Abstract
Radiation therapy is one of the primary treatment modalities for cancer along with chemotherapy and surgical therapy. The main mechanism of the tumor reduction after irradiation has been considered to be damage to the tumor DNA. However, we found that tumor-specific CTL, which were induced in the draining lymph nodes (DLN) and tumor tissue of tumor-bearing mice, play a crucial role in the inhibition of tumor growth by radiation. Indeed, the therapeutic effect of irradiation was almost completely abolished in tumor-bearing mice by depleting CD8(+) T cells through anti-CD8 monoclonal antibody administration. In mice whose DLN were surgically ablated or genetically defective (Aly/Aly mice), the generation of tetramer(+) tumor-specific CTL at the tumor site was greatly reduced in parallel with the attenuation of the radiation-induced therapeutic effect against the tumor. This indicates that DLN are essential for the activation and accumulation of radiation-induced CTL, which are essential for inhibition of the tumor. A combined therapy of local radiation with Th1 cell therapy augmented the generation of tumor-specific CTL at the tumor site and induced a complete regression of the tumor, although radiation therapy alone did not exhibit such a pronounced therapeutic effect. Thus, we conclude that the combination treatment of local radiation therapy and Th1 cell therapy is a rational strategy to augment antitumor activity mediated by tumor-specific CTL.
Highlights
Radiation therapy is one of the major modalities for the treatment of human cancer and has been established as an excellent local treatment for malignant tumors [1]
Lymphocytes were isolated from tumor draining lymph nodes (DLN) and tumor mass to examine the generation of model tumor antigen (OVA)–specific CTL by staining with Ovalbumin protein (OVA)/H-2Kb tetramer
The frequency of OVA-tetramer+ CD8+ CTL in EG7-bearing mice treated with radiation therapy was markedly elevated in tumor DLN and tumor tissue compared with sham-irradiated mice or EL4-irradiated mice [0.4% in DLN and 0.5% in CD8+ tumor-infiltrating T lymphocytes (TIL); Fig. 1A]
Summary
Radiation therapy is one of the major modalities for the treatment of human cancer and has been established as an excellent local treatment for malignant tumors [1]. Radiotherapy does not always achieve the same level of efficacy against tumors as surgery or chemotherapy. It has been considered that the main mechanism of the tumor reduction after irradiation is direct damage to the tumor DNA by ionizing irradiation. Some studies have reported that tumor local irradiation elicits immunomodulatory effects and induces tumor-specific immune responses [2,3,4,5,6]. Lugade and colleagues [2] showed that local radiation increased both the generation of tumor peptide–reactive IFN-γ–producing antitumor immune cells and their traffick-.
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