Combination of External Beam Radiotherapy (EBRT) With Intratumoral Injection of Dendritic Cells as Neo-Adjuvant Treatment of High-Risk Soft Tissue Sarcoma Patients

Finkelstein, Steven E.; Iclozan, Cristina; Bui, Marilyn M.; Cotter, Matthew J.; Ramakrishnan, Rupal; Ahmed, Jamil; Noyes, David; Cheong, David; Gonzalez, Ricardo J.; Heysek, Randy V.; Berman, Claudia G.; Lenox, Brianna; Janssen, William E.; Zager, Jonathan S.; Sondak, Vernon K.; Letson, G. Douglas; Antonia, Scott; Gabrilovich, Dmitry I.

doi:10.1016/j.ijrobp.2010.12.068

Cited by 106 publications

(68 citation statements)

References 29 publications

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“…At surgery, the tumors showed infiltration by T cells, with tumor-specific immune responses demonstrated in nine of 17 patients. Remarkably, at 1-year follow-up, 12 of 17 patients were free from progression of their cancer (115).…”

Section: Translation Of Successful Preclinical Combinations To the CLmentioning

confidence: 93%

Combining Radiotherapy and Cancer Immunotherapy: A Paradigm Shift

Formenti

Demaria²

2013

JNCI: Journal of the National Cancer Institute

852

660

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The therapeutic application of ionizing radiation has been largely based on its cytocidal power combined with the ability to selectively target tumors. Radiotherapy effects on survival of cancer patients are generally interpreted as the consequence of improved local control of the tumor, directly decreasing systemic spread. Experimental data from multiple cancer models have provided sufficient evidence to propose a paradigm shift, whereby some of the effects of ionizing radiation are recognized as contributing to systemic antitumor immunity. Recent examples of objective responses achieved by adding radiotherapy to immunotherapy in metastatic cancer patients support this view. Therefore, the traditional palliative role of radiotherapy in metastatic disease is evolving into that of a powerful adjuvant for immunotherapy. This combination strategy adds to the current anticancer arsenal and offers opportunities to harness the immune system to extend survival, even among metastatic and heavily pretreated cancer patients. We briefly summarize key evidence supporting the role of radiotherapy as an immune adjuvant. A critical appraisal of the current status of knowledge must include potential immunosuppressive effects of radiation that can hamper its capacity to convert the irradiated tumor into an in situ, individualized vaccine. Moreover, we discuss some of the current challenges to translate this knowledge to the clinic as more trials testing radiation with different immunotherapies are proposed.

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Section: Translation Of Successful Preclinical Combinations To the CLmentioning

confidence: 93%

Combining Radiotherapy and Cancer Immunotherapy: A Paradigm Shift

Formenti

Demaria²

2013

JNCI: Journal of the National Cancer Institute

852

660

View full text Add to dashboard Cite

show abstract

“…Early clinical trials testing vaccination with ex vivo generated DCs pulsed with tumor antigens provided proof-of-principle evidence that therapeutic immunity could be elicited; however, clinical benefit measured by regression of established tumors in patients with stage IV cancer was observed in only a small percentage of patients (Palucka et al 2008). Patients with soft tissue sarcoma who received fractionated external beam radiation in combination with administration of intratumoral DCs demonstrated an increased T-cell infiltration, with tumoral CD4 + T cells positively correlating with tumor-specific immune responses (Finkelstein et al 2011). Thus, new-generation DC vaccines are needed that generate large numbers of high avidity effector anti-tumor T cells able to overcome suppressive mechanisms in the tumor microenvironment.…”

Section: Cancer Immunotherapy I: Augmenting the Anti-tumor Immune Resmentioning

confidence: 99%

Immune microenvironments in solid tumors: new targets for therapy

Shiao¹,

Ganesan²,

Rugo³

et al. 2011

Genes Dev.

282

235

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Leukocytes and their soluble mediators play important regulatory roles in all aspects of solid tumor development. While immunotherapeutic strategies have conceptually held clinical promise, with the exception of a small percentage of patients, they have failed to demonstrate effective, consistent, and durable anti-cancer responses. Several subtypes of leukocytes that commonly infiltrate solid tumors harbor immunosuppressive activity and undoubtedly restrict the effectiveness of these strategies. Several of these same immune cells also foster tumor development by expression of potent protumor mediators. Given recent evidence revealing that immune-based mechanisms regulate the response to conventional cytotoxic therapy, it seems reasonable to speculate that tumor progression could be effectively diminished by combining cytotoxic strategies with therapies that blunt protumor immunebased effectors and/or neutralize those that instead impede development of desired anti-tumor immunity, thus providing synergistic effects between traditional cytotoxic and immune-modulatory approaches.

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“…A particularly exciting development, hailed by the editors of Science as the scientific breakthrough of 2013 (5), is that novel immunotherapeutic strategies show remarkable responses in some patients, especially if combined with common cytotoxic agents. Radiotherapy and chemotherapeutic agents have been shown to substantially enhance tumorspecific immune responses in well-established tumors (4,(6)(7)(8)(9)(10)(11). The synergy between radiotherapy and immunotherapy stems from radiation-induced effects including (i) immunogenic cell death that locally exposes a wealth of tumor antigens and…”

Section: Introductionmentioning

confidence: 99%

Abscopal Benefits of Localized Radiotherapy Depend on Activated T-cell Trafficking and Distribution between Metastatic Lesions

et al. 2016

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It remains unclear how localized radiotherapy for cancer metastases can occasionally elicit a systemic antitumor effect, known as the abscopal effect, but historically, it has been speculated to reflect the generation of a host immunotherapeutic response. The ability to purposefully and reliably induce abscopal effects in metastatic tumors could meet many unmet clinical needs. Here, we describe a mathematical model that incorporates physiologic information about T-cell trafficking to estimate the distribution of focal therapy-activated T cells between metastatic lesions. We integrated a dynamic model of tumor-immune interactions with systemic T-cell trafficking patterns to simulate the development of metastases. In virtual case studies, we found that the dissemination of activated T cells among multiple metastatic sites is complex and not intuitively predictable. Furthermore, we show that not all metastatic sites participate in systemic immune surveillance equally, and therefore the success in triggering the abscopal effect depends, at least in part, on which metastatic site is selected for localized therapy. Moreover, simulations revealed that seeding new metastatic sites may accelerate the growth of the primary tumor, because T-cell responses are partially diverted to the developing metastases, but the removal of the primary tumor can also favor the rapid growth of preexisting metastatic lesions. Collectively, our work provides the framework to prospectively identify anatomically defined focal therapy targets that are most likely to trigger an immune-mediated abscopal response and therefore may inform personalized treatment strategies in patients with metastatic disease. Cancer Res; 76(5); 1009-18. Ó2016 AACR.

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Combination of External Beam Radiotherapy (EBRT) With Intratumoral Injection of Dendritic Cells as Neo-Adjuvant Treatment of High-Risk Soft Tissue Sarcoma Patients

Cited by 106 publications

References 29 publications

Combining Radiotherapy and Cancer Immunotherapy: A Paradigm Shift

Combining Radiotherapy and Cancer Immunotherapy: A Paradigm Shift

Immune microenvironments in solid tumors: new targets for therapy

Abscopal Benefits of Localized Radiotherapy Depend on Activated T-cell Trafficking and Distribution between Metastatic Lesions

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