Your search keyword '"Poschke I"' showing total 3 results

1. Camouflage and sabotage: tumor escape from the immune system.

Author

Poschke I, Mougiakakos D, and Kiessling R

Subjects

Animals, Antigen Presentation, Clinical Trials as Topic, Disease Models, Animal, Histocompatibility Antigens Class I genetics, Histocompatibility Antigens Class I immunology, Humans, Immunosuppression Therapy, Myeloid Cells immunology, Neoplasms immunology, Neoplasms metabolism, Neoplasms pathology, Oxidative Stress, T-Lymphocytes, Regulatory immunology, Histocompatibility Antigens Class I metabolism, Immune System, Immunotherapy trends, Neoplasms therapy, Tumor Escape

Abstract

The field of tumor immunology has made great progress in understanding tumor immune interactions. As a consequence a number of immuno-therapeutic approaches have been successfully introduced into the clinic and a large number of promising therapeutic strategies are investigated in ongoing clinical trials. Evaluation of anti-tumor immunity in such trials as well as in animal models has shown that tumor escape from immune recognition and tumor-mediated suppression of anti-tumor immunity can pose a significant obstacle to successful cancer therapy. Here, we review mechanisms of tumor immune escape and immune-subversion with a focus on the research interests in our laboratory: loss of MHC class I on tumor cells, increased oxidative stress, recruitment of myeloid-derived suppressor cells, and regulatory T cells.

Published

2011

2. Differential tumor infiltration by T-cells characterizes intrinsic molecular subtypes in breast cancer.

Author

Miyan, M., Schmidt-Mende, J., Kiessling, R., Poschke, I., and de Boniface, J.

Subjects

BREAST cancer patients, BREAST cancer treatment, IMMUNE system, T cells, BREAST cancer prognosis, ANTIGENS, BREAST tumors, IMMUNOHISTOCHEMISTRY, LYMPHOCYTES, PROGNOSIS, PHENOTYPES, LYMPHOCYTE count

Abstract

Background: Molecular subtypes of breast cancer and presence of tumor-infiltrating immune cells have both been implicated as important predictive and prognostic factors for improved risk stratification and treatment individualization of breast cancer patients. Their association, however, has not been studied in detail. The aim of this study was to evaluate the expression of the T cell markers CD8, FoxP3, CD3 and ζ-chain in molecular subtypes of the invasive margin and tumor center of breast cancer and corresponding sentinel nodes and to deduct prognostic information from these findings.Methods: Tumor and sentinel node sections from 177 patients with primary, invasive, unilateral early-stage breast cancer were stained by immunohistochemistry and T-cell phenotypes quantified manually. Clinical data were collected from medical records.Results: The degree of T-cell infiltration and expression of all markers differed significantly among the molecular subtypes, being highest in non-luminal, more aggressive tumors: more T-cell infiltration and higher expression of all markers were associated with hormone receptor negativity, higher proliferation and higher histological grades, but also with larger tumor size. Basal-like tumors, and most remarkably their tumor centers, hosted the highest number of FoxP3+ T-cells with an unfavorable ratio to cytotoxic CD8+ T-cells. T-cell infiltration was generally higher in the invasive margin than the tumor center. A scoring system based on densities of CD3 and CD8 could significantly separate molecular subtypes (p < 0.001).Conclusions: Thus, immunological patterns with functional implications within each subtype are associated with prognostic factors. These findings should be further validated in studies using larger patient populations and longer follow-up. [ABSTRACT FROM AUTHOR]

Published

2016

3. Myeloid-derived suppressor cells impair the quality of dendritic cell vaccines.

Author

Poschke, I., Mao, Y., Adamson, L., Salazar-Onfray, F., Masucci, G., and Kiessling, R.

Subjects

*DENDRITIC cells, *IMMUNE system, *MELANOMA, *MONOCYTES, *CYTOKINES, *VACCINATION

Abstract

Myeloid-derived suppressor cells (MDSC) are important regulators of the immune system and key players in tumor-induced suppression of T-cell responses. CD14+HLA-DR−/low MDSC have been detected in a great number of malignancies, including melanoma. MDSC are known to be impaired in their ability to differentiate along the myeloid lineage, e.g., into dendritic cells (DC). This is a concern for utilization of monocyte-derived DC for vaccination of patients with melanoma or other cancers exhibiting accumulation of CD14+ MDSC. When producing DC according to standard operating procedures of two currently ongoing clinical trials, we found that MDSC co-purified with monocytes isolated by elutriation. MDSC frequencies did not affect yield or viability of the produced DC, but induced a dose-dependent decrease in DC maturation, ability to take up antigen, migrate and induce T-cell IFNγ production. Changes in DC characteristics were most notable when 'pathological' frequencies of >50% CD14+HLA-DR− cells were present in the starting culture. The impaired DC quality could not be explained by altered cytokine production or increased oxidative stress in the cultures. Tracking of HLA-DR− cells throughout the culture period revealed that the observed changes were partially due to the impaired maturation and functionality of the originally HLA-DR− population, but also to their negative effects on HLA-DR+ cells. In conclusion, MDSC could be induced to differentiate into DC but, due to the impairment of overall DC vaccine quality when >50% HLA-DR− cells were present in the starting culture, their removal could be advisable. [ABSTRACT FROM AUTHOR]

Published

2012