Close Association between Fas Ligand (FasL; CD95L)‐positive Tumor‐associated Macrophages and Apoptotic Cancer Cells along Invasive Margin of Colorectal Carcinoma: A Proposal on Tumor‐Host Interactions
- 1 March 2002
- journal article
- Published by Wiley in Japanese Journal of Cancer Research
- Vol. 93 (3) , 320-328
- https://doi.org/10.1111/j.1349-7006.2002.tb02175.x
Abstract
Anti‐tumor immune responses are considered to be one of the key host reactions in human colorectal cancer, with T cells as important effector cells. For the induction of tumor‐specific immunity, processing of cancer cells and pruning of T cells by antigen‐presenting cells are important. The present study was designed to clarify the relationship between Fas ligand (FasL; CD95L) expression and apoptotic cancer cells. Immunohistochemistry using frozen sections taken from 58 patients with colorectal cancer revealed that stromal cells composed mainly of tumor‐associated macrophages expressed FasL, leaving cancer cells negative for FasL. These macrophages were abundantly distributed along the invasive margin. In situ hybridization revealed that these macrophages as well as cancer cells expressed FasL mRNA, whereas macrophages in the normal colon mucosa rarely expressed FasL. Apoptotic cancer cells recognized by monoclonal antibody M30 CytoDEATH were localized not only in cancer cell nests, but also in the stroma along the invasive margin showing a dissociated pattern, which was particularly evident in the areas of FasL+ macrophages. Furthermore, these macrophages, phenotypically similar to dendritic cells, occasionally contained M30+ apoptotic cancer cells in the cytoplasm. Clinicopathologic analyses in 123 cases revealed 1) a positive correlation between the degree of dissociated M30+ apoptotic cancer cells and the number of macrophages along the invasive margin and 2) an inverse association between the degree of dissociated M30+ apoptotic cancer cells and the occurrence of hematogenous metastasis after surgical resection of the primary tumor. In conclusion, the present study shows the impor‐ tance of FasL+ activated macrophages as one of the host defense mechanisms against cancer cell spread in human colorectal cancer.Keywords
This publication has 36 references indexed in Scilit:
- Cutting Edge: The Tumor Counterattack Hypothesis Revisited: Colon Cancer Cells Do Not Induce T Cell Apoptosis Via the Fas (CD95, APO-1) PathwayThe Journal of Immunology, 2000
- Not so Fas: Re-evaluating the mechanisms of immune privilege and tumor escapeNature Medicine, 2000
- Clinicopathologic significance of urokinase receptor- and mmp-9-positive stromal cells in human colorectal cancer: Functional multiplicity of matrix degradation on hematogenous metastasisInternational Journal of Cancer, 2000
- Phagocytosis Triggers Macrophage Release of Fas Ligand and Induces Apoptosis of Bystander LeukocytesThe Journal of Immunology, 1999
- Fas ligand expression in primary colon adenocarcinomas: evidence that the Fas counterattack is a prevalent mechanism of immune evasion in human colon cancerThe Journal of Pathology, 1998
- CD8+ T cells infiltrated within cancer cell nests as a prognostic factor in human colorectal cancer.1998
- Human monocytic cells contain high levels of intracellular Fas ligand: rapid release following cellular activation.The Journal of Immunology, 1997
- Antitumor effect of locally produced CD95 ligandNature Medicine, 1997
- Cytolytic T-cell cytotoxicity is mediated through perforin and Fas lytic pathwaysNature, 1994
- Adoptive T Cell Therapy of Tumors: Mechanisms Operative in the Recognition and Elimination of Tumor CellsPublished by Elsevier ,1991