The oncogene product Vav is a crucial regulator of primary cytotoxic T cell responses but has no apparent role in CD28-mediated co-stimulation

Penninger, Josef; Fischer, Klaus; Sasaki, Takehiko; Kozieradzki, I.; Lê, Jennifer; Tedford, Kerry; Bachmaier, Kurt; Ohashi, Pamela S.; Bachmann, Martin F.

doi:10.1002/(sici)1521-4141(199905)29:05<1709::aid-immu1709>3.0.co;2-o

Cited by 35 publications

(11 citation statements)

References 39 publications

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“…The difference in the ability of Vav1-deficient T cells to proliferate in vivo vs. in vitro may be due to the presence of costimulatory signals in the lymphoid organ, which are absent in a simplified in vitro proliferation assay. In other studies, examination of antiviral responses in Vav1-deficient mice showed decreased primary CD8 cytotoxic T cell responses, although these became normal following secondary restimulation in vitro (39).…”

Section: Vav1 In Peripheral T Cell Functionmentioning

confidence: 78%

Vav1: a key signal transducer downstream of the TCR

Tybulewicz¹,

Ardouin

Prisco

et al. 2003

Immunological Reviews

104

105

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Vav1 is a 95-kDa protein expressed in all hemopoietic cells that becomes rapidly tyrosine phosphorylated following T cell antigen receptor (TCR) stimulation. Vav1 contains multiple domains characteristic of signal transducing proteins, including a Dbl homology domain, a hallmark of a guanine nucleotide exchange factor (GEF) for Rho-family GTPases. Indeed Vav1 is a GEF for Rac1, Rac2 and RhoG, and it is activated following tyrosine phosphorylation. Generation of mice deficient in Vav1 has shown that it plays an important role in selection events within the thymus, including both positive and negative selection, consistent with Vav1 transducing TCR signals required to drive these processes. Furthermore, Vav1-deficient T cells are defective in TCR-induced proliferation and cytokine synthesis. Analysis of TCR signaling pathways in Vav1-deficient T cells and thymocytes has shown that Vav1 is required to transduce signals to the activation of a calcium flux, extracellular signal-regulated kinase (ERK) and the nuclear factor kappaB (NF-kappaB) transcription factor. Vav1 has also been shown to control the activation of phospholipase Cgamma1 (PLCgamma1) via both phosphoinositide-3-kinase (PI3K)-dependent and -independent pathways. Finally, Vav1 has been shown to transduce TCR signals to some but not all cytoskeleton-dependent pathways. In particular, Vav1 is required for efficient TCR-induced conjugate formation with antigen presenting cells (APCs), activation of the integrin leukocyte function-associated antigen-1 (LFA-1) and cell polarization.

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Section: Vav1 In Peripheral T Cell Functionmentioning

confidence: 78%

Vav1: a key signal transducer downstream of the TCR

Tybulewicz¹,

Ardouin

Prisco

et al. 2003

Immunological Reviews

104

105

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“…Vav-1 -/-mice have reduced numbers of both T and NK T cells, as well as defects in primary cytotoxic T cell responses [24]. Therefore, to generate Vav-1 -/-LAK populations comparable to wild type, before culture we first depleted CD4 + and CD8 + cells from the spleen.…”

Section: Discussionmentioning

confidence: 99%

Vav-1 regulates NK T cell development and NK cell cytotoxicity

2001

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“…[46][47][48][49][50] Vav-deficient T cells were shown to be defective in TCR-induced actin polymerization. 51,52 Low densities of agonist peptides or short-lived peptides induced a transient phosphorylation of Vav in T cells treated with inhibitory doses of peptides, which was accompanied by no detectable actin polymerization.…”

Section: Low-density Tcr Ligand and Apls And Intracellular Signallingmentioning

confidence: 99%

Suboptimal engagement of the T‐cell receptor by a variety of peptide–MHC ligands triggers T‐cell anergy

Sadegh‐Nasseri

Dalai

Ferris³

et al. 2009

Immunology

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Nearly 15 years of detailed investigations devoted to the understanding of the mechanism of APL function resulted in a wealth of information regarding TCR signalling at the membrane interface and the nature of intracellular signalling molecules. All studied antagonist and partial agonist peptide variants were thought to have identical anchor residues to the agonist peptides, and hence form stable complexes with MHC molecules. Thus it was logical to assume that their differences from the agonist must

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The oncogene product Vav is a crucial regulator of primary cytotoxic T cell responses but has no apparent role in CD28-mediated co-stimulation

Cited by 35 publications

References 39 publications

Vav1: a key signal transducer downstream of the TCR

Vav1: a key signal transducer downstream of the TCR

Vav-1 regulates NK T cell development and NK cell cytotoxicity

Suboptimal engagement of the T‐cell receptor by a variety of peptide–MHC ligands triggers T‐cell anergy

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