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      Molecular machineries of pH dysregulation in tumor microenvironment: potential targets for cancer therapy

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          Abstract

          Introduction: Cancer is an intricate disorder/dysfunction of cells that can be defined as a genetic heterogeneity in human disease. Therefore, it is characterized by several adaptive complex hallmarks. Among them, the pH dysregulation appears as a symbol of aberrant functions within the tumor microenvironment (TME). In comparison with normal tissues, in the solid tumors, we face with an irregular acidification and alkalinization of the extracellular and intracellular fluids.

          Methods: In this study, we comprehensively discussed the most recent reports on the hallmarks of solid tumors to provide deep insights upon the molecular machineries involved in the pH dysregulation of solid tumors and their impacts on the initiation and progression of cancer.

          Results: The dysregulation of pH in solid tumors is fundamentally related to the Warburg effect and hypoxia, leading to expression of a number of molecular machineries, including: NHE1, H+ pump V-ATPase, CA-9, CA-12, MCT-1, GLUT-1. Activation of proton exchangers and transporters (PETs) gives rise to formation of TME. This condition favors the cancer cells to evade from the anoikis and apoptosis, granting them aggressive and metastasis phenotype, as well as resistance to chemotherapy and radiation therapy. This review aimed to discuss the key molecular changes of tumor cells in terms of bio-energetics and cancer metabolism in relation with pH dysregulation. During this phenomenon, the intra- and extracellular metabolites are altered and/or disrupted. Such molecular alterations provide molecular hallmarks for direct targeting of the PETs by potent relevant inhibitors in combination with conventional cancer therapies as ultimate therapy against solid tumors.

          Conclusion: Taken all, along with other treatment strategies, targeting the key molecular machineries related to intra- and extracellular metabolisms within the TME is proposed as a novel strategy to inhibit or block PETs that are involved in the pH dysregulation of solid tumors.

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            The extracellular matrix (ECM) may contribute to the drug resistance of a solid tumor by preventing the penetration of therapeutic agents. We measured differences in interstitial resistance to macromolecule (IgG) motion in four tumor types and found an unexpected correspondence between transport resistance and the mechanical stiffness. The interstitial diffusion coefficient of IgG was measured in situ by fluorescence redistribution after photobleaching. Tissue elastic modulus and hydraulic conductivity were measured by confined compression of excised tissue. In apparent contradiction to an existing paradigm, these functional properties are correlated with total tissue content of collagen, not glycosaminoglycan. An extended collagen network was observed in the more penetration-resistant tumors. Collagenase treatment of the more penetration-resistant tumors significantly increased the IgG interstitial diffusion rate. We conclude that collagen influences the tissue resistance to macromolecule transport, possibly by binding and stabilizing the glycosaminoglycan component of the ECM. These findings suggest a new method to screen tumors for potential resistance to macromolecule-based therapy. Moreover, collagen and collagen-proteoglycan bonds are identified as potential targets of treatment to improve macromolecule delivery.
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              Macrophages and cathepsin proteases blunt chemotherapeutic response in breast cancer.

              Tanaya Shree, Oakley Olson, Benelita Elie (2011)
              The microenvironment is known to critically modulate tumor progression, yet its role in regulating treatment response is poorly understood. Here we found increased macrophage infiltration and cathepsin protease levels in mammary tumors following paclitaxel (Taxol) chemotherapy. Cathepsin-expressing macrophages protected against Taxol-induced tumor cell death in coculture, an effect fully reversed by cathepsin inhibition and mediated partially by cathepsins B and S. Macrophages were also found to protect against tumor cell death induced by additional chemotherapeutics, specifically etoposide and doxorubicin. Combining Taxol with cathepsin inhibition in vivo significantly enhanced efficacy against primary and metastatic tumors, supporting the therapeutic relevance of this effect. Additionally incorporating continuous low-dose cyclophosphamide dramatically impaired tumor growth and metastasis and improved survival. This study highlights the importance of integrated targeting of the tumor and its microenvironment and implicates macrophages and cathepsins in blunting chemotherapeutic response.
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                Author and article information

                Journal
                Journal ID (nlm-ta): Bioimpacts
                Journal ID (iso-abbrev): Bioimpacts
                Journal ID (publisher-id): BioImpacts
                Title: BioImpacts : BI
                Publisher: Tabriz University of Medical Sciences
                ISSN (Print): 2228-5652
                ISSN (Electronic): 2228-5660
                Publication date (Print): 2017
                Publication date (Electronic): 07 June 2017
                Volume: 7
                Issue: 2
                Pages: 115-133
                Affiliations
                1Department of Biology, Fars Science and Research Branch, Islamic Azad University, Marvdasht, Iran
                2Department of Biology, Marvdasht Branch, Islamic Azad University, Marvdasht, Iran
                3Research Center for Pharmaceutical Nanotechnology, Biomedicine Institute, Tabriz University of Medical Sciences, Tabriz, Iran
                4Department of Pharmaceutics, Faculty of Pharmacy, Tabriz University of Medical Sciences, Tabriz, Iran
                5Department of Genetic, Tabriz Branch, Islamic Azad University, Tabriz, Iran
                Author notes
                [* ] Corresponding author: Yadollah Omidi, yomidi@ 123456yahoo.com
                Article
                DOI: 10.15171/bi.2017.15
                PMC ID: 5524986
                PubMed ID: 28752076
                SO-VID: 9115e49c-b6c7-4bd3-9923-ad4857063882
                Copyright © © 2017 The Author(s)
                License:

                This work is published by BioImpacts as an open access article distributed under the terms of the Creative Commons Attribution License ( http://creativecommons.org/licenses/by-nc/4.0/). Non-commercial uses of the work are permitted, provided the original work is properly cited.

                History
                Date received : 24 April 2017
                Date revision received : 28 May 2017
                Date accepted : 06 June 2017
                Page count
                Figures: 6, Tables: 1, References: 182, Pages: 19
                Categories
                Subject: Review

                Keywords: cancer,carbonic anhydrases,hypoxia,ph dysregulation,sodium-hydrogen exchanger,tumor microenvironment,vacuolar-type h+-atpase,targeted therapy of cancer,synthetic lethality
                Data availability:
                Keywords: cancer, carbonic anhydrases, hypoxia, ph dysregulation, sodium-hydrogen exchanger, tumor microenvironment, vacuolar-type h+-atpase, targeted therapy of cancer, synthetic lethality

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