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The Potential of Combining Tubulin-Targeting Anticancer Therapeutics and Immune Therapy

Cancer immune therapy has recently shown tremendous promise to combat many different cancers. The microtubule is a well-defined and very effective cancer therapeutic target. Interestingly, several lines of evidence now suggest that microtubules are intimately connected to the body’s immune responses...

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Autores principales: Fong, Alexis, Durkin, Amanda, Lee, Hoyun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6387102/
https://www.ncbi.nlm.nih.gov/pubmed/30704031
http://dx.doi.org/10.3390/ijms20030586
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author Fong, Alexis
Durkin, Amanda
Lee, Hoyun
author_facet Fong, Alexis
Durkin, Amanda
Lee, Hoyun
author_sort Fong, Alexis
collection PubMed
description Cancer immune therapy has recently shown tremendous promise to combat many different cancers. The microtubule is a well-defined and very effective cancer therapeutic target. Interestingly, several lines of evidence now suggest that microtubules are intimately connected to the body’s immune responses. This raises the possibility that the combination of microtubule inhibitors and immune therapy can be a highly effective option for cancer treatments. However, our understanding on this potentially important aspect is still very limited, due in part to the multifaceted nature of microtubule functions. Microtubules are not only involved in maintaining cell morphology, but also a variety of cellular processes, including the movement of secretory vesicles and organelles, intracellular macromolecular assembly, signaling pathways, and cell division. Microtubule inhibitors may be subdivided into two classes: Anti-depolymerization agents such as the taxane family, and anti-polymerization agents such as colchicine and vinka alkaloids. These two different classes may have different effects on immune cell subtypes. Anti-depolymerization agents can not only induce NK cells, but also appear to inhibit T regulatory (Treg) cells. However, different inhibitors may have different functions even among the same class. For example, the doxetaxel anti-depolymerization agent up-regulates cytotoxic T cells, while paclitaxel down-regulates them. Certain anti-polymerization agents such as colchicine appear to down-regulate most immune cell types, while inducing dendritic cell maturation and increasing M1 macrophage population. In contrast, the vinblastine anti-polymerization agent activates many of these cell types, albeit down-regulating Treg cells. In this review, we focus on the various effects of tubulin inhibitors on the activities of the body’s immune system, in the hope of paving the way to develop an effective cancer therapy by combining tubulin-targeting anticancer agents and immune therapy.
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spelling pubmed-63871022019-02-27 The Potential of Combining Tubulin-Targeting Anticancer Therapeutics and Immune Therapy Fong, Alexis Durkin, Amanda Lee, Hoyun Int J Mol Sci Review Cancer immune therapy has recently shown tremendous promise to combat many different cancers. The microtubule is a well-defined and very effective cancer therapeutic target. Interestingly, several lines of evidence now suggest that microtubules are intimately connected to the body’s immune responses. This raises the possibility that the combination of microtubule inhibitors and immune therapy can be a highly effective option for cancer treatments. However, our understanding on this potentially important aspect is still very limited, due in part to the multifaceted nature of microtubule functions. Microtubules are not only involved in maintaining cell morphology, but also a variety of cellular processes, including the movement of secretory vesicles and organelles, intracellular macromolecular assembly, signaling pathways, and cell division. Microtubule inhibitors may be subdivided into two classes: Anti-depolymerization agents such as the taxane family, and anti-polymerization agents such as colchicine and vinka alkaloids. These two different classes may have different effects on immune cell subtypes. Anti-depolymerization agents can not only induce NK cells, but also appear to inhibit T regulatory (Treg) cells. However, different inhibitors may have different functions even among the same class. For example, the doxetaxel anti-depolymerization agent up-regulates cytotoxic T cells, while paclitaxel down-regulates them. Certain anti-polymerization agents such as colchicine appear to down-regulate most immune cell types, while inducing dendritic cell maturation and increasing M1 macrophage population. In contrast, the vinblastine anti-polymerization agent activates many of these cell types, albeit down-regulating Treg cells. In this review, we focus on the various effects of tubulin inhibitors on the activities of the body’s immune system, in the hope of paving the way to develop an effective cancer therapy by combining tubulin-targeting anticancer agents and immune therapy. MDPI 2019-01-30 /pmc/articles/PMC6387102/ /pubmed/30704031 http://dx.doi.org/10.3390/ijms20030586 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Review
Fong, Alexis
Durkin, Amanda
Lee, Hoyun
The Potential of Combining Tubulin-Targeting Anticancer Therapeutics and Immune Therapy
title The Potential of Combining Tubulin-Targeting Anticancer Therapeutics and Immune Therapy
title_full The Potential of Combining Tubulin-Targeting Anticancer Therapeutics and Immune Therapy
title_fullStr The Potential of Combining Tubulin-Targeting Anticancer Therapeutics and Immune Therapy
title_full_unstemmed The Potential of Combining Tubulin-Targeting Anticancer Therapeutics and Immune Therapy
title_short The Potential of Combining Tubulin-Targeting Anticancer Therapeutics and Immune Therapy
title_sort potential of combining tubulin-targeting anticancer therapeutics and immune therapy
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6387102/
https://www.ncbi.nlm.nih.gov/pubmed/30704031
http://dx.doi.org/10.3390/ijms20030586
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