Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment

Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment

Neutrophils, the most abundant leukocytes in human blood, are essential fighter immune cells against microbial infection. Based on the finding that neutrophils can either restrict or promote cancer progression, tumor-associated neutrophils (TAN) are classified into anti-tumor N1 and pro-tumor N2 sub...

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Main Authors: Yuting Zhang, Guoqiang Liu, Miaomiao Sun, Xin Lu
Format: Article
Language:English
Published: China Anti-Cancer Association 2020-02-01
Series:Cancer Biology & Medicine
Subjects:
tumor-associated neutrophil
polymorphonuclear myeloid-derived suppressor cell
immunosuppression
cancer immunotherapy
nanoparticle drug delivery
Online Access:http://www.cancerbiomed.org/index.php/cocr/article/view/1566
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spelling doaj-aa7a24424d5e4de1b73e43855b396ffd2020-11-25T03:25:48ZengChina Anti-Cancer AssociationCancer Biology & Medicine2095-39412020-02-01171324310.20892/j.issn.2095-3941.2019.0372Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatmentYuting Zhang0Guoqiang Liu1Miaomiao Sun2Xin Lu3Department of Biological Sciences, Boler-Parseghian Center for Rare and Neglected Diseases, Harper Cancer Research Institute, University of Notre Dame, Notre Dame, IN 46556, USADepartment of Biological Sciences, Boler-Parseghian Center for Rare and Neglected Diseases, Harper Cancer Research Institute, University of Notre Dame, Notre Dame, IN 46556, USADepartment of Biological Sciences, Boler-Parseghian Center for Rare and Neglected Diseases, Harper Cancer Research Institute, University of Notre Dame, Notre Dame, IN 46556, USADepartment of Biological Sciences, Boler-Parseghian Center for Rare and Neglected Diseases, Harper Cancer Research Institute, University of Notre Dame, Notre Dame, IN 46556, USANeutrophils, the most abundant leukocytes in human blood, are essential fighter immune cells against microbial infection. Based on the finding that neutrophils can either restrict or promote cancer progression, tumor-associated neutrophils (TAN) are classified into anti-tumor N1 and pro-tumor N2 subsets. One of the major mechanisms underlying the tumor-promoting function of N2-TANs is suppression of adaptive immune cells, in particular, cytotoxic T lymphocytes. Currently, no established methodologies are available that can unequivocally distinguish immunosuppressive TANs and granulocytic/polymorphonuclear myeloid-derived suppressor cells (G/PMN-MDSC). In view of the critical role of PMN-MDSCs in immune evasion and resistance to cancer immunotherapy, as established from data obtained with diverse cancer models, therapeutic strategies targeting these cells have been actively developed to enhance the efficacy of immunotherapy. Here, we have reviewed the available literature on strategies targeting PMN-MDSCs and summarized the findings into four categories: (1) depletion of existing PMN-MDSCs, (2) blockade of the development of PMN-MDSCs, (3) blockade of PMN-MDSC recruitment, (4) inhibition of immunosuppressive function. Owing to their high mobility to inflamed organs and ability to trespass the blood-brain barrier, neutrophils are outstanding candidate carriers in nanoparticle-based therapies. Another attractive application of neutrophils in cancer therapy is the use of neutrophil membrane-derived nanovesicles as a surrogate of extracellular vesicles for more efficient and scalable drug delivery. In the second part of the review, we have highlighted recent advances in the field of neutrophil-based cancer drug delivery. Overall, we believe that neutrophil-based therapeutics are a rapidly growing area of cancer therapy with significant potential benefits.http://www.cancerbiomed.org/index.php/cocr/article/view/1566tumor-associated neutrophilpolymorphonuclear myeloid-derived suppressor cellimmunosuppressioncancer immunotherapynanoparticle drug delivery
collection DOAJ
language English
format Article
sources DOAJ
author Yuting Zhang
Guoqiang Liu
Miaomiao Sun
Xin Lu
spellingShingle Yuting Zhang
Guoqiang Liu
Miaomiao Sun
Xin Lu
Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment
Cancer Biology & Medicine
tumor-associated neutrophil
polymorphonuclear myeloid-derived suppressor cell
immunosuppression
cancer immunotherapy
nanoparticle drug delivery
author_facet Yuting Zhang
Guoqiang Liu
Miaomiao Sun
Xin Lu
author_sort Yuting Zhang
title Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment
title_short Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment
title_full Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment
title_fullStr Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment
title_full_unstemmed Targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment
title_sort targeting and exploitation of tumor-associated neutrophils to enhance immunotherapy and drug delivery for cancer treatment
publisher China Anti-Cancer Association
series Cancer Biology & Medicine
issn 2095-3941
publishDate 2020-02-01
description Neutrophils, the most abundant leukocytes in human blood, are essential fighter immune cells against microbial infection. Based on the finding that neutrophils can either restrict or promote cancer progression, tumor-associated neutrophils (TAN) are classified into anti-tumor N1 and pro-tumor N2 subsets. One of the major mechanisms underlying the tumor-promoting function of N2-TANs is suppression of adaptive immune cells, in particular, cytotoxic T lymphocytes. Currently, no established methodologies are available that can unequivocally distinguish immunosuppressive TANs and granulocytic/polymorphonuclear myeloid-derived suppressor cells (G/PMN-MDSC). In view of the critical role of PMN-MDSCs in immune evasion and resistance to cancer immunotherapy, as established from data obtained with diverse cancer models, therapeutic strategies targeting these cells have been actively developed to enhance the efficacy of immunotherapy. Here, we have reviewed the available literature on strategies targeting PMN-MDSCs and summarized the findings into four categories: (1) depletion of existing PMN-MDSCs, (2) blockade of the development of PMN-MDSCs, (3) blockade of PMN-MDSC recruitment, (4) inhibition of immunosuppressive function. Owing to their high mobility to inflamed organs and ability to trespass the blood-brain barrier, neutrophils are outstanding candidate carriers in nanoparticle-based therapies. Another attractive application of neutrophils in cancer therapy is the use of neutrophil membrane-derived nanovesicles as a surrogate of extracellular vesicles for more efficient and scalable drug delivery. In the second part of the review, we have highlighted recent advances in the field of neutrophil-based cancer drug delivery. Overall, we believe that neutrophil-based therapeutics are a rapidly growing area of cancer therapy with significant potential benefits.
topic tumor-associated neutrophil
polymorphonuclear myeloid-derived suppressor cell
immunosuppression
cancer immunotherapy
nanoparticle drug delivery
url http://www.cancerbiomed.org/index.php/cocr/article/view/1566
work_keys_str_mv AT yutingzhang targetingandexploitationoftumorassociatedneutrophilstoenhanceimmunotherapyanddrugdeliveryforcancertreatment
AT guoqiangliu targetingandexploitationoftumorassociatedneutrophilstoenhanceimmunotherapyanddrugdeliveryforcancertreatment
AT miaomiaosun targetingandexploitationoftumorassociatedneutrophilstoenhanceimmunotherapyanddrugdeliveryforcancertreatment
AT xinlu targetingandexploitationoftumorassociatedneutrophilstoenhanceimmunotherapyanddrugdeliveryforcancertreatment
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