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      Core Cross‐Linked Polymeric Micelles for Specific Iron Delivery: Inducing Sterile Inflammation in Macrophages

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          Macrophage plasticity and polarization: in vivo veritas.

          Diversity and plasticity are hallmarks of cells of the monocyte-macrophage lineage. In response to IFNs, Toll-like receptor engagement, or IL-4/IL-13 signaling, macrophages undergo M1 (classical) or M2 (alternative) activation, which represent extremes of a continuum in a universe of activation states. Progress has now been made in defining the signaling pathways, transcriptional networks, and epigenetic mechanisms underlying M1-M2 or M2-like polarized activation. Functional skewing of mononuclear phagocytes occurs in vivo under physiological conditions (e.g., ontogenesis and pregnancy) and in pathology (allergic and chronic inflammation, tissue repair, infection, and cancer). However, in selected preclinical and clinical conditions, coexistence of cells in different activation states and unique or mixed phenotypes have been observed, a reflection of dynamic changes and complex tissue-derived signals. The identification of mechanisms and molecules associated with macrophage plasticity and polarized activation provides a basis for macrophage-centered diagnostic and therapeutic strategies.
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            Macrophage Polarization.

            Macrophage polarization refers to how macrophages have been activated at a given point in space and time. Polarization is not fixed, as macrophages are sufficiently plastic to integrate multiple signals, such as those from microbes, damaged tissues, and the normal tissue environment. Three broad pathways control polarization: epigenetic and cell survival pathways that prolong or shorten macrophage development and viability, the tissue microenvironment, and extrinsic factors, such as microbial products and cytokines released in inflammation. A plethora of advances have provided a framework for rationally purifying, describing, and manipulating macrophage polarization. Here, I assess the current state of knowledge about macrophage polarization and enumerate the major questions about how activated macrophages regulate the physiology of normal and damaged tissues.
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              Distinct role of macrophages in different tumor microenvironments.

              Macrophages are prominent in the stromal compartment of virtually all types of malignancy. These highly versatile cells respond to the presence of stimuli in different parts of tumors with the release of a distinct repertoire of growth factors, cytokines, chemokines, and enzymes that regulate tumor growth, angiogenesis, invasion, and/or metastasis. The distinct microenvironments where tumor-associated macrophages (TAM) act include areas of invasion where TAMs promote cancer cell motility, stromal and perivascular areas where TAMs promote metastasis, and avascular and perinecrotic areas where hypoxic TAMs stimulate angiogenesis. This review will discuss the evidence for differential regulation of TAMs in these microenvironments and provide an overview of current attempts to target or use TAMs for therapeutic purposes.
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                Author and article information

                Contributors
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                Journal
                Advanced Healthcare Materials
                Adv. Healthcare Mater.
                Wiley
                2192-2640
                2192-2659
                October 2021
                June 16 2021
                October 2021
                : 10
                : 19
                : 2100385
                Affiliations
                [1 ]Leiden Academic Centre for Drug Research (LACDR) Leiden University Einsteinweg 55 Leiden 2333CC The Netherlands
                [2 ]Department of Chemistry Johannes Gutenberg University Mainz Duesbergweg 10‐14 Mainz 55128 Germany
                [3 ]European Molecular Biology Laboratory (EMBL) Collaboration for Joint PhD Degree between EMBL and the Faculty of Biosciences University of Heidelberg Meyerhofstr.1 Heidelberg 69117 Germany
                [4 ]Molecular Medicine Partnership Unit (MMPU) Otto‐Meyerhof‐Zentrum Im Neuenheimer Feld 350 Heidelberg 69120 Germany
                [5 ]Translational Lung Research Center Heidelberg (TLRC) German Center for Lung Research (DZL) University of Heidelberg Im Neuenheimer Feld 350 Heidelberg 69120 Germany
                [6 ]Department of Pediatric Oncology, Hematology, Immunology, and Pulmonology Heidelberg University Hospital Im Neuenheimer Feld 350 Heidelberg 69120 Germany
                [7 ]Department of Molecular Thoracic Oncology German Cancer Research Center (DKFZ) Im Neuenheimer Feld 280 Heidelberg 69120 Germany
                [8 ]Max Planck Institute for Polymer Research Ackermannweg 10 Mainz 55128 Germany
                [9 ]Department for Biosciences University of Oslo Blindernveien 31 Oslo 0371 Norway
                [10 ]Institute of Physics Johannes Gutenberg University Mainz Staudingerweg 9 Mainz 55128 Germany
                [11 ]Institute of Biochemistry I Faculty of Medicine Goethe‐University Frankfurt Theodor‐Stern‐Kai 7 Frankfurt am Main 60590 Germany
                Article
                10.1002/adhm.202100385
                34137217
                41428a2b-8917-4774-b098-3aea00003321
                © 2021

                http://creativecommons.org/licenses/by-nc/4.0/

                http://doi.wiley.com/10.1002/tdm_license_1.1

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