Fibroblasts from different sites may promote or inhibit recruitment of flowing lymphocytes by endothelial cells

McGettrick, Helen M.; Smith, Emily; Filer, Andrew; Kissane, Stephen; Salmon, M; Buckley, Christopher D.; Rainger, G. Ed; Nash, Gerard B.

doi:10.1002/eji.200838232

Cited by 79 publications

(180 citation statements)

References 49 publications

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“…In agreement with previous observations (7,8), we found that a function-blocking Ab against CXCR3 nearly abolished the adhesion of flowing PBL to TNF-and IFN-stimulated EC (Fig. 2A).…”

Section: Vascular Ec Stimulated With Tnf and Ifn Preferentially Recrusupporting

confidence: 93%

“…There is also a strong presumption that chemokine signals are sufficient to promote lymphocyte migration over and through the endothelial monolayer and into inflamed tissue. In the case of EC treatment with TNF plus IFN, chemokines acting through the lymphocyte-borne receptor CXCR3 have been shown to stabilize attachment, but the signals inducing transendothelial migration have not been defined (7,8). Transendothelial migration of T cells has been observed within minutes of adhesion to EC activated with TNF (where blockade of b 2 integrins was inhibitory) (4), with TNF plus IFN (7), and for EC stimulated with TNF and to which stromal-derived factor-1a (CXCL12) or CCL19 (ELC) had been added to the EC surface (9).…”

mentioning

confidence: 99%

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Prostaglandin D2 Regulates CD4+ Memory T Cell Trafficking across Blood Vascular Endothelium and Primes These Cells for Clearance across Lymphatic Endothelium

Ahmed

McGettrick

Yates

et al. 2011

The Journal of Immunology

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Memory lymphocytes support inflammatory and immune responses. To do this, they enter tissue via blood vascular endothelial cells (BVEC) and leave tissue via lymphatic vascular endothelial cells (LVEC). In this study, we describe a hierarchy of signals, including novel regulatory steps, which direct the sequential migration of human T cells across the blood and the lymphatic EC. Cytokine-stimulated (TNF and IFN) human BVEC preferentially recruited memory T cells from purified PBL. Lymphocyte recruitment from flow could be blocked using a function-neutralizing Ab against CXCR3. However, a receptor antagonist directed against the PGD2 receptor DP2 (formerly chemoattractant receptor-homologous molecule expressed on Th2 cells) inhibited transendothelial migration, demonstrating that the sequential delivery of the chemokine and prostanoid signals was required for efficient lymphocyte recruitment. CD4+ T cells recruited by BVEC migrated with significantly greater efficiency across a second barrier of human LVEC, an effect reproduced by the addition of exogenous PGD2 to nonmigrated cells. Migration across BVEC or exogenous PGD2 modified the function, but not the expression, of CCR7, so that chemotaxis toward CCL21 was significantly enhanced. Thus, chemokines may not regulate all stages of lymphocyte migration during inflammation, and paradigms describing their trafficking may need to account for the role of PGD2.

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“…In agreement with previous observations (7,8), we found that a function-blocking Ab against CXCR3 nearly abolished the adhesion of flowing PBL to TNF-and IFN-stimulated EC (Fig. 2A).…”

Section: Vascular Ec Stimulated With Tnf and Ifn Preferentially Recrusupporting

confidence: 93%

mentioning

confidence: 99%

Prostaglandin D2 Regulates CD4+ Memory T Cell Trafficking across Blood Vascular Endothelium and Primes These Cells for Clearance across Lymphatic Endothelium

Ahmed

McGettrick

Yates

et al. 2011

The Journal of Immunology

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“…This molecule is regulated by other components of the ECM such as TSP1 and tumor necrosis factor-inducible gene 6 protein (TSG6) (60). These two proteins were presently observed to be up-regulated in stimulated NHDF, indicating that fibroblasts may be involved in regulating the recruitment of leukocytes by endothelial cells during inflammation, which was also observed by McGettrick et al (61). Such interrelations between angiogenesis and ECM reorganization as well as between fibroblasts and endothelial cells are further demonstrated by the interrelation of two important proteins mentioned before, PRRX1 and TNC.…”

Section: Discussionsupporting

confidence: 60%

Contribution of Human Fibroblasts and Endothelial Cells to the Hallmarks of Inflammation as Determined by Proteome Profiling

Slany

Bileck

Kreutz

et al. 2016

Molecular & Cellular Proteomics

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In order to systematically analyze proteins fulfilling effector functionalities during inflammation, here we present a comprehensive proteome study of inflammatory activated primary human endothelial cells and fibroblasts. Cells were stimulated with interleukin 1-␤ and fractionated in order to obtain secreted, cytoplasmic and nuclear protein fractions. Proteins were submitted to a data-dependent bottom up analytical platform using a QExactive orbitrap and the MaxQuant software for protein identification and label-free quantification. Results were further combined with similarly generated data previously obtained from the analysis of inflammatory activated peripheral blood mononuclear cells. Applying a false discovery rate of less than 0.01 at both, peptide and protein level, a total of 8370 protein groups assembled from 117,599 peptides was identified; mass spectrometry data have been made fully accessible via ProteomeXchange with identifier PXD003406 to PXD003417. Comparative proteome analysis allowed us to determine common and cell type-specific inflammation signatures comprising novel candidate marker molecules and related expression patterns of transcription factors. Cardinal features of inflammation such as interleukin 1-␤ processing and the interferon response differed substantially between the investigated cells. Furthermore, cells also exerted similar inflammation-related tasks; however, by making use of different sets of proteins. Hallmarks of inflammation thus emerged, including angiogenesis, extracellular matrix reorganization, adaptive and innate immune responses, oxidative stress response, cell proliferation and differentiation, cell adhesion and migration in addition to monosaccharide metabolic processes, representing both, common and cell type-specific responsibilities of cells during inflammation. Molecular & Cellular

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“…The manner in which fibroblasts alter the adhesiveness of endothelial cells has been shown to be in part dependent upon the milieu from which the fibroblast was derived. For instance, rheumatoid arthritis-derived synovial fibroblasts increased adherence of lymphocytes to endothelial cells while those taken from uninflamed microenvironments (dermal fibroblasts) actually decreased adherence of lymphocytes [125]. Fibroblasts themselves express adhesion molecules with most expressing ICAM-1 particularly in the presence of T cells and with even greater levels of expression in the presence of activated T cells [113].…”

Section: Fibroblasts and Trafficking: Chemokines And Angiogenesismentioning

confidence: 99%

T Cells and Stromal Fibroblasts in Human Tumor Microenvironments Represent Potential Therapeutic Targets

Barnas

Simpson-Abelson

Yokota

et al. 2010

Cancer Microenvironment

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The immune system of cancer patients recognizes tumor-associated antigens expressed on solid tumors and these antigens are able to induce tumor-specific humoral and cellular immune responses. Diverse immunotherapeutic strategies have been used in an attempt to enhance both antibody and T cell responses to tumors. While several tumor vaccination strategies significantly increase the number of tumor-specific lymphocytes in the blood of cancer patients, most vaccinated patients ultimately experience tumor progression. CD4+ and CD8+ T cells with an effector memory phenotype infiltrate human tumor microenvironments, but most are hyporesponsive to stimulation via the T cell receptor (TCR) and CD28 under conditions that activate memory T cells derived from the peripheral blood of the cancer patients or normal donors. Attempts to identify cells and molecules responsible for the TCR signaling arrest of tumor-infiltrating T cells have focused largely upon the immunosuppressive effects of tumor cells, tolerogenic dendritic cells and regulatory T cells. Here we review potential mechanisms by which human T cell function is arrested in the tumor microenvironment with a focus on the immunomodulatory effects of stromal fibroblasts. Determining in vivo which cells and molecules are responsible for the TCR arrest in human tumor-infiltrating T cells will be necessary to formulate and test strategies to prevent or reverse the signaling arrest of the human T cells in situ for a more effective design of tumor vaccines. These questions are now addressable using novel human xenograft models of tumor microenvironments.

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Fibroblasts from different sites may promote or inhibit recruitment of flowing lymphocytes by endothelial cells

Cited by 79 publications

References 49 publications

Prostaglandin D2 Regulates CD4+ Memory T Cell Trafficking across Blood Vascular Endothelium and Primes These Cells for Clearance across Lymphatic Endothelium

Prostaglandin D2 Regulates CD4+ Memory T Cell Trafficking across Blood Vascular Endothelium and Primes These Cells for Clearance across Lymphatic Endothelium

Contribution of Human Fibroblasts and Endothelial Cells to the Hallmarks of Inflammation as Determined by Proteome Profiling

T Cells and Stromal Fibroblasts in Human Tumor Microenvironments Represent Potential Therapeutic Targets

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