Hepatocyte Growth Factor Receptor c-Met Instructs T Cell Cardiotropism and Promotes T Cell Migration to the Heart via Autocrine Chemokine Release

Komarowska, Izabela; Coe, David; Wang, Guosu; Haas, Robert; Mauro, Claudio; Kishore, Madhav; Cooper, Dianne; Nadkarni, Suchita; Fu, Hongmei; Steinbrüchel, Daniel A.; Pitzalis, Costantino; Anderson, Graham; Bucy, Pat; Lombardi, Giovanna; Breckenridge, Ross A.; Marelli‐Berg, Federica M.

doi:10.1016/j.immuni.2015.05.014

Cited by 94 publications

(99 citation statements)

References 32 publications

(51 reference statements)

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“…Taken together, the results presented by Komarowska et al (2015) introduce a new paradigm for cardiac T cell tropism. In addition, the data are exciting because they raise the potential to alter tissuetropism of T cells that might modulate T cell-mediated pathology in the heartand relevant therapeutic compounds are already available.…”

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confidence: 66%

Another TLO in the Wall: Education and Control of T Cells in Atherosclerotic Arteries

Onder

Ludewig

2015

Immunity

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confidence: 66%

Another TLO in the Wall: Education and Control of T Cells in Atherosclerotic Arteries

Onder

Ludewig

2015

Immunity

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“…In this issue of Immunity, Komarowska et al (2015) describe an autocrine loop that is initiated by cardiac-expressed hepatocyte growth factor to direct T cells into the heart during inflammation and cardiac transplant rejection.…”

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confidence: 99%

“…Do tissue-derived factors induce specific sets of adhesion factors on T cells? In this issue of Immunity, Komarowska et al (2015) set out to address this experimentally, by investigating the role of hepatocyte growth factor (HGF) in T cell homing to the heart. Although it has been proposed previously that the chemokine receptors CXCR3 (and its ligand CXCL10) as well as CCR4 are contributing to T cell accumulation during heart transplantation (Hancock et al, 2001; Hü ser et al, 2005), it was unknown how the myocardium imprints cardiotropism during priming and differentiation of heart-specific T cells and whether such imprinting would take place in inflamed tissue or the draining lymph nodes.…”

mentioning

confidence: 99%

“…Although it has been proposed previously that the chemokine receptors CXCR3 (and its ligand CXCL10) as well as CCR4 are contributing to T cell accumulation during heart transplantation (Hancock et al, 2001; Hü ser et al, 2005), it was unknown how the myocardium imprints cardiotropism during priming and differentiation of heart-specific T cells and whether such imprinting would take place in inflamed tissue or the draining lymph nodes. Findings from Komarowska et al (2015) suggest that HGF might be a master regulator of T cell cardiotropism.…”

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confidence: 99%

“…The centerpiece of Komarowska et al (2015)'s study is a series of in vitro and in vivo experiments, in which a 7-day treatment with HGF in parallel with strong induction of TCR signaling via anti-CD3 and anti-CD28 stimulation enhanced responsiveness to the chemokines CXCL10 and CCL22 in migration assays in vitro, as well as directing cells to the peritoneal cavity in mice. These effects were dependent on binding of HGF to its receptor c-Met and induction of an intracellular signaling cascade involving Akt and STAT3 engagement.…”

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confidence: 99%

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HGF Guides T Cells into the Heart

Wolf

Ley

2015

Immunity

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SOCS1: Regulator of T Cells in Autoimmunity and Cancer

Ilangumaran

Bobbala

Ramanathan

2017

Current Topics in Microbiology and Immunology

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SOCS1 is a negative feedback regulator of cytokine and growth factor receptor signaling, and plays an indispensable role in attenuating interferon gamma signaling. Studies on SOCS1-deficient mice have established a crucial role for SOCS1 in regulating CD8 T cell homeostasis. In the thymus, SOCS1 prevents thymocytes that had failed positive selection from surviving and expanding, ensures negative selection and prevents inappropriate developmental skewing toward the CD8 lineage. In the periphery, SOCS1 not only controls production of T cell stimulatory cytokines but also attenuates the sensitivity of CD8 T cells to synergistic cytokine stimulation and antigen non-specific activation. As cytokine stimulation of CD8 T lymphocytes increases their sensitivity to low affinity TCR ligands, SOCS1 likely contributes to peripheral T cell tolerance by putting brakes on aberrant T cell activation driven by inflammatory cytokines. In addition, SOCS1 is critical to maintain the stability of T regulatory cells and control their plasticity to become pathogenic Th17 and Th1 cells under the harmful influence of inflammatory cytokines. SOCS1 also regulates T cell activation by dendritic cells via modulating their generation, maturation, antigen presentation, costimulatory signaling, and cytokine production. The above control mechanisms of SOCS1 on T cells, T regulatory cells and dendritic cells collectively contribute to immunological tolerance and prevent autoimmune manifestation. On other hand, silencing SOCS1 in dendritic cells or CD8 T cells stimulates efficient antitumor immunity. Thus, even though SOCS1 is not a cell surface checkpoint inhibitor, its regulatory functions on T cell responses qualify SOCS1as a "non-classical" checkpoint blocker. SOCS1 also functions as a tumor suppressor in cancer cells by regulating oncogenic signal transduction pathways. The loss of SOCS1 expression observed in many tumors may have an impact on classical checkpoint pathways. The potential to exploit SOCS1 to treat inflammatory/autoimmune diseases and elicit antitumor immunity is discussed.

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Hepatocyte Growth Factor Receptor c-Met Instructs T Cell Cardiotropism and Promotes T Cell Migration to the Heart via Autocrine Chemokine Release

Cited by 94 publications

References 32 publications

Another TLO in the Wall: Education and Control of T Cells in Atherosclerotic Arteries

Another TLO in the Wall: Education and Control of T Cells in Atherosclerotic Arteries

HGF Guides T Cells into the Heart

SOCS1: Regulator of T Cells in Autoimmunity and Cancer

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