Imprinting of Skin/Inflammation Homing in CD4+ T Cells Is Controlled by DNA Methylation within the <i>Fucosyltransferase 7</i> Gene

Pink, Matthias; Ratsch, Boris A.; Mardahl, Maibritt; Polansky, Julia K.; Karl, Martin; Baumgrass, Ria; Wallner, Stefan; Cadenas, Cristina; Gianmoena, Kathrin; Floess, Stefan; Chen, Wei; Nordstroem, Karl; Tierling, Sascha; Olek, Sven; Walter, Jörn; Syrbe, Uta

doi:10.4049/jimmunol.1502434

Cited by 18 publications

(13 citation statements)

References 55 publications

(58 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Importantly, malignant cells of the peripheral blood expressed the skin-homing receptor CLA as shown by flow cytometry ( Figure S4 ), consistent with corresponding gene upregulation of both SELPLG and the fucosyltransferase FUT7 ( 50 ) ( Figure 6D ), indicating their retained capability to home to the skin ( 51 , 52 ).…”

Section: Resultssupporting

confidence: 62%

Single-Cell RNA Sequencing Reveals Tissue Compartment-Specific Plasticity of Mycosis Fungoides Tumor Cells

et al. 2021

View full text Add to dashboard Cite

Mycosis fungoides (MF) is the most common primary cutaneous T-cell lymphoma. While initially restricted to the skin, malignant cells can appear in blood, bone marrow and secondary lymphoid organs in later disease stages. However, only little is known about phenotypic and functional properties of malignant T cells in relationship to tissue environments over the course of disease progression. We thus profiled the tumor micromilieu in skin, blood and lymph node in a patient with advanced MF using single-cell RNA sequencing combined with V-D-J T-cell receptor sequencing. In skin, we identified clonally expanded T-cells with characteristic features of tissue-resident memory T-cells (TRM, CD69+CD27-NR4A1+RGS1+AHR+). In blood and lymph node, the malignant clones displayed a transcriptional program reminiscent of a more central memory-like phenotype (KLF2+TCF7+S1PR1+SELL+CCR7+), while retaining tissue-homing receptors (CLA, CCR10). The skin tumor microenvironment contained potentially tumor-permissive myeloid cells producing regulatory (IDO1) and Th2-associated mediators (CCL13, CCL17, CCL22). Given their expression of PVR, TNFRSF14 and CD80/CD86, they might be under direct control by TIGIT+CTLA4+CSF2+TNFSF14+ tumor cells. In sum, this study highlights the adaptive phenotypic and functional plasticity of MF tumor cell clones. Thus, the TRM-like phenotype enables long-term skin residence of MF cells. Their switch to a TCM-like phenotype with persistent skin homing molecule expression in the circulation might explain the multi-focal nature of MF.

show abstract

Section: Resultssupporting

confidence: 62%

Single-Cell RNA Sequencing Reveals Tissue Compartment-Specific Plasticity of Mycosis Fungoides Tumor Cells

et al. 2021

View full text Add to dashboard Cite

show abstract

“…The changes in cell surface glycosylation observed with oncogenic transformation are likely mediated by epigenetic mechanisms. Inflammatory mediators (such as TNF-α 48 and G-CSF 49 ) have previously been reported to lead to increased ST3GAL4, FUT4, and FUT7 expression, which are largely regulated by repressive promoter methylation 50,51 . Thus, it is tempting to speculate that the altered glycosylation (and increase in E-selectin binding potential) on malignant cells is associated with the epigenetic changes in DNA methylation and histone modulation that occurs during oncogenesis, possibly re-enforced by tumorassociated inflammation.…”

Section: Discussionmentioning

confidence: 99%

Endothelial E-selectin inhibition improves acute myeloid leukaemia therapy by disrupting vascular niche-mediated chemoresistance

et al. 2020

View full text Add to dashboard Cite

The endothelial cell adhesion molecule E-selectin is a key component of the bone marrow hematopoietic stem cell (HSC) vascular niche regulating balance between HSC self-renewal and commitment. We now report in contrast, E-selectin directly triggers signaling pathways that promote malignant cell survival and regeneration. Using acute myeloid leukemia (AML) mouse models, we show AML blasts release inflammatory mediators that upregulate endothelial niche E-selectin expression. Alterations in cell-surface glycosylation associated with oncogenesis enhances AML blast binding to E-selectin and enable promotion of prosurvival signaling through AKT/NF-κB pathways. In vivo AML blasts with highest E-selectin binding potential are 12-fold more likely to survive chemotherapy and main contributors to disease relapse. Absence (in Sele −/− hosts) or therapeutic blockade of E-selectin using small molecule mimetic GMI-1271/Uproleselan effectively inhibits this niche-mediated pro-survival signaling, dampens AML blast regeneration, and strongly synergizes with chemotherapy, doubling the duration of mouse survival over chemotherapy alone, whilst protecting endogenous HSC.

show abstract

“…77 – 79 CLA bears the tetrasaccharide moiety, sLe X , which is recognized by the HECA-452 mAb, and its biosynthesis is catalyzed in part by FTIV and VII, of which the latter enzyme can be induced by IL-2, IL-7, IL-12, TGF-β, Ag-priming, and promoter demethylation and is suppressed by IL-4 and retinoic acid. 30 , 71 , 80 – 84 Knockout mice lacking FTIV and FTVII fail to generate T eff cells that home to skin. 30 Skin inflammation upregulates cognate ligands on dermal postcapillary microvessels recognized by skin-tropic receptors, including E-selectin (in humans and other primates), and both E- and P-selectin (in non-primate mammals), chemokines CCL17 (CCR4 receptor) and CCL27 (CCR10 receptor), ICAM-1 (LFA-1 receptor) and VCAM-1 (VLA-4 receptor).…”

Section: The Conventional Multi-step Paradigm Of T Cell Homingmentioning

confidence: 99%

T-lymphocyte homing: an underappreciated yet critical hurdle for successful cancer immunotherapy

Sackstein

Schatton

Barthel

2017

Laboratory Investigation

166

151

View full text Add to dashboard Cite

Advances in cancer immunotherapy have offered new hope for patients with metastatic disease. This unfolding success story has been exemplified by a growing arsenal of novel immunotherapeutics, including blocking antibodies targeting immune checkpoint pathways, cancer vaccines, and adoptive cell therapy (ACT). Nonetheless, clinical benefit remains highly variable and patient-specific, in part, because all immunotherapeutic regimens vitally hinge on the capacity of endogenous and/or adoptively-transferred T effector (Teff) cells, including chimeric antigen receptor (CAR) T cells, to home efficiently into tumor target tissue. Thus, defects intrinsic to the multi-step T cell homing cascade have become an obvious, though significantly underappreciated contributor to immunotherapy resistance. Conspicuous have been low intralesional frequencies of tumor-infiltrating T-lymphocytes (TILs) below clinically beneficial threshold levels, and peripheral rather than deep lesional TIL infiltration. Therefore, a Teff cell ‘homing deficit’ may arguably represent a dominant factor responsible for ineffective immunotherapeutic outcomes, as tumors resistant to immune-targeted killing thrive in such permissive, immune-vacuous microenvironments. Fortunately, emerging data is shedding light into the diverse mechanisms of immune escape by which tumors restrict Teff cell trafficking and lesional penetrance. In this review, we scrutinize evolving knowledge on the molecular determinants of Teff cell navigation into tumors. By integrating recently described, though sporadic information of pivotal adhesive and chemokine homing signatures within the tumor microenvironment with better established paradigms of T cell trafficking under homeostatic or infectious disease scenarios, we seek to refine currently incomplete models of Teff cell entry into tumor tissue. We further summarize how cancers thwart homing to escape immune-mediated destruction and raise awareness of the potential impact of immune checkpoint blockers on Teff cell homing. Finally, we speculate on innovative therapeutic opportunities for augmenting Teff cell homing capabilities to improve immunotherapy-based tumor eradication in cancer patients, with special focus on malignant melanoma.

show abstract

Imprinting of Skin/Inflammation Homing in CD4+ T Cells Is Controlled by DNA Methylation within the Fucosyltransferase 7 Gene

Cited by 18 publications

References 55 publications

Single-Cell RNA Sequencing Reveals Tissue Compartment-Specific Plasticity of Mycosis Fungoides Tumor Cells

Single-Cell RNA Sequencing Reveals Tissue Compartment-Specific Plasticity of Mycosis Fungoides Tumor Cells

Endothelial E-selectin inhibition improves acute myeloid leukaemia therapy by disrupting vascular niche-mediated chemoresistance

T-lymphocyte homing: an underappreciated yet critical hurdle for successful cancer immunotherapy

Contact Info

Product

Resources

About