An Epithelial Cell Line That Can Stimulate Alloproliferation of Resting CD4+ T Cells, But Not After IFN-γ Stimulation

McCormack, Ann; Moyes, David L.; Shi, Yun; Fabre, John W.; Yacoub, Magdi H.; Rose, Marlene L.

doi:10.4049/jimmunol.165.2.734

Cited by 11 publications

(9 citation statements)

References 44 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These data make it unlikely that an anergy defect in T cells is responsible for making p21 -/-mice prone to lupus erythematosus [24][25][26]. Moreover, p21 -/-mice on a different background were not lupus-prone [38]. The defects of T and B cells leading to loss of self-tolerance in lupus are complex and have only partially been characterized [39].…”

Section: Discussionmentioning

confidence: 99%

The cyclin‐dependent kinase inhibitors p27^Kip1 and p21^Cip1 are not essential in T cell anergy

Verdoodt

Blazek²,

Rauch³

et al. 2003

Eur J Immunol

View full text Add to dashboard Cite

Recent evidence suggests that the cyclin-dependent kinase (Cdk) inhibitors p27 Kip1 and p21 Cip1 are important factors in T cell anergy, but it has remained unclear whether anergy can be induced in their absence. We therefore induced anergy by stimulation of purified T cells from wild-type, p21Cip1-/-, and p27Kip1-/-mice with anti-CD3 antibodies. Anergic wild-type T cells were arrested in the G1 phase of the cell cycle with a high p27Kip1 protein level and low Cdk2 activity. In p27 -/-and p21 -/-T cells, the pattern of protein expression was preserved, but Cdk2 activity was increased. To confirm the in vivo relevance of these data, anergy was induced by repeated injection of mice with staphylococcal enterotoxin B (SEB), which leads to partial deletion of the responsive V g 8 + T cell population and anergy in the remaining T cells. p21 -/-mice and wild-type mice reacted similarly to this treatment. p27 -/-mice showed reduced deletion of SEB-responsive T cells, but persisting T cells were anergic. These data indicate that other cell cycle regulators contribute to the cell cycle arrest of anergic T cells, as neither Cdk inhibitor is required for the induction of anergy.

show abstract

Section: Discussionmentioning

confidence: 99%

The cyclin‐dependent kinase inhibitors p27^Kip1 and p21^Cip1 are not essential in T cell anergy

Verdoodt

Blazek²,

Rauch³

et al. 2003

Eur J Immunol

View full text Add to dashboard Cite

show abstract

“…HLA-DR expression was induced in Eahy.926 by permanent transfection with the class II transactivator (CIITA) (19) or induced in aortic EC or human heart microvascular EC by interferon (IFN)-␥ pretreatment (20,21). HLA-DR-restricted CD4ϩ T cells that could proliferate to EC expressing the appropriate HLA-DR molecules are referred to as ECspecific T cells, and those that did not were termed third party T cells.…”

mentioning

confidence: 99%

“…cells were cultured in Dulbecco's modified Eagle's medium (Sigma, Dorset, UK) containing 10% FCS (Sigma) and 0.04% hypoxanthine, aminopterin, thymidine (Invitrogen, Paisley, UK) and passaged weekly. Eahy.926 that was permanently transfected with CIITA (EahyCIITA) (19) was cultured as described previously in this report, with 0.2 mg/mL geneticin (Invitrogen). Human aortic EC and human heart microvascular EC (HHMEC) were isolated from donor aorta or ventricle, respectively.…”

mentioning

confidence: 99%

Effect of Cognate Human CD4+ T Cell and Endothelial Cell Interactions Upon Chemokine Production

2004

Self Cite

View full text Add to dashboard Cite

show abstract

“…This cell line has been shown to respond to cytokines and support transendothelial migration of leukocytes in a similar manner as primary endothelial cells (44). Untreated Eahy.926 do not express MHC class II (44), but MHC class II expression can be induced by permanent transfection with the MHC class II trans-activator CIITA (EahyCIITA) or by 4-day treatment of Eahy.926 with IFN-␥ (45). We have previously shown that transfection of Eahy.926 with CIITA induced MHC class II expression (DR13, DR11) whereas other molecules, including ICAM-1 and VCAM-1, which may be involved in transmigration, are not up-regulated (45).…”

mentioning

confidence: 99%

“…Untreated Eahy.926 do not express MHC class II (44), but MHC class II expression can be induced by permanent transfection with the MHC class II trans-activator CIITA (EahyCIITA) or by 4-day treatment of Eahy.926 with IFN-␥ (45). We have previously shown that transfection of Eahy.926 with CIITA induced MHC class II expression (DR13, DR11) whereas other molecules, including ICAM-1 and VCAM-1, which may be involved in transmigration, are not up-regulated (45). In this way we have been able to dissect the effects of MHC class II expression on T cell migration from other proinflammatory effects that might be mediated by IFN-␥.…”

mentioning

confidence: 99%

IFN-γ Reverses the Stop Signal Allowing Migration of Antigen-Specific T Cells into Inflammatory Sites

Tay

McCormack

Rose

2003

The Journal of Immunology

Self Cite

View full text Add to dashboard Cite

In humans the majority of endothelial cells (EC) constitutively express MHC class II Ags. We know that in vitro ECs can activate CD45RO+ B7-independent CD4+ T cells to proliferate and produce IL-2. The in vivo correlate of this T cell response is not known, and here we have explored whether endothelial expression of MHC class II Ags affects the transendothelial migration of alloreactive CD4+ CD45RO+ B7-independent T cells. Alloreactive CD4+ T cell clones and lines were generated against HLA-DR11, DR13, DR4, and DR1 MHC Ags, and their rates of migration across untreated EC line Eahy.926 (MHC class II negative) or Eahy.926 transfected with CIITA (EahyCIITA) to express DR11 and DR13 were investigated. The migrations of EahyCIITA-specific T cell clones and lines were retarded in a DR-specific manner, and retardation was reversed in the presence of mAb to DR Ag. When investigating the ability of T cells to proliferate in response to EahyCIITA before and after transmigration, migrated cells were still able to proliferate, but the frequency of EahyCIITA-specific cells was much reduced compared with that of nonmigrated cells. The use of fluorescently labeled T cells revealed that specific cells become trapped within the endothelial monolayer. Pretreatment of EahyCIITA with IFN-γ restored the ability of DR11- or DR13-specific T cells to transmigrate and proliferate, thus abrogating DR-specific retardation. We conclude that cognate interaction between T cells and endothelial MHC class II initiates a stop signal possibly similar to an immunological synapse, but this is overcome in an inflammatory milieu.

show abstract

An Epithelial Cell Line That Can Stimulate Alloproliferation of Resting CD4+ T Cells, But Not After IFN-γ Stimulation

Cited by 11 publications

References 44 publications

The cyclin‐dependent kinase inhibitors p27^Kip1 and p21^Cip1 are not essential in T cell anergy

The cyclin‐dependent kinase inhibitors p27^Kip1 and p21^Cip1 are not essential in T cell anergy

Effect of Cognate Human CD4+ T Cell and Endothelial Cell Interactions Upon Chemokine Production

IFN-γ Reverses the Stop Signal Allowing Migration of Antigen-Specific T Cells into Inflammatory Sites

Contact Info

Product

Resources

About

An Epithelial Cell Line That Can Stimulate Alloproliferation of Resting CD4+ T Cells, But Not After IFN-γ Stimulation

Cited by 11 publications

References 44 publications

The cyclin‐dependent kinase inhibitors p27Kip1 and p21Cip1 are not essential in T cell anergy

The cyclin‐dependent kinase inhibitors p27Kip1 and p21Cip1 are not essential in T cell anergy

Effect of Cognate Human CD4+ T Cell and Endothelial Cell Interactions Upon Chemokine Production

IFN-γ Reverses the Stop Signal Allowing Migration of Antigen-Specific T Cells into Inflammatory Sites

Contact Info

Product

Resources

About

The cyclin‐dependent kinase inhibitors p27^Kip1 and p21^Cip1 are not essential in T cell anergy

The cyclin‐dependent kinase inhibitors p27^Kip1 and p21^Cip1 are not essential in T cell anergy