal macrophage populations. In the context of the viral genome and infection of the mouse host, the m131-m129 (MCK-2) gene product confers increased inflammation, higher levels of viremia, and higher titers of virus in salivary glands, consistent with a role in promoting dissemination by attracting an important mononuclear leukocyte population. Other characterized primate CMVs, but not other primate betaherpesviruses, encode gene products similar to human UL146 and UL147. Other characterized rodent CMVs encode a gene product similar to the murine CMV chemokine homolog, although not as a spliced gene product. Thus chemokines, like viral proteins that downmodulate MHC class I expression or have sequence homology to host MHC class I proteins, have evolved in primate and rodent CMVs to carry out an analogous set of immunomodulatory functions during infection of the host even though they arise from distinct origins.

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Year:  2002        PMID: 12224512     DOI: 10.1007/978-3-642-59421-2_14

Source DB:  PubMed          Journal:  Curr Top Microbiol Immunol        ISSN: 0070-217X            Impact factor:   4.291


  15 in total

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4.  Cytomegalovirus MCK-2 controls mobilization and recruitment of myeloid progenitor cells to facilitate dissemination.

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5.  Alveolar Macrophages Are a Prominent but Nonessential Target for Murine Cytomegalovirus Infecting the Lungs.

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7.  Human cytomegalovirus UL145 gene is highly conserved among clinical strains.

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8.  Selective modification of antigen-specific T cells by RNA electroporation.

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9.  Protein coding content of the UL)b' region of wild-type rhesus cytomegalovirus.

Authors:  Kristie L Oxford; Meghan K Eberhardt; Kai-Wen Yang; Lisa Strelow; Suzanne Kelly; Shan-Shan Zhou; Peter A Barry
Journal:  Virology       Date:  2008-02-20       Impact factor: 3.616

10.  Passive immunization reduces murine cytomegalovirus-induced brain pathology in newborn mice.

Authors:  Durdica Cekinović; Mijo Golemac; Ester Pernjak Pugel; Jelena Tomac; Luka Cicin-Sain; Irena Slavuljica; Russell Bradford; Sonja Misch; Thomas H Winkler; Michael Mach; William J Britt; Stipan Jonjić
Journal:  J Virol       Date:  2008-10-08       Impact factor: 5.103

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