Atherosclerosis

1997

DOI: 10.1016/s0021-9150(97)00135-4

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Costimulatory molecules in human atherosclerotic plaques: an indication of antigen specific T lymphocyte activation

Onno J. de Boer

¹

,

²

,

Allard C. van der Wal

³

et al.

Abstract: Atherosclerotic plaques contain inflammation, composed largely of macrophages and lymphocytes. A proportion of lymphocytes shows signs of activation, but the question arises whether they are activated in an antigen specific way. The expression of costimulatory molecules-receptors that provide accessory signals during antigen-specific activation is a prerequisite for such a condition. This aspect of inflammation in atherosclerotic lesions has not been investigated. Human arterial segments with diffuse intimal t… Show more

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Discussion1

Regulation Of Proatherogenic Adaptive Immune Responses1

Cd281

The Journal Of Histochemistry and Cytochemistry Multiple Immun1

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Cited by 76 publications

(57 citation statements)

References 32 publications

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“…Whereas production of helper cell-derived cytokines as IL-21 and IL-2 is limited to the antigenic activation phase, IL-15 can be produced by a number of lymphoid and nonlymphoid cells (44). It is feasible that viruses elicit distinct helper cell cytokine profiles by differential infection of APC and by different target cell tropism, thereby also determining the number and phenotype of CD8 ϩ T cells during the memory phase (45)(46)(47).…”

Section: Discussionmentioning

confidence: 99%

The Size and Phenotype of Virus-Specific T Cell Populations Is Determined by Repetitive Antigenic Stimulation and Environmental Cytokines

¹

,

²

,

et al. 2004

The Journal of Immunology

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Based on the expression of the TNFR SFP CD27, two Ag-primed CD8+ T cell subsets can be discerned in the circulation of healthy individuals: CD27+ T cells that produce a variety of cytokines but do not display immediate cytolytic activity; and cytotoxic CD27− T cells, which secrete only IFN-γ and TNF-α. The mechanism that controls the generation of these different phenotypes is unknown. We show that CMV reactivation not only increases the number of virus-specific T cells but also induces their transition from a CD27+ to a CD27− phenotype. In support of a relation between pool size and phenotype in a cohort of latently infected individuals, the number of Ag-specific CD27− CD8+ T cells was found to be linearly related to the total number of CMV-specific CD8+ T cells. In vitro studies revealed that the acquisition of the CD27− phenotype on CMV-specific T cells depended on the interaction of CD27 with its cellular ligand, CD70. Expression of CD70 was proportional to the amount of antigenic stimulation and blocked by the CD4+ T cell-derived cytokine IL-21. Thus, induction of CD70, which may vary in distinct viral infections, appears to be a key factor in determining the size and phenotype of the CMV-specific T cell population in latently infected individuals.

“…Whereas production of helper cell-derived cytokines as IL-21 and IL-2 is limited to the antigenic activation phase, IL-15 can be produced by a number of lymphoid and nonlymphoid cells (44). It is feasible that viruses elicit distinct helper cell cytokine profiles by differential infection of APC and by different target cell tropism, thereby also determining the number and phenotype of CD8 ϩ T cells during the memory phase (45)(46)(47).…”

Section: Discussionmentioning

confidence: 99%

The Size and Phenotype of Virus-Specific T Cell Populations Is Determined by Repetitive Antigenic Stimulation and Environmental Cytokines

¹

,

²

,

et al. 2004

The Journal of Immunology

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Based on the expression of the TNFR SFP CD27, two Ag-primed CD8+ T cell subsets can be discerned in the circulation of healthy individuals: CD27+ T cells that produce a variety of cytokines but do not display immediate cytolytic activity; and cytotoxic CD27− T cells, which secrete only IFN-γ and TNF-α. The mechanism that controls the generation of these different phenotypes is unknown. We show that CMV reactivation not only increases the number of virus-specific T cells but also induces their transition from a CD27+ to a CD27− phenotype. In support of a relation between pool size and phenotype in a cohort of latently infected individuals, the number of Ag-specific CD27− CD8+ T cells was found to be linearly related to the total number of CMV-specific CD8+ T cells. In vitro studies revealed that the acquisition of the CD27− phenotype on CMV-specific T cells depended on the interaction of CD27 with its cellular ligand, CD70. Expression of CD70 was proportional to the amount of antigenic stimulation and blocked by the CD4+ T cell-derived cytokine IL-21. Thus, induction of CD70, which may vary in distinct viral infections, appears to be a key factor in determining the size and phenotype of the CMV-specific T cell population in latently infected individuals.

“…Costimulatory and coinhibitory pathways have significant effects on atherosclerotic lesion development, as recently reviewed (133). The costimulators CD80, CD86, CD275, and CD252 can be detected on lesional macrophages in human and mouse lesions (134)(135)(136)(137)(138), as can their receptors on lesional T cells. A proatherogenic effect has been demonstrated for CD80, CD86, and CD252 (136,137,139) as well as for CD137, a costimulatory receptor expressed on T lymphocytes (138,140).…”

Section: Regulation Of Proatherogenic Adaptive Immune Responsesmentioning

confidence: 99%

Adaptive immunity in atherogenesis: new insights and therapeutic approaches

et al. 2013

J. Clin. Invest.

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Many remarkable advances have improved our understanding of the cellular and molecular events in the pathogenesis of atherosclerosis. Chief among these is the accumulating knowledge of how the immune system contributes to all phases of atherogenesis, including well-known inflammatory reactions consequent to intimal trapping and oxidation of LDL. Advances in our understanding of the innate and adaptive responses to these events have helped to clarify the role of inflammation in atherogenesis and suggested new diagnostic modalities and novel therapeutic targets. Here we focus on recent advances in understanding how adaptive immunity affects atherogenesis.

“…Ϫ T cells in atherosclerotic plaques, an immunohistochemical study found that only a very low percentage (Ϸ10%) of T cells in human plaques express the CD28 antigen, 16 suggesting that many of the CD4 ϩ cells would result in CD28 Ϫ . In rheumatoid arthritis, levels of CD4 ϩ…”

Section: Cd28mentioning

confidence: 99%

A Tale of Two Diseases

²

1999

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A cute coronary syndromes are responsible for most of the morbidity and mortality caused by coronary atherosclerosis. Both unstable angina and acute myocardial infarction are characterized by coronary thrombosis, usually caused by rupture or fissuring of a coronary plaque. Yet the occurrence of plaque rupture and coronary thrombosis is not related to severity of coronary plaques, and functional factors other than the mere presence of atherosclerotic lesions play an important role.

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