Differential regulation of CD8(+) T cell senescence in mice and men

Ali Akbar; MVD Soares; FJ Plunkett; Michael Salmon

doi:10.1016/S0047-6374(00)00198-6

Differential regulation of CD8(+) T cell senescence in mice and men

Ali Akbar, MVD Soares, FJ Plunkett, Michael Salmon

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Abstract

The cytotoxic CD8+ T cell population expands considerably during acute immune infection with virus. Most of these cells are removed by apoptosis at the end of the immune response. However, a balance has to be attained between clearance and retention of a memory population of cells, which respond more rapidly and efficiently to secondary encounter with the antigen. In this article, the role of apoptosis and in particular the development of replicative senescence as mechanisms which control this homeostatic balance are discussed. Although similar mechanisms regulate apoptosis in both humans and rodents, the available data suggests that replicative senescence may be controlled differently in these species, suggesting the there may be different constraints in the regulation of CD8+ T cell memory between different species.

Original language	English
Pages (from-to)	69-76
Number of pages	8
Journal	Mechanisms of Ageing and Development
Volume	121
DOIs	https://doi.org/10.1016/S0047-6374(00)00198-6
Publication status	Published - 20 Jan 2001

Keywords

telomeres
apoptosis memory
replicative senescence

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10.1016/S0047-6374(00)00198-6

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title = "Differential regulation of CD8(+) T cell senescence in mice and men",

abstract = "The cytotoxic CD8+ T cell population expands considerably during acute immune infection with virus. Most of these cells are removed by apoptosis at the end of the immune response. However, a balance has to be attained between clearance and retention of a memory population of cells, which respond more rapidly and efficiently to secondary encounter with the antigen. In this article, the role of apoptosis and in particular the development of replicative senescence as mechanisms which control this homeostatic balance are discussed. Although similar mechanisms regulate apoptosis in both humans and rodents, the available data suggests that replicative senescence may be controlled differently in these species, suggesting the there may be different constraints in the regulation of CD8+ T cell memory between different species.",

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T1 - Differential regulation of CD8(+) T cell senescence in mice and men

AU - Akbar, Ali

AU - Soares, MVD

AU - Plunkett, FJ

AU - Salmon, Michael

PY - 2001/1/20

Y1 - 2001/1/20

N2 - The cytotoxic CD8+ T cell population expands considerably during acute immune infection with virus. Most of these cells are removed by apoptosis at the end of the immune response. However, a balance has to be attained between clearance and retention of a memory population of cells, which respond more rapidly and efficiently to secondary encounter with the antigen. In this article, the role of apoptosis and in particular the development of replicative senescence as mechanisms which control this homeostatic balance are discussed. Although similar mechanisms regulate apoptosis in both humans and rodents, the available data suggests that replicative senescence may be controlled differently in these species, suggesting the there may be different constraints in the regulation of CD8+ T cell memory between different species.

AB - The cytotoxic CD8+ T cell population expands considerably during acute immune infection with virus. Most of these cells are removed by apoptosis at the end of the immune response. However, a balance has to be attained between clearance and retention of a memory population of cells, which respond more rapidly and efficiently to secondary encounter with the antigen. In this article, the role of apoptosis and in particular the development of replicative senescence as mechanisms which control this homeostatic balance are discussed. Although similar mechanisms regulate apoptosis in both humans and rodents, the available data suggests that replicative senescence may be controlled differently in these species, suggesting the there may be different constraints in the regulation of CD8+ T cell memory between different species.

KW - telomeres

KW - apoptosis memory

KW - replicative senescence

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DO - 10.1016/S0047-6374(00)00198-6

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VL - 121

SP - 69

EP - 76

JO - Mechanisms of Ageing and Development

JF - Mechanisms of Ageing and Development

ER -

Differential regulation of CD8(+) T cell senescence in mice and men

Abstract

Keywords

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