Your search keyword '"Hansmann, Martin-Leo"' showing total 5 results

1. Epstein-Barr virus-infected B cells expanding in germinal centers of infectious mononucleosis patients do not participate in the germinal center reaction

Author

Kurth, Julia, Hansmann, Martin-Leo, Rajewsky, Klaus, and Kuppers, Ralf

Subjects

Epstein-Barr virus -- Genetic aspects, Science and technology

Abstract

To assess the impact of the germinal center (GC) reaction on viral spread in Epstein-Barr virus (EBV) infection, we isolated EB[V.sup.+] GC B cells from the tonsils of two infectious mononucleosis patients, sequenced their rearranged V genes, and determined expression of the EBV latency genes EBV nuclear antigen 2 and latent membrane protein 1. Most [EBV.sup.+] GC B cells belonged to clones of cells harboring somatically mutated V gene rearrangements. Ongoing somatic hypermutation, the hallmark of the GC reaction, was seen only in uninfected GC B cell clones, not in [EBV.sup.+] B cell clones. Thus, in infectious mononucleosis, GC and/or memory B cells are directly infected by EBV and expand without somatic hypermutation, whereas the GC passage of EBV-infected naive B cells does not contribute detectably to the generation of infected memory B cells, the main reservoir of EBV during persistence. Most, if not all, EBV-infected cells in GCs exhibited an unusual EBV gene expression pattern in that they were positive for EBV nuclear antigen 2 but negative for latent membrane protein 1. Although the three main types of EBV-associated B cell lymphomas (Burkitt's, Hodgkin's, and posttransplant lymphornas) presumably are derived from GC B cells, [EBV.sup.+] GC B cells resembling these [EBV.sup.+] GC B cell lymphomas in terms of EBV gene expression and somatic hypermutation pattern could not be identified.

Published

2003

2. Isolation of viable Hodgkin and Reed-Sternberg cells from Hodgkin disease tissues

Author

Irsch, Johannes, Nitsch, Silke, Hansmann, Martin-Leo, Rajewsky, Klaus, Tesch, Hans, Diehl, Volker, Jox, Andrea, Kuppers, Ralf, and Radbruch, Andreas

Subjects

Hodgkin's disease -- Research, Cancer cells -- Analysis, Clone cells -- Research, Lymphatic diseases -- Research, Science and technology

Abstract

Hodgkin disease (HD) is characterized by a small number of malignant Hodgkin and Reed-Sternberg (H/RS) cells among a major population of nonmalignant cells. The analysis of H/RS cells has been hampered by their low frequency and fragility. Here, we describe the isolation of viable H/RS cells from HD affected tissues by high gradient magnetic cell sorting (MACS) according to expression of CD30. The cells were enriched to a purity of up to 50%. H/RS cells were distinguished from other [CD30.sup.+] cells by the expression of CD15, their size and granularity. No CD30/CD15 double-positive cells could be enriched from a lymph node affected by the lymphocyte predominant subtype of HD, activated lymph nodes or peripheral blood of healthy donors. For two cases of HD individual MACS-purified H/RS cells and H/RS cells micromanipulated from tissue sections of the same lymphoma specimens were analyzed for Ig gene rearrangements. In both cases, identical V gene rearrangements were amplified from both sources of H/RS cells, showing that H/RS cells were successfully enriched. Moreover, the finding that in both cases no additional Ig gene rearrangements other than the ones identified in the H/RS cells micromanipulated from tissue sections were amplified from the MACS-purified H/RS cells further supports the monoclonality of these cells throughout the affected lymph nodes. The isolation of viable H/RS cells ex vivo is prerequisite for a direct study of gene expression by those cells and of their interaction with cells in their vicinity.

Published

1998

3. Hodgkin and Reed-Sternberg cells in lymphocyte predominant Hodgkin disease represent clonal populations of germinal center-derived tumor B cells

Author

Braeuninger, Andreas, Kuppers, Ralf, Strickler, John G., Wacker, Hans-Heinrich, Rajewsky, Klaus, and Hansmann, Martin-Leo

Subjects

Hodgkin's disease -- Research, Clone cells -- Research, Tumors -- Growth, Gene mutations -- Research, Science and technology

Abstract

Among the four subtypes of Hodgkin disease (HD), lymphocyte-predominant (LP) HD is now generally considered as a separate entity. The B cell nature of the typical Hodgkin and Reed-Sternberg (HRS) cells and their variants (L and H, lymphocytic and histiocytic cells) in LP HD has long been suspected, but the question of whether these cells represent a true tumor clone is unclear. We previously demonstrated clonal Ig gene rearrangements in one case of LP HD. In the present study, five cases of LP HD were analyzed by micromanipulation of single HRS cells from frozen tissue sections and DNA amplification of rearranged Ig heavy chain genes from those cells. Clonal V gene rearrangements harboring somatic mutations were detected in each case. In three cases ongoing somatic mutation was evident. This shows that HRS cells in LP HD are a clonal tumor population derived from germinal center B cells. The pattern of somatic mutation indicates that HRS cells in LP HD are selected for antibody expression. This, and the presence of ongoing mutation discriminates LP from classical HD.

Published

1997

4. Hodgkin disease: Hodgkin and Reed-Sternberg cells picked from histological sections show clonal immunoglobulin gene rearrangements and appear to be derived from B cells at various stages of development

Author

Kuppers, Ralf, Rajewsky, Klaus, Zhao, Min, Simons, Gunther, Laumann, Ralf, Fischer, Robert, and Hansmann, Martin-Leo

Subjects

Hodgkin's disease -- Research, B cells -- Physiological aspects, Immunoglobulins -- Genetic aspects, Science and technology

Abstract

Micromanipulation technique helps isolate Hodgkin and Reed-Sternberg (HRS) cells from histological sections of three cases of Hodgkin lymphoma, and PCR technique helps analyze individual cells for immunoglobulin variable (V) gene rearrangements. The HRS cells of each of the three cases exhibited a single heavy-chain V (VH) gene rearrangement, indicating that these cells belong to a single clone. A nodular sclerosis HD case had a potentially functional VH rearrangement. A germinal center B-cell origin of the HRS cells is suggested by the somatic mutations and intraclonal diversity in the VH genes for lymphocyte-predominant HD. Mixed-cellularity HD has a pre-B-cell origin, as indicated by the nonfunctional V gene rearrangements found on sequence analysis.

Published

1994

5. Incomplete cytokinesis and re-fusion of small mononucleated Hodgkin cells lead to giant multinucleated Reed-Sternberg cells.

Author

Rengstl, Benjamin, Newrzela, Sebastian, Heinrich, Tim, Weiser, Christian, Thalheimer, Frederic B., Schmid, Frederike, Warner, Kathrin, Hartmann, Sylvia, Schroeder, Timm, Küppers, Ralf, Rieger, Michael A., and Hansmann, Martin-Leo

Subjects

HODGKIN'S disease, CELL lines, CELL proliferation, LYMPHOPROLIFERATIVE disorders, MICROTUBULES, DIAGNOSIS

Abstract

Multinucleated Reed-Sternberg (RS) cells are pathognomonic for classical Hodgkin lymphoma (HL), and their presence is essential for diagnosis. How these giant tumor cells develop is controversial, however. It has been postulated that RS cells arise from mononucleated Hodgkin cells via endomitosis. Conversely, continuous single-cell tracking of HL cell lines by long-term time-lapse microscopy has identified cell fusion as the main route of RS cell formation. In contrast to growth-induced formation of giant Hodgkin cells, fusion of small mononuclear cells followed by a size increase gives rise to giant RS cells. Of note, fusion of cells originating from the same ancestor, termed re-fusion, is seen nearly exclusively. In the majority of cases, re-fusion of daughter cells is preceded by incomplete cytokinesis, as demonstrated by microtubule bonds among the cells. We confirm at the level of individual tracked cells that giant Hodgkin and RS cells have little proliferative capacity, further supporting small mononuclear Hodgkin cells as the proliferative compartment of the HL tumor clone. In addition, sister cells show a shared propensity for re-fusion, providing evidence of early RS cell fate commitment. Thus, RS cell generation is related neither to cell fusion of unrelated Hodgkin cells nor to endomitosis, but rather is mediated by re-fusion of daughter cells that underwent mitosis. This surprising finding supports the existence of a unique mechanism for the generation of multinuclear RS cells that may have implications beyond HL, given that RS-like cells are frequently observed in several other lymphoproliferative diseases as well. [ABSTRACT FROM AUTHOR]

Published

2013