Issue 3, 2014

ER stress, autophagy and immunogenic cell death in photodynamic therapy-induced anti-cancer immune responses

Abstract

Tumours are a form of pseudo-organs with their own microenvironment where the cancer cells nurture a dysfunctional immune environment incapable of inciting anti-tumour immunity. It had been proposed that the only way to counteract such an immune system dysfunction in tumours is by eliciting, therapeutically, a cancer cell death pathway that is accompanied by high immunogenicity and possibly inhibits or reduces the influence of the pro-tumourigenic cytokine signalling. Subsequently, a small and a large-scale screening study as well as several targeted studies found that few, selected anticancer therapeutic regimens are able to induce a promising kind of cancer cell demise called immunogenic cell death (ICD), which can activate the immune system owing to the spatiotemporally defined emission of danger signals. Recently, photodynamic therapy (PDT) utilizing the photosensitiser, hypericin (Hyp), became the first PDT paradigm characterized to be capable of inducing bona fide ICD. In the present perspective, we discuss the various technical, conceptual, and molecular advancements and unprecedented results revealed by Hyp-PDT that have influenced the fields of ICD, ER stress biology, cancer cell death, anti-cancer immune responses, photoimmunology and PDT.

Graphical abstract: ER stress, autophagy and immunogenic cell death in photodynamic therapy-induced anti-cancer immune responses

Article information

Article type
Perspective
Submitted
18 Sep 2013
Accepted
14 Jan 2014
First published
15 Jan 2014

Photochem. Photobiol. Sci., 2014,13, 474-487

Author version available

ER stress, autophagy and immunogenic cell death in photodynamic therapy-induced anti-cancer immune responses

A. D. Garg and P. Agostinis, Photochem. Photobiol. Sci., 2014, 13, 474 DOI: 10.1039/C3PP50333J

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