In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology

In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology

FDA approval of anti-CTLA4 in 2011 for melanoma immunotherapy was paradigm shifting and dramatically accelerated cancer immunotherapy research. The investment and effort have been exceptionally large, with a commensurate impressive pace of discovery. Historical and current research has validated the...

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Main Authors: Chenkai Mao, Michael-Joseph Gorbet, Akansha Singh, Ashish Ranjan, Steven Fiering
Format: Article
Language:English
Published: Taylor & Francis Group 2020-12-01
Series:International Journal of Hyperthermia
Subjects:
in situ vaccination
cancer immunotherapy
nanotechnology
nanoparticles
Online Access:http://dx.doi.org/10.1080/02656736.2020.1810333
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spelling doaj-5c859731bb1e4bb9a21cf3d094b95e4e2021-01-26T11:50:08ZengTaylor & Francis GroupInternational Journal of Hyperthermia0265-67361464-51572020-12-0137341710.1080/02656736.2020.18103331810333In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunologyChenkai Mao0Michael-Joseph Gorbet1Akansha Singh2Ashish Ranjan3Steven Fiering4Department of Microbiology and Immunology, Geisel School of Medicine at DartmouthDepartment of Physiological Sciences, College of Veterinary Medicine, Oklahoma State UniversityDepartment of Physiological Sciences, College of Veterinary Medicine, Oklahoma State UniversityDepartment of Physiological Sciences, College of Veterinary Medicine, Oklahoma State UniversityDepartment of Microbiology and Immunology, Geisel School of Medicine at DartmouthFDA approval of anti-CTLA4 in 2011 for melanoma immunotherapy was paradigm shifting and dramatically accelerated cancer immunotherapy research. The investment and effort have been exceptionally large, with a commensurate impressive pace of discovery. Historical and current research has validated the following key points: tumors are recognized by the immune system; tumors develop an immunosuppressive environment which suppresses the antitumor immune response; successful immunotherapy must overcome that tumor-mediated immunosuppression. While cancer immunotherapy research expanded, a parallel effort developing nanoparticles (NP) for cancer diagnosis and therapy also received major investment and expanded. Initially the two efforts appeared to have minimal synergy. Systemically administered nanoparticles are rapidly ingested by phagocytic leukocytes, and therefore nanotechnologists developed strategies to avoid NP ingestion by leukocytes in order to accomplish nanoparticle accumulation in tumors rather than liver and spleen. Recently, nanotechnology and cancer immunotherapy have increasingly merged since phagocytic leukocytes are the key to reversing the local tumor immunosuppression and the tendency of NP to be phagocytosed can be exploited to manipulate phagocytes for immunotherapy. This review focuses on in situ vaccination (ISV), an immunotherapy approach that can utilize direct injection of immunostimulatory reagents, including NPs, into tumors to disrupt the local immunosuppression, stimulate effective immune response against the treated tumor, and most importantly, generate a systemic antitumor immune response to eliminate metastatic tumors. While there are many specific options for using NP for ISV (reviewed further in this special issue), this review focuses on immunology concepts needed to understand and design successful NP ISV approaches.http://dx.doi.org/10.1080/02656736.2020.1810333in situ vaccinationcancer immunotherapynanotechnologynanoparticles
collection DOAJ
language English
format Article
sources DOAJ
author Chenkai Mao
Michael-Joseph Gorbet
Akansha Singh
Ashish Ranjan
Steven Fiering
spellingShingle Chenkai Mao
Michael-Joseph Gorbet
Akansha Singh
Ashish Ranjan
Steven Fiering
In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology
International Journal of Hyperthermia
in situ vaccination
cancer immunotherapy
nanotechnology
nanoparticles
author_facet Chenkai Mao
Michael-Joseph Gorbet
Akansha Singh
Ashish Ranjan
Steven Fiering
author_sort Chenkai Mao
title In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology
title_short In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology
title_full In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology
title_fullStr In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology
title_full_unstemmed In situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology
title_sort in situ vaccination with nanoparticles for cancer immunotherapy: understanding the immunology
publisher Taylor & Francis Group
series International Journal of Hyperthermia
issn 0265-6736
1464-5157
publishDate 2020-12-01
description FDA approval of anti-CTLA4 in 2011 for melanoma immunotherapy was paradigm shifting and dramatically accelerated cancer immunotherapy research. The investment and effort have been exceptionally large, with a commensurate impressive pace of discovery. Historical and current research has validated the following key points: tumors are recognized by the immune system; tumors develop an immunosuppressive environment which suppresses the antitumor immune response; successful immunotherapy must overcome that tumor-mediated immunosuppression. While cancer immunotherapy research expanded, a parallel effort developing nanoparticles (NP) for cancer diagnosis and therapy also received major investment and expanded. Initially the two efforts appeared to have minimal synergy. Systemically administered nanoparticles are rapidly ingested by phagocytic leukocytes, and therefore nanotechnologists developed strategies to avoid NP ingestion by leukocytes in order to accomplish nanoparticle accumulation in tumors rather than liver and spleen. Recently, nanotechnology and cancer immunotherapy have increasingly merged since phagocytic leukocytes are the key to reversing the local tumor immunosuppression and the tendency of NP to be phagocytosed can be exploited to manipulate phagocytes for immunotherapy. This review focuses on in situ vaccination (ISV), an immunotherapy approach that can utilize direct injection of immunostimulatory reagents, including NPs, into tumors to disrupt the local immunosuppression, stimulate effective immune response against the treated tumor, and most importantly, generate a systemic antitumor immune response to eliminate metastatic tumors. While there are many specific options for using NP for ISV (reviewed further in this special issue), this review focuses on immunology concepts needed to understand and design successful NP ISV approaches.
topic in situ vaccination
cancer immunotherapy
nanotechnology
nanoparticles
url http://dx.doi.org/10.1080/02656736.2020.1810333
work_keys_str_mv AT chenkaimao insituvaccinationwithnanoparticlesforcancerimmunotherapyunderstandingtheimmunology
AT michaeljosephgorbet insituvaccinationwithnanoparticlesforcancerimmunotherapyunderstandingtheimmunology
AT akanshasingh insituvaccinationwithnanoparticlesforcancerimmunotherapyunderstandingtheimmunology
AT ashishranjan insituvaccinationwithnanoparticlesforcancerimmunotherapyunderstandingtheimmunology
AT stevenfiering insituvaccinationwithnanoparticlesforcancerimmunotherapyunderstandingtheimmunology
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