Literature DB >> 21703422

Human renal cell carcinoma induces a dendritic cell subset that uses T-cell crosstalk for tumor-permissive milieu alterations.

Ainhoa-M Figel1, Dorothee Brech, Petra U Prinz, Ulrike K Lettenmeyer, Judith Eckl, Adriana Turqueti-Neves, Josef Mysliwietz, David Anz, Nicole Rieth, Niklas Muenchmeier, Alexander Buchner, Stefan Porubsky, Sabine I Siegert, Stephan Segerer, Peter J Nelson, Elfriede Noessner.   

Abstract

Tissue dendritic cells (DCs) may influence the progression of renal cell carcinoma (RCC) by regulating the functional capacity of antitumor effector cells. DCs and their interaction with T cells were analyzed in human RCC and control kidney tissues. The frequency of CD209(+) DCs in RCCs was found to be associated with an unfavorable T(H)1 cell balance in the tissue and advanced tumor stages. The CD209(+) DCs in RCC were unusual because most of them co-expressed macrophage markers (CD14, CD163). The phenotype of these enriched-in-renal-carcinoma DCs (ercDCs) could be reiterated in vitro by carcinoma-secreted factors (CXCL8/IL-8, IL-6, and vascular endothelial growth factor). ErcDCs resembled conventional DCs in costimulatory molecule expression and antigen cross-presentation. They did not suppress cognate cytotoxic T-lymphocyte function and did not cause CD3ζ down-regulation, FOXP3 induction, or T-cell apoptosis in situ or in vitro; thus, they are different from classic myeloid-derived suppressor cells. ErcDCs secreted high levels of metalloproteinase 9 and used T-cell crosstalk to increase tumor-promoting tumor necrosis factor α and reduce chemokines relevant for T(H)1-polarized lymphocyte recruitment. This modulation of the tumor environment exerted by ercDCs suggests an immunologic mechanism by which tumor control can fail without involving cytotoxic T-lymphocyte inhibition. Pharmacologic targeting of the deviated DC differentiation could improve the efficacy of immunotherapy against RCC.
Copyright © 2011 American Society for Investigative Pathology. Published by Elsevier Inc. All rights reserved.

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Year:  2011        PMID: 21703422      PMCID: PMC3123875          DOI: 10.1016/j.ajpath.2011.03.011

Source DB:  PubMed          Journal:  Am J Pathol        ISSN: 0002-9440            Impact factor:   4.307


  61 in total

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2.  Tumor-infiltrating Foxp3-CD4+CD25+ T cells predict poor survival in renal cell carcinoma.

Authors:  Sameer A Siddiqui; Xavier Frigola; Sandra Bonne-Annee; Maria Mercader; Susan M Kuntz; Amy E Krambeck; Shomik Sengupta; Haidong Dong; John C Cheville; Christine M Lohse; Christopher J Krco; W Scott Webster; Bradley C Leibovich; Michael L Blute; Keith L Knutson; Eugene D Kwon
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3.  Type, density, and location of immune cells within human colorectal tumors predict clinical outcome.

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Journal:  Science       Date:  2006-09-29       Impact factor: 47.728

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Review 5.  Taking dendritic cells into medicine.

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  18 in total

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Journal:  J Am Soc Nephrol       Date:  2015-04-08       Impact factor: 10.121

2.  Tumor stroma-derived factors skew monocyte to dendritic cell differentiation toward a suppressive CD14+ PD-L1+ phenotype in prostate cancer.

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Journal:  Oncoimmunology       Date:  2014-12-13       Impact factor: 8.110

3.  Identification and Quantitation of Leukocyte Populations in Human Kidney Tissue by Multi-parameter Flow Cytometry.

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4.  Accumulation of tolerogenic human 6-sulfo LacNAc dendritic cells in renal cell carcinoma is associated with poor prognosis.

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Review 5.  Implications of the tumor immune microenvironment for staging and therapeutics.

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Review 8.  Metastatic renal cell carcinoma: update on epidemiology, genetics, and therapeutic modalities.

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9.  Intratumoral alterations of dendritic-cell differentiation and CD8(+) T-cell anergy are immune escape mechanisms of clear cell renal cell carcinoma.

Authors:  Elfriede Noessner; Dorothee Brech; Anna N Mendler; Ilias Masouris; Ramona Schlenker; Petra U Prinz
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Review 10.  Dendritic Cell Plasticity in Tumor-Conditioned Skin: CD14(+) Cells at the Cross-Roads of Immune Activation and Suppression.

Authors:  Rieneke van de Ven; Jelle J Lindenberg; Dinja Oosterhoff; Tanja D de Gruijl
Journal:  Front Immunol       Date:  2013-11-25       Impact factor: 7.561

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