Abstract

Naive T lymphocytes travel to T-cell areas of secondary lymphoid organs in search of antigen presented by dendritic cells. Once activated, they proliferate vigorously, generating effector cells that can migrate to B-cell areas or to inflamed tissues. A fraction of primed T lymphocytes persists as circulating memory cells that can confer protection and give, upon secondary challenge, a qualitatively different and quantitatively enhanced response. The nature of the cells that mediate the different facets of immunological memory remains unresolved. Here we show that expression of CCR7, a chemokine receptor that controls homing to secondary lymphoid organs, divides human memory T cells into two functionally distinct subsets. CCR7- memory cells express receptors for migration to inflamed tissues and display immediate effector function. In contrast, CCR7+ memory cells express lymph-node homing receptors and lack immediate effector function, but efficiently stimulate dendritic cells and differentiate into CCR7- effector cells upon secondary stimulation. The CCR7+ and CCR7- T cells, which we have named central memory (TCM) and effector memory (TEM), differentiate in a step-wise fashion from naive T cells, persist for years after immunization and allow a division of labour in the memory response.

Keywords

Homing (biology)EffectorC-C chemokine receptor type 7Cell biologyBiologyImmunologyCytotoxic T cellChemokine receptorIL-2 receptorMemory T cellChemokineT cellImmune systemIn vitro

MeSH Terms

CellsCulturedHumansImmunologic MemoryInterferon-gammaL-SelectinLeukopoiesisLymphocyte ActivationLymphoid TissueReceptorsCCR7ReceptorsChemokineReceptorsLymphocyte HomingT-Lymphocyte Subsets

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Publication Info

Year
1999
Type
article
Volume
401
Issue
6754
Pages
708-712
Citations
5709
Access
Closed

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5709
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433
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4832
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Cite This

Federica Sallusto, Danielle Lenig, Reinhold Förster et al. (1999). Two subsets of memory T lymphocytes with distinct homing potentials and effector functions. Nature , 401 (6754) , 708-712. https://doi.org/10.1038/44385

Identifiers

DOI
10.1038/44385
PMID
10537110

Data Quality

Data completeness: 81%