Chemokines and Chemokine Receptors: Positioning Cells for Host Defense and Immunity

Griffith, Jason W.; Sokol, Caroline L.; Luster, Andrew D.

doi:10.1146/annurev-immunol-032713-120145

Cited by 1,565 publications

(1,605 citation statements)

References 261 publications

(234 reference statements)

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“…1). We found that TILs generally expressed an activated chemokine receptor pattern 17 including high frequencies of CCR5 + , CXCR3 + and CXCR4 + (Fig. 1C).…”

Section: Resultsmentioning

confidence: 85%

“…While IL-8 may induce recruitment of T cells, T cells' extravasation and migration into peripheral tissues rely on selectin and integrin binding in concert with chemokine signaling to mediate rolling and firm adhesion to the endothelial wall. 17 , 36 Our xenograft model relies on stromal chemokines secreted by mouse endothelial cells and fibroblasts, and despite some sequence similarity and evolutionary conserved regions, there is a greater disparity, and these may not necessarily support T cell adhesion, extravasation and tumor infiltration. 37 In line with this, HEVs in human melanoma lesions have been shown to be major gateways for tumor infiltrating lymphocytes, 38 however lack of host immune cells in the NOG mouse model, and thus no orchestrating chemokines and cytokines, HEVs are most likely not produced in this model.…”

Section: Discussionmentioning

confidence: 99%

“…Among the common pro-inflammatory chemokine receptors are CCR5 and CXCR3, whereas site specific chemokine receptors such as CCR9 or CCR10 are upregulated on T cells primed in the mesenteric or skin draining LNs for subsequent homing to either gut or skin respectively. 16 , 17 …”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Chemokine receptor engineering of T cells with CXCR2 improves homing towards subcutaneous human melanomas in xenograft mouse model

et al. 2018

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Adoptive cell therapy (ACT) using in vitro expanded tumor infiltrating T lymphocytes (TILs) from biopsy material represents a highly promising treatment of disseminated cancer. A crucial prerequisite for successful ACT is sufficient recruitment of transferred lymphocytes to the tumor site; however, despite infusion of billions of lymphocytes, T cell infiltration into the tumor post ACT is limited. By PCR and Luminex analyses we found that a majority of malignant melanoma (MM) cell lines expressed chemokines CXCL1/Groα, CXCL8/IL-8, CXCL12/SDF-1 and CCL2. Concerning expression of the corresponding receptors on T cells, only the IL-8 receptor, CXCR2, was not expressed on T cells. CXCR2 was therefore expressed in T cells by lentiviral transduction, and shown to lead to ligand specific transwell migration of engineered T cells, as well as increased migration towards MM conditioned medium. In vivo homing was assessed in a xenograft NOG mouse model. Mice with subcutaneous human melanoma were treated with MAGE-A3 specific T cells transduced with either CXCR2 or MOCK. Transducing T cells carrying the MAGE-A3a3a high affinity T cell receptor with CXCR2 increased tumor infiltration. Flow cytometry analysis 7 days after ACT showed a doubling in CD3+ T cells in tumor digest of mice receiving CXCR2 transduced T cells compared to MOCK treated mice, a finding confirmed by immunohistochemistry. In conclusion, our CXCR2 transduced T cells are functional in vitro and transduction with CXCR2 increases in vivo homing of T cells to tumor site.

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“…1). We found that TILs generally expressed an activated chemokine receptor pattern 17 including high frequencies of CCR5 + , CXCR3 + and CXCR4 + (Fig. 1C).…”

Section: Resultsmentioning

confidence: 85%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Chemokine receptor engineering of T cells with CXCR2 improves homing towards subcutaneous human melanomas in xenograft mouse model

et al. 2018

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“…23 Expression profiling revealed that the chemotaxis pathway was more active in FoxD1 þ /Col1 À pericytes than in other lung fibroblasts, including higher levels of Ccl4 (macrophage inflammatory protein-1b), Cxcl2 (macrophage inflammatory protein-2), Ccl21 (secondary lymphoid-tissue chemokine), and Ccl5 (regulated on activation normal T cell expressed and secreted), which combined could attract neutrophils, monocytes, macrophages, dendritic cells, NK cells, and other classes of innate lymphocytes, and T cells (Figure 3). 10,63 The Col1 À pericyte subset also preferentially expressed a variety of immune sensing and response genes. Activation of the NLRP3 inflammasome to produce IL-1b is one of the strongest defenses against infections, but can also severely damage tissue and plays a highly pathogenic role in lung fibrosis.…”

Section: Pericytes Act As the Immune System's Sentriesmentioning

confidence: 99%

Lung Pericytes and Resident Fibroblasts

Barron

Gharib

Duffield

2016

The American Journal of Pathology

101

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Pericytes, resident fibroblasts, and mesenchymal stem cells are poorly described cell populations. They have recently been characterized in much greater detail in rodent lungs and have been shown to play important roles in development, homeostasis, response to injury and pathogens, as well as recovery from damage. These closely related mesenchymal cell populations form extensive connections to the lung's internal structure, as well as its internal and external surfaces. They generate and remodel extracellular matrix, coregulate the vasculature, help maintain and restore the epithelium, and act as sentries for the immune system. In this review, we revisit these functions in light of significant advances in characterizing and tracking lung fibroblast populations in rodents. Lineage tracing experiments have mapped the heritage, identified functions that discriminate lung pericytes from resident fibroblasts, identified a subset of mesenchymal stem cells, and shown these populations to be the predominant progenitors of pathological fibroblasts and myofibroblasts in lung diseases. These findings point to the importance of resident lung mesenchymal populations as therapeutic targets in acute lung injury as well as fibrotic and degenerative diseases. Far from being passive and quiescent, pericytes and resident fibroblasts are busily sensing and responding, through diverse mechanisms, to changes in lung health and function. (Am J Pathol 2016 http://dx

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“…In contrast to conventional T cells that recirculate between SLOs via blood and lymph, Tregs exhibit an expanded migratory pattern that includes tertiary tissues (14). A previous report demonstrated that KLF2 maintains naive T cells in a homeostatic migration pattern and, much like activated lymphocytes that quickly degrade this transcription factor, Klf2 excision causes quiescent T cells to vacate SLOs and enter peripheral tissues (15).…”

Section: Klf2 Acts As a Rheostat To Control Expression Of Treg Homingmentioning

confidence: 99%

Peripheral tolerance can be modified by altering KLF2-regulated Treg migration

Kumar

Rabacal

Volanakis

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Tregs are essential for maintaining peripheral tolerance, and thus targeting these cells may aid in the treatment of autoimmunity and cancer by enhancing or reducing suppressive functions, respectively. Before these cells can be harnessed for therapeutic purposes, it is necessary to understand how they maintain tolerance under physiologically relevant conditions. We now report that transcription factor Kruppel-like factor 2 (KLF2) controls naive Treg migration patterns via regulation of homeostatic and inflammatory homing receptors, and that in its absence KLF2-deficient Tregs are unable to migrate efficiently to secondary lymphoid organs (SLOs). Diminished Treg trafficking to SLOs is sufficient to initiate autoimmunity, indicating that SLOs are a primary site for maintaining peripheral tolerance under homeostatic conditions. Disease severity correlates with impaired Treg recruitment to SLOs and, conversely, promotion of Tregs into these tissues can ameliorate autoimmunity. Moreover, stabilizing KLF2 expression within the Treg compartment enhances peripheral tolerance by diverting these suppressive cells from tertiary tissues into SLOs. Taken together, these results demonstrate that peripheral tolerance is enhanced or diminished through modulation of Treg trafficking to SLOs, a process that can be controlled by adjusting KLF2 protein levels.

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Chemokines and Chemokine Receptors: Positioning Cells for Host Defense and Immunity

Cited by 1,565 publications

References 261 publications

Chemokine receptor engineering of T cells with CXCR2 improves homing towards subcutaneous human melanomas in xenograft mouse model

Chemokine receptor engineering of T cells with CXCR2 improves homing towards subcutaneous human melanomas in xenograft mouse model

Lung Pericytes and Resident Fibroblasts

Peripheral tolerance can be modified by altering KLF2-regulated Treg migration

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