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Latent Cytomegalovirus-Driven Recruitment of Activated CD4+ T Cells Promotes Virus Reactivation.

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TLDR
In this paper, the effect of HCMV latent infection on the secretome of CD14+ monocytes was analyzed, identifying an upregulation of both CCL8 and CXCL10 chemokines in the CD 14+ latency-associated secretome.
Abstract
Human cytomegalovirus (HCMV) infection is not cleared by the initial immune response but persists for the lifetime of the host, in part due to its ability to establish a latent infection in cells of the myeloid lineage. HCMV has been shown to manipulate the secretion of cellular proteins during both lytic and latent infection; with changes caused by latent infection mainly investigated in CD34+ progenitor cells. Whilst CD34+ cells are generally bone marrow resident, their derivative CD14+ monocytes migrate to the periphery where they briefly circulate until extravasation into tissue sites. We have analyzed the effect of HCMV latent infection on the secretome of CD14+ monocytes, identifying an upregulation of both CCL8 and CXCL10 chemokines in the CD14+ latency-associated secretome. Unlike CD34+ cells, the CD14+ latency-associated secretome did not induce migration of resting immune cell subsets but did induce migration of activated NK and T cells expressing CXCR3 in a CXCL10 dependent manner. As reported in CD34+ latent infection, the CD14+ latency-associated secretome also suppressed the anti-viral activity of stimulated CD4+ T cells. Surprisingly, however, co-culture of activated autologous CD4+ T cells with latently infected monocytes resulted in reactivation of HCMV at levels comparable to those observed using M-CSF and IL-1β cytokines. We propose that these events represent a potential strategy to enable HCMV reactivation and local dissemination of the virus at peripheral tissue sites.

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An immunologist’s guide to immunosenescence and its treatment

TL;DR: In this article , the authors focused on the biological and clinical meaning of immunosenescence and discussed the role of changes in lifestyle as a potential therapeutic approach, and pointed out that age is only part of the problem.
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Evasion of the Host Immune Response by Betaherpesviruses.

TL;DR: In this article, the authors highlight the complex interplay between betaherpesviruses and the human immune response, focusing on protein function and explore methods by which the immune system first responds to beta-herpesvirus infection as well as mechanisms by which viruses subvert normal cellular functions to evade the immune systems and facilitate viral latency, persistence, and reactivation.
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A Viral Long Non-Coding RNA Protects against Cell Death during Human Cytomegalovirus Infection of CD14+ Monocytes

TL;DR: A novel way in which HCMV protects infected monocytes from pro-death signals to optimise latent carriage is demonstrated, and a role for the β2.7 viral transcript is identified, the most abundantly expressed viral RNA during latency but for which no latency-associated function has ever been ascribed.
Journal ArticleDOI

Advances in Model Systems for Human Cytomegalovirus Latency and Reactivation

TL;DR: This review will discuss the details and challenges of various models including hematopoietic progenitor cells, monocytes, cell lines, and humanized mice and highlight the utility and functional differences between these models and the necessary experimental design required to define latency and reactivation.
References
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TL;DR: These results identify cytokines, antigen-presenting cells and microbial products that promote the polarization of human TH-17 cells and emphasize an important difference in the requirements for the differentiation of TH- 17 cells in humans and mice.
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Blood monocytes: development, heterogeneity, and relationship with dendritic cells.

TL;DR: Functional characterization of monocytes is in progress in humans and rodents and will provide a better understanding of the pathophysiology of inflammation.
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The chemokine receptors CXCR3 and CCR5 mark subsets of T cells associated with certain inflammatory reactions.

TL;DR: Results demonstrate that the chemokine receptor CXCR3 and CCR5 are markers for T cells associated with certain inflammatory reactions, particularly TH-1 type reactions, and appear to identify subsets of T cells in blood with a predilection for homing to these sites.
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Broadly targeted human cytomegalovirus-specific CD4+ and CD8+ T cells dominate the memory compartments of exposed subjects

TL;DR: The first glimpse of the total human T cell response to a complex infectious agent is provided and insight into the rules governing immunodominance and cross-reactivity in complex viral infections of humans is provided.
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