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Circulating monocytes and tumor-associated macrophages express recombined immunoglobulins in glioblastoma patients

Busch, Svenja ; Talamini, Marina ; Brenner, Steffen ; Abdulazim, Amr ; Hänggi, Daniel ; Neumaier, Michael ; Seiz-Rosenhagen, Marcel ; Fuchs, Tina

In: Clin Trans Med, 8 (2019), Nr. 18. pp. 1-14. ISSN 2001-1326

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Download (1MB) | Lizenz: Creative Commons LizenzvertragCirculating monocytes and tumor-associated macrophages express recombined immunoglobulins in glioblastoma patients by Busch, Svenja ; Talamini, Marina ; Brenner, Steffen ; Abdulazim, Amr ; Hänggi, Daniel ; Neumaier, Michael ; Seiz-Rosenhagen, Marcel ; Fuchs, Tina underlies the terms of Creative Commons Attribution 4.0

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Abstract

Background: Glioblastoma is the most common and malignant brain tumor in adults. Glioblastoma is usually fatal 12–15 months after diagnosis and the current possibilities in therapy are mostly only palliative. Therefore, new forms of diagnosis and therapy are urgently needed. Since tumor-associated macrophages are key players in tumor progression and survival there is large potential in investigating their immunological characteristics in glioblastoma patients. Recent evidence shows the expression of variable immunoglobulins and TCRαβ in subpopulations of monocytes, in vitro polarized macrophages and macrophages in the tumor microenvironment. We set out to investigate the immunoglobulin sequences of circulating monocytes and tumor-associated macrophages from glioblastoma patients to evaluate their potential as novel diagnostic or therapeutic targets.

Results: We routinely find consistent expression of immunoglobulins in tumor-associated macrophages (TAM) and circulating monocytes from all glioblastoma patients analyzed in this study. However, the immunoglobulin repertoires of circulating monocytes and TAM are generally more restricted compared to B cells. Furthermore, the immunoglobulin expression in the macrophage populations negatively correlates with the tumor volume. Interestingly, the comparison of somatic mutations, V-chain usage, CDR3-length and the distribution of used heavy chain genes on the locus of chromosome 14 of the immunoglobulins from myeloid to B cells revealed virtually no differences.

Conclusions: The investigation of the immunoglobulin repertoires from TAM and circulating monocytes in glioblastoma-patients revealed a negative correlation to the tumor volume, which could not be detected in the immunoglobulin repertoires of the patients’ B lymphocytes. Furthermore, the immunoglobulin repertoires of monocytes were more diverse than the repertoires of the macrophages in the tumor microenvironment from the same patients suggesting a tumor-specific immune response which could be advantageous for the use as diagnostic or therapeutic target.

Document type: Article
Journal or Publication Title: Clin Trans Med
Volume: 8
Number: 18
Publisher: Springer Open
Place of Publication: Berlin ; Heidelberg
Date Deposited: 07 Aug 2019 11:33
Date: 2019
ISSN: 2001-1326
Page Range: pp. 1-14
Faculties / Institutes: Medizinische Fakultät Mannheim > Institut für Klinische Chemie
DDC-classification: 610 Medical sciences Medicine
Uncontrolled Keywords: Glioblastoma, Immunoglobulins, Monocytes, Tumor-associated macrophages, Tumor volume
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