Selective expression of IL-7 receptor on memory T cells identifies early CD40L-dependent generation of distinct CD8
            <sup>+</sup>
            memory T cell subsets

Huster, Katharina M.; Busch, Verena; Schiemann, Matthias; Linkemann, Kathrin; Kerksiek, Kristen M.; Wagner, Hermann; Busch, Dirk H.

doi:10.1073/pnas.0308054101

Cited by 428 publications

(467 citation statements)

References 33 publications

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“…In the model by Sallusto et al [11], CCR7 + CD62L + antigen-experienced CD8 T cells circulate through secondary lymphoid tissue and are termed central memory cells, while CCR7 -CD62L +/-effector memory CD8 T cells migrate to peripheral sites. However, the process of T cell differentiation in response to antigen is highly complex, and other cell surface receptors such as CD7, CD27, CD28, CD45RA, CCR5 and CD127 can be used to identify functionally distinct subsets of effector and memory T cells [12][13][14][15][16][17][18][19].…”

Section: Introductionmentioning

confidence: 99%

“…Most of these cells expressed CCR5, a chemokine receptor which enables homing to the inflammatory chemokines RANTES, MIP-1a and MIP1b [29]. A small proportion of the tonsil CXCR5 + CD8 T cells expressed the IL-7 receptor CD127, which, as data from murine models indicate, may be important for long-term memory T cell generation [15,16]. A majority of CXCR5 + CD8 T cells were CD57 -, but a clear subset with intermediate to high expression representing about a third of cells was also observed (Fig.…”

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confidence: 99%

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CXCR5⁺ CCR7^– CD8 T cells are early effector memory cells that infiltrate tonsil B cell follicles

et al. 2007

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Naive and central memory CD8 T cells use CCR7 to recirculate through T cell zones of secondary lymphoid organs where they can encounter antigen. Here we describe a subset of human CD8 T cells expressing CXCR5 which enables homing in response to CXCL13 produced within B cell follicles. CXCR5 + CD8 T cells were found in tonsil B cell follicles, and isolated cells migrated towards CXCL13 in vitro. They expressed CD27, CD28, CD45RO, CD69, and were CD7 low , and produced IFN-c and granzyme A but lacked perforin, a functional profile suggesting that these cells are early effector memory cells in the context of contemporary T cell differentiation models. Receptors important in the interaction with B cells, including CD70, OX40 and ICOS, were induced upon activation, and CXCR5 + CD8 T cells could to some extent support survival and IgG production in tonsil B cells. Furthermore, CXCR5 + CD8 T cells expressed CCR5 but no CCR7, suggesting a migration pattern distinct from that of follicular CD4 T cells. The finding that a subset of early effector memory CD8 T cells use CXCR5 to locate to B cell follicles indicates that MHC class I-restricted CD8 T cells are part of the follicular T cell population. IntroductionCD8 T cells are lymphocytes of the adaptive immune system which recognize viral and bacterial peptides presented by MHC class I molecules and are indispensable in the control of many intracellular infections [1]. When appropriately stimulated by antigen presented by dendritic cells (DC) in secondary lymphoid tissues, they proliferate vigorously, become effector cells, and upon resolution of infection a small population of antigen-specific CD8 T cells are maintained as long-lived memory cells [2][3][4]. A primary effector mechanism of CD8 T cells is the killing of infected cells via the targeted release of the lytic effector molecules perforin and granzymes, and via expression of death receptors. However, there is significant functional heterogeneity in CD8 T cells and they are also efficient in producing anti-viral and pro-inflammatory cytokines [5][6][7][8]. The effector mechanisms used may depend on the pathogen and on the type of cell or tissue that is infected [8].CD8 T cell responses involve the differentiation of naive T cells into distinct types of effector and memory cells [2, 3,9]. One approach to analyse a T cell response is to examine the expression of receptors that mediate homing of T cells, such as CD62L, which binds to glycosylation-dependent cell adhesion molecule 1 on [4,20,21]. CXCR5 is a chemokine receptor which is expressed on all B cells and on specialized subsets of DC and T cells [22]. It has only one known ligand, the chemokine CXCL13, mainly produced by stromal cells and follicular DC within B cell follicles [23][24][25]. CXCR5 + CD4 T cells, known as follicular homing T helper cells, are found in B cell follicles and contribute to the generation of effective humoral immune responses by supporting antibody production and isotype class switching [26,27]. However, some of the processes and mec...

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Section: Introductionmentioning

confidence: 99%

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confidence: 99%

CXCR5⁺ CCR7^– CD8 T cells are early effector memory cells that infiltrate tonsil B cell follicles

et al. 2007

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“…These are (i) a proliferation phase that involves the growth and differentiation of naïve CD8 + T cells into effector T cells; (ii) a contraction or transition phase that entails the transition from the large population of effector CD8 + T cells to a smaller population (≈ 5-10%) of long-lived CD8 + memory T (Tm) cells (2); and (iii) a maintenance phase that is comprised of long-term CD8 + Tm cell survival in the host. The long-lived CD8 + Tm cell population can be rapidly reactivated and expanded upon Ag restimulation for recall responses.…”

Section: Introductionmentioning

confidence: 99%

Defect of CD8+ Memory T Cells Developed in Absence of IL-12 Priming for Secondary Expansion

Moyana

et al. 2008

Cell Mol Immunol

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“…Although studies using LCMV-infected mice have shown that these two molecules can mark CD8 + memory cell precursors [26][27][28]31], other studies using peptide-pulsed DCs or peptide immunization have shown that IL-7R is not a marker for such precursors [38][39][40][41]. Antigen-presenting cells expressing thymic leukemia antigen TL can boost CD8αα expression by T cells, and CD8αα expression induces IL-7Rα expression [29].…”

Section: Discussionmentioning

confidence: 99%

“…3B). Since IL-7R and CD8αα have been reported to be early markers of memory CD8 + T cells [26][27][28][29][30][31], IL-7R and CD8aa expression were tracked using flow cytometry on CD8 + T cells after the initial inoculation. No increases in CD8 + IL-7R + or CD8αα + cells were detected in blood or spleen in any of the mice we tested over the first 14 days after the second initial vaccination (data not shown).…”

Section: Vaccination With Socs1-downregulated Bmdcs Enhanced Ova-specmentioning

confidence: 99%

SOCS1 downregulation in dendritic cells promotes memory T-cell responses

Aldrich

Sanders

Lapteva

et al. 2008

Vaccine

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SOCS1-1 is crucial for control of immune cell cytokine expression, including those cytokines known to enable memory T cell formation and homeostasis. In this study, we found that immunization with SOCS1-downregulated bone marrow-derived dendritic cells generated increased antigen-specific CD8 + T memory cells and antigen-specific responses, as measured by ELISPOT, CTL assays, serum ELISAs, and T-cell proliferation assays. Bone marrow-derived dendritic cells in which SOCS1 was downregulated expressed increased levels of surface IL-15Ra and thymic leukemia (TL) antigen, both of which support memory cell development. This work supports a crucial role for SOCS1 in regulation of dendritic cell-directed generation of memory T cell responses.

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Selective expression of IL-7 receptor on memory T cells identifies early CD40L-dependent generation of distinct CD8 ⁺ memory T cell subsets

Cited by 428 publications

References 33 publications

CXCR5⁺ CCR7^– CD8 T cells are early effector memory cells that infiltrate tonsil B cell follicles

CXCR5⁺ CCR7^– CD8 T cells are early effector memory cells that infiltrate tonsil B cell follicles

Defect of CD8+ Memory T Cells Developed in Absence of IL-12 Priming for Secondary Expansion

SOCS1 downregulation in dendritic cells promotes memory T-cell responses

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Selective expression of IL-7 receptor on memory T cells identifies early CD40L-dependent generation of distinct CD8 + memory T cell subsets

Cited by 428 publications

References 33 publications

CXCR5+ CCR7– CD8 T cells are early effector memory cells that infiltrate tonsil B cell follicles

CXCR5+ CCR7– CD8 T cells are early effector memory cells that infiltrate tonsil B cell follicles

Defect of CD8+ Memory T Cells Developed in Absence of IL-12 Priming for Secondary Expansion

SOCS1 downregulation in dendritic cells promotes memory T-cell responses

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Selective expression of IL-7 receptor on memory T cells identifies early CD40L-dependent generation of distinct CD8 ⁺ memory T cell subsets

CXCR5⁺ CCR7^– CD8 T cells are early effector memory cells that infiltrate tonsil B cell follicles

CXCR5⁺ CCR7^– CD8 T cells are early effector memory cells that infiltrate tonsil B cell follicles