Your search keyword '"Mahnke, Yolanda D."' showing total 3 results

1. Human melanoma-specific CD8+ T-cells from metastases are capable of antigen-specific degranulation and cytolysis directly ex vivo.

Author

Mahnke, Yolanda D., Devêvre, Estelle, Baumgaertner, Petra, Matter, Maurice, Rufer, Nathalie, Romero, Pedro, and Speiser, Daniel E.

Subjects

*CD8 antigen, *T cells, *CANCER cells, *METASTASIS, *VIRUS diseases, *TUMOR immunology

Abstract

The relatively low frequencies of tumor Ag-specific T-cells in PBMC and metastases from cancer patients have long precluded the analysis of their direct ex vivo cytolytic capacity. Using a new composite technique that works well with low cell numbers, we aimed at determining the functional competence of melanoma-specific CD8+ T-cells. A multiparameter flow cytometry based technique was applied to assess the cytolytic function, degranulation and IFNγ production by tumor Ag-specific CD8+ T-cells from PBMC and tumor-infiltrated lymph nodes (TILN) of melanoma patients. We found strong cytotoxicity by T-cells not only when they were isolated from PBMC but also from TILN. Cytotoxicity was observed against peptide-pulsed target cells and melanoma cells presenting the naturally processed endogenous antigen. However, unlike their PBMC-derived counterparts, T-cells from TILN produced only minimal amounts of IFNγ, while exhibiting similar levels of degranulation, revealing a critical functional dichotomy in metastatic lesions. Our finding of partial functional impairment fits well with the current knowledge that T-cells from cancer metastases are so-called exhausted, a state of T-cell hyporesponsiveness also found in chronic viral infections. The identification of responsible mechanisms in the tumor microenvironment is important for improving cancer therapies. [ABSTRACT FROM AUTHOR]

Published

2012

2. Maintenance of long-term tumour-specific T-cell memory by residual dormant tumour cells.

Author

Mahnke, Yolanda D., Schwendemann, Jochen, Beckhove, Philipp, and Schirrmacher, Volker

Subjects

*T cells, *HLA histocompatibility antigens, *MAJOR histocompatibility complex, *CELL adhesion molecules, *CANCER cells, *IMMUNE system, *IMMUNOLOGY

Abstract

LacZ (Gal)-reactive immune cells were transferred into athymic nu/ nu mice inoculated with Gal-expressing syngeneic tumour cells (ESbL-Gal) in order to study tumour-protective T-cell memory. This transfer prevented tumour outgrowth in recipients and resulted in the persistence of a high frequency of Gal-specific CD8+ T cells in the bone marrow and spleen. In contrast, such Ag-specific memory CD8+ T cells were not detectable by peptide–major histocompatibility complex (MHC) multimer staining in animals that had not previously received an antigenic challenge. Even though CD44hi memory T cells from the bone marrow showed a significantly higher turnover rate, as judged by bromodeoxyuridine (BrdU) incorporation, than respective cells from spleen or lymph nodes, as well as in comparison to CD44lo naïve T cells, these findings suggest that tumour-associated antigen (TAA) from residual dormant tumour cells are implicated in maintaining high frequencies of long-term surviving Gal-specific memory CD8+ T cells. Memory T cells could be recruited to the peritoneal cavity by tumour vaccination of immunoprotected nu/ nu mice and exhibited ex vivo antitumour reactivity. Long-term immune memory and tumour protection could be maintained over four successive transfers between tumour-inoculated recipients, which involved periodic antigenic restimulation in vivo prior to reisolating the cells for adoptive transfer. Using a cell line (ESbL-Gal-BM) that was established from dormant tumour cells isolated from the bone marrow of immunoprotected animals, it could be demonstrated that the tumour cells had up-regulated the expression of MHC class I molecules and down-regulated the expression of several adhesion molecules during the in vivo passage. Our results suggest that the bone marrow microenvironment has special features that are of importance for the maintenance of tumour dormancy and immunological T-cell memory, and that a low level of persisting antigen favours the maintenance of Ag-specific memory T cells over irrelevant memory T cells. [ABSTRACT FROM AUTHOR]

Published

2005

3. LiveCount Assay: Concomitant measurement of cytolytic activity and phenotypic characterisation of CD8+ T-cells by flow cytometry

Author

Devêvre, Estelle, Romero, Pedro, and Mahnke, Yolanda D.

Subjects

*CANCER treatment, *TUMORS, *CANCER cells, *PREVENTION of communicable diseases

Abstract

Abstract: Tumour immunologists strive to develop efficient tumour vaccination and adoptive transfer therapies that enlarge the pool of tumour-specific and -reactive effector T-cells in vivo. To assess the efficiency of the various strategies, ex vivo assays are needed for the longitudinal monitoring of the patient''s specific immune responses providing both quantitative and qualitative data. In particular, since tumour cell cytolysis is the end goal of tumour immunotherapy, routine immune monitoring protocols need to include a read-out for the cytolytic efficiency of Ag-specific cells. We propose to combine current immune monitoring techniques in a highly sensitive and reproducible multi-parametric flow cytometry based cytotoxicity assay that has been optimised to require low numbers of Ag-specific T-cells. The possibility of reanalysing those T-cells that have undergone lytic activity is illustrated by the concomitant detection of CD107a upregulation on the surface of degranulated T-cells. To date, the LiveCount Assay provides the only possibility of assessing the ex vivo cytolytic activity of low-frequency Ag-specific cytotoxic T-lymphocytes from patient material. [Copyright &y& Elsevier]

Published

2006