Stem cell-like plasticity of naïve and distinct memory CD8+ T cell subsets

Christian Stemberger; Michael Neuenhahn; Friedemann E. Gebhardt; Matthias Schiemann; Veit R. Buchholz; Dirk H. Busch

doi:10.1016/j.smim.2009.02.004

Stem cell-like plasticity of naïve and distinct memory CD8⁺ T cell subsets

Christian Stemberger, Michael Neuenhahn, Friedemann E. Gebhardt, Matthias Schiemann, Veit R. Buchholz, Dirk H. Busch

Chair of Medical Microbiology, Immunology and Hygiene

Research output: Contribution to journal › Review article › peer-review

68 Scopus citations

Abstract

Most models regarding the 'clonal' origin of CD8⁺ T cell effector and memory subset diversification suggest that during the first contact of a naïve T cell with the priming antigen-presenting cell major decisions for subsequent differentiation are made. Data using novel single-cell T cell tracking technologies demonstrate that a single naïve CD8⁺ T cell can give rise to virtually all different subtypes of effector and memory T cells, and direct major determinants of subset diversification to the time period beyond the first cell division. Thereby, some 'stem cell-like' characteristics typical for naïve T cells are probably still maintained within distinct subsets of memory T cells. These observations have direct consequences for clinical applications like adoptive T cell therapy.

Original language	English
Pages (from-to)	62-68
Number of pages	7
Journal	Seminars in Immunology
Volume	21
Issue number	2
DOIs	https://doi.org/10.1016/j.smim.2009.02.004
State	Published - Apr 2009

Keywords

Adoptive T cell transfer
Memory stem cell
Single-cell transfer
T cell memory differentiation

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10.1016/j.smim.2009.02.004

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title = "Stem cell-like plasticity of na{\"i}ve and distinct memory CD8+ T cell subsets",

abstract = "Most models regarding the 'clonal' origin of CD8+ T cell effector and memory subset diversification suggest that during the first contact of a na{\"i}ve T cell with the priming antigen-presenting cell major decisions for subsequent differentiation are made. Data using novel single-cell T cell tracking technologies demonstrate that a single na{\"i}ve CD8+ T cell can give rise to virtually all different subtypes of effector and memory T cells, and direct major determinants of subset diversification to the time period beyond the first cell division. Thereby, some 'stem cell-like' characteristics typical for na{\"i}ve T cells are probably still maintained within distinct subsets of memory T cells. These observations have direct consequences for clinical applications like adoptive T cell therapy.",

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author = "Christian Stemberger and Michael Neuenhahn and Gebhardt, {Friedemann E.} and Matthias Schiemann and Buchholz, {Veit R.} and Busch, {Dirk H.}",

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AU - Stemberger, Christian

AU - Neuenhahn, Michael

AU - Gebhardt, Friedemann E.

AU - Schiemann, Matthias

AU - Buchholz, Veit R.

AU - Busch, Dirk H.

PY - 2009/4

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AB - Most models regarding the 'clonal' origin of CD8+ T cell effector and memory subset diversification suggest that during the first contact of a naïve T cell with the priming antigen-presenting cell major decisions for subsequent differentiation are made. Data using novel single-cell T cell tracking technologies demonstrate that a single naïve CD8+ T cell can give rise to virtually all different subtypes of effector and memory T cells, and direct major determinants of subset diversification to the time period beyond the first cell division. Thereby, some 'stem cell-like' characteristics typical for naïve T cells are probably still maintained within distinct subsets of memory T cells. These observations have direct consequences for clinical applications like adoptive T cell therapy.

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Stem cell-like plasticity of naïve and distinct memory CD8⁺ T cell subsets

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Keywords

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