Boosting Tumor-Specific Immunity Using PDT

Maeding, Nicole; Verwanger, Thomas; Krammer, Barbara

doi:10.3390/cancers8100091

Cited by 83 publications

(71 citation statements)

References 78 publications

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“…Several landmark reviews by Castano et al (2006), Mroz et al (2011) and Meading et al . (2016) have described in depth how PDT is capable of eliciting tumor‐specific adaptive immunity . In this review, we will focus only on the major steps involved in achieving an adaptive antitumor response following photodynamic insult to tumors to bridge the fundamentals of photochemistry, ICD and adaptive immunity with the potential for enriching the T‐cell repertoire (Fig.…”

Section: Activation Of the Adaptive Immune Systemmentioning

confidence: 99%

The Course of Immune Stimulation by Photodynamic Therapy: Bridging Fundamentals of Photochemically Induced Immunogenic Cell Death to the Enrichment of T‐Cell Repertoire

Nath

Obaid

Hasan

2019

Photochem & Photobiology

103

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Photodynamic therapy (PDT) is a potentially immunogenic and FDA‐approved antitumor treatment modality that utilizes the spatiotemporal combination of a photosensitizer, light and oftentimes oxygen, to generate therapeutic cytotoxic molecules. Certain photosensitizers under specific conditions, including ones in clinical practice, have been shown to elicit an immune response following photoillumination. When localized within tumor tissue, photogenerated cytotoxic molecules can lead to immunogenic cell death (ICD) of tumor cells, which release damage‐associated molecular patterns and tumor‐specific antigens. Subsequently, the T‐lymphocyte (T cell)–mediated adaptive immune system can become activated. Activated T cells then disseminate into systemic circulation and can eliminate primary and metastatic tumors. In this review, we will detail the multistage cascade of events following PDT of solid tumors that ultimately lead to the activation of an antitumor immune response. More specifically, we connect the fundamentals of photochemically induced ICD with a proposition on potential mechanisms for PDT enhancement of the adaptive antitumor response. We postulate a hypothesis that during the course of the immune stimulation process, PDT also enriches the T‐cell repertoire with tumor‐reactive activated T cells, diversifying their tumor‐specific targets and eliciting a more expansive and rigorous antitumor response. The implications of such a process are likely to impact the outcomes of rational combinations with immune checkpoint blockade, warranting investigations into T‐cell diversity as a previously understudied and potentially transformative paradigm in antitumor photodynamic immunotherapy.

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Section: Activation Of the Adaptive Immune Systemmentioning

confidence: 99%

The Course of Immune Stimulation by Photodynamic Therapy: Bridging Fundamentals of Photochemically Induced Immunogenic Cell Death to the Enrichment of T‐Cell Repertoire

Nath

Obaid

Hasan

2019

Photochem & Photobiology

103

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“…Ample evidence shows that both the innate and adaptive immune systems participate in PDT-induced tumour elimination (Nowis et al 2005;Castano et al, 2006). The immune response is activated by PDT-induced tumour cell death or damage, which triggers the release of various damage-associated molecular patterns (DAMPs) including heat shock protein 70 (HSP70), calreticulin (CRT), high-mobility group box 1 (HMDB1), and ATP (Korbelik 2006;Maeding et al 2016;Tanaka et al 2016). A particularly immunogenic type of cell death is necrosis, where a lot of DAMPs are released, but apoptotic and stressed cells contribute as well, especially if the extent of damage is large and/or rapidly peaks upon PDT application (Korbelik 2006).…”

Section: Pdt and The Immune System Pdt-mediated Immune Responses In Cmentioning

confidence: 99%

Porphyrin-based cationic amphiphilic photosensitisers as potential anticancer, antimicrobial and immunosuppressive agents

2017

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Photodynamic therapy (PDT) combines a photosensitiser, light and molecular oxygen to induce oxidative stress that can be used to kill pathogens, cancer cells and other highly proliferative cells. There is a growing number of clinically approved photosensitisers and applications of PDT, whose main advantages include the possibility of selective targeting, localised action and stimulation of the immune responses. Further improvements and broader use of PDT could be accomplished by designing new photosensitisers with increased selectivity and bioavailability. Porphyrin-based photosensitisers with amphiphilic properties, bearing one or more positive charges, are an effective tool in PDT against cancers, microbial infections and, most recently, autoimmune skin disorders. The aim of the review is to present some of the recent examples of the applications and research that employ this specific group of photosensitisers. Furthermore, we will highlight the link between their structural characteristics and PDT efficiency, which will be helpful as guidelines for rational design and evaluation of new PSs.

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“…103,104 Therefore, oxygen self-enriched nanoparticles are beneficial for not only the enhanced PDT effect but also for overcoming chemoresistance. 106 Kabingu et al demonstrated that local PDT can inhibit the growth of the primary tumor and the untreated distant tumors due to the infiltration of CD8 + T cells. Tumor cells undergoing apoptosis or necrosis release tumor-associated antigens.…”

Section: Recent Advance Of Nanoparticle-based Pdtmentioning

confidence: 99%

Nanoparticle‐based photothermal and photodynamic immunotherapy for tumor treatment

Hou

Tao

Pang

et al. 2018

Intl Journal of Cancer

186

123

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Nanoparticle-based phototherapies, such as photothermal therapy (PTT) and photodynamic therapy (PDT), exhibit strong efficacy, minimal invasion and negligible side effects in tumor treatment. These phototherapies have received considerable attention and been extensively studied in recent years. In addition to directly killing tumor cells through heat and reactive oxygen species, PTT and PDT can also induce various antitumor effects. In particular, the resultant massive tumor cell death after PTT and PDT triggers immune responses, including the redistribution and activation of immune effector cells, the expression and secretion of cytokines and the transformation of memory T lymphocytes. The antitumor effects can be enhanced by immune checkpoint blockage therapy. This article reviewed the recent advances of nanoparticle-based PTT and PDT, summarized the studies on nanoparticle-based photothermal and photodynamic immunotherapies in vitro and in vivo, and discussed challenges and future research directions.

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Boosting Tumor-Specific Immunity Using PDT

Cited by 83 publications

References 78 publications

The Course of Immune Stimulation by Photodynamic Therapy: Bridging Fundamentals of Photochemically Induced Immunogenic Cell Death to the Enrichment of T‐Cell Repertoire

The Course of Immune Stimulation by Photodynamic Therapy: Bridging Fundamentals of Photochemically Induced Immunogenic Cell Death to the Enrichment of T‐Cell Repertoire

Porphyrin-based cationic amphiphilic photosensitisers as potential anticancer, antimicrobial and immunosuppressive agents

Nanoparticle‐based photothermal and photodynamic immunotherapy for tumor treatment

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