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      CD13 promotes mesenchymal stem cell-mediated regeneration of ischemic muscle

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          Abstract

          Mesenchymal stem cells (MSCs) are multipotent, tissue-resident cells that can facilitate tissue regeneration and thus, show great promise as potential therapeutic agents. Functional MSCs have been isolated and characterized from a wide array of adult tissues and are universally identified by the shared expression of a core panel of MSCs markers. One of these markers is the multifunctional cell surface peptidase CD13 that has been shown to be expressed on human and murine MSCs from many tissues. To investigate whether this universal expression indicates a functional role for CD13 in MSC biology we isolated, expanded and characterized MSCs from bone marrow of wild type (WT) and CD13 KO mice. Characterization of these cells demonstrated that both WT and CD13 KO MSCs expressed the full complement of MSC markers (CD29, CD44, CD49e, CD105, Sca1), showed comparable proliferation rates and were capable of differentiating toward the adipogenic and osteogenic lineages. However, MSCs lacking CD13 were unable to differentiate into vascular cells, consistent with our previous characterization of CD13 as an angiogenic regulator. Compared to WT MSCs, adhesion and migration on various extracellular matrices of CD13 KO MSCs were significantly impaired, which correlated with decreased phospho-FAK levels and cytoskeletal alterations. Crosslinking human MSCs with activating CD13 antibodies increased cell adhesion to endothelial monolayers and induced FAK activation in a time dependent manner. In agreement with these in vitro data, intramuscular injection of CD13 KO MSCs in a model of severe ischemic limb injury resulted in significantly poorer perfusion, decreased ambulation, increased necrosis and impaired vascularization compared to those receiving WT MSCs. This study suggests that CD13 regulates FAK activation to promote MSC adhesion and migration, thus, contributing to MSC-mediated tissue repair. CD13 may present a viable target to enhance the efficacy of mesenchymal stem cell therapies.

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          Mesenchymal stem cells: biology, pathophysiology, translational findings, and therapeutic implications for cardiac disease.

          Adam Williams, Joshua Hare (2011)
          Mesenchymal stem cells (MSCs) are a prototypical adult stem cell with capacity for self-renewal and differentiation with a broad tissue distribution. Initially described in bone marrow, MSCs have the capacity to differentiate into mesoderm- and nonmesoderm-derived tissues. The endogenous role for MSCs is maintenance of stem cell niches (classically the hematopoietic), and as such, MSCs participate in organ homeostasis, wound healing, and successful aging. From a therapeutic perspective, and facilitated by the ease of preparation and immunologic privilege, MSCs are emerging as an extremely promising therapeutic agent for tissue regeneration. Studies in animal models of myocardial infarction have demonstrated the ability of transplanted MSCs to engraft and differentiate into cardiomyocytes and vasculature cells, recruit endogenous cardiac stem cells, and secrete a wide array of paracrine factors. Together, these properties can be harnessed to both prevent and reverse remodeling in the ischemically injured ventricle. In proof-of-concept and phase I clinical trials, MSC therapy improved left ventricular function, induced reverse remodeling, and decreased scar size. This article reviews the current understanding of MSC biology, mechanism of action in cardiac repair, translational findings, and early clinical trial data of MSC therapy for cardiac disease.
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            Adult stem cells from bone marrow (MSCs) isolated from different strains of inbred mice vary in surface epitopes, rates of proliferation, and differentiation potential.

            Alexandra Peister, Jason A. Mellad, Benjamin L Larson (2004)
            For reasons that are not apparent, it has been difficult to isolate and expand the adult stem cells referred to as mesenchymal stem cells or marrow stromal cells (MSCs) from murine bone marrow. We developed a protocol that provides rapidly expanding MSCs from 5 strains of inbred mice. The MSCs obtained from 5 different strains of mice were similar to human and rat MSCs in that they expanded more rapidly if plated at very low density, formed single-cell-derived colonies, and readily differentiated into either adipocytes, chondrocytes, or mineralizing cells. However, the cells from the 5 strains differed in their media requirements for optimal growth, rates of propagation, and presence of the surface epitopes CD34, stem cell antigen-1 (Sca-1), and vascular cell adhesion molecule 1 (VCAM-1). The protocol should make it possible to undertake a large number of experiments with MSCs in transgenic mice that have previously not been possible. The differences among MSCs from different strains may explain some of the conflicting data recently published on the engraftment of mouse MSCs or other bone marrow cells into nonhematopoietic tissues.
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              Aminopeptidase N is a receptor for tumor-homing peptides and a target for inhibiting angiogenesis.

              R Pasqualini, W Arap, R Ashmun (2000)
              Phage that display a surface peptide with the NGR sequence motif home selectively to tumor vasculature in vivo. A drug coupled to an NGR peptide has more potent antitumor effects than the free drug [W. Arap et al., Science (Washington DC), 279: 377-380, 1998]. We show here that the receptor for the NGR peptides in tumor vasculature is aminopeptidase N (APN; also called CD13). NGR phage specifically bound to immunocaptured APN and to cells engineered to express APN on their surface. Antibodies against APN inhibited in vivo tumor homing by the NGR phage. Immunohistochemical staining showed that APN expression is up-regulated in endothelial cells within mouse and human tumors. In another tissue that undergoes angiogenesis, corpus luteum, blood vessels also expressed APN, but APN was not detected in blood vessels of various other normal tissues stained under the same conditions. APN antagonists specifically inhibited angiogenesis in chorioallantoic membranes and in the retina and suppressed tumor growth. Thus, APN is involved in angiogenesis and can serve as a target for delivering drugs into tumors and for inhibiting angiogenesis.
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                Author and article information

                Journal
                Journal ID (nlm-ta): Front Physiol
                Journal ID (iso-abbrev): Front Physiol
                Journal ID (publisher-id): Front. Physiol.
                Title: Frontiers in Physiology
                Publisher: Frontiers Media S.A.
                ISSN (Electronic): 1664-042X
                Publication date (Electronic preprint): 02 December 2013
                Publication date (Electronic): 09 January 2014
                Publication date Collection: 2013
                Volume: 4
                Electronic Location Identifier: 402
                Affiliations
                [1] 1Center for Vascular Biology, University of Connecticut Health Center Farmington, CT, USA
                [2] 2Department of Anesthesiology, Texas Tech University Health Sciences Center Lubbock, TX, USA
                [3] 3Center on Aging, University of Connecticut Health Center Farmington, CT, USA
                [4] 4Drug Discovery, Genomics Institute of the Novartis Research Foundation San Diego, CA, USA
                Author notes

                Edited by: Lucas Guimarães-Ferreira, Federal University of Espirito Santo, Brazil

                Reviewed by: Brenda Schoffstall, Barry University, USA; Atsushi Asakura, University of Minnesota, USA

                *Correspondence: Morgan E. Carlson, Center on Aging, University of Connecticut Health Center, 263 Farmington Ave., Farmington, CT 06030, USA e-mail: mcarlson@ 123456gnf.org ;
                Linda H. Shapiro, Center for Vascular Biology, University of Connecticut Health Center, 263 Farmington Ave., Farmington, CT 06030, USA e-mail: lshapiro@ 123456neuron.uchc.edu

                This article was submitted to Striated Muscle Physiology, a section of the journal Frontiers in Physiology.

                Article
                DOI: 10.3389/fphys.2013.00402
                PMC ID: 3885827
                PubMed ID: 24409152
                SO-VID: b198ee38-24d2-49b7-98ef-8caf9c404bd4
                Copyright © Copyright © 2014 Rahman, Subramani, Ghosh, Denninger, Takeda, Fong, Carlson and Shapiro.
                License:

                This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

                History
                Date received : 31 October 2013
                Date accepted : 21 December 2013
                Page count
                Figures: 7, Tables: 0, Equations: 0, References: 40, Pages: 12, Words: 7595
                Categories
                Subject: Physiology
                Subject: Original Research Article

                ScienceOpen disciplines: Anatomy & Physiology
                Keywords: cd13,mesenchymal stem cells,adhesion,cell transplantation,hindlimb ischemia
                Data availability:
                ScienceOpen disciplines: Anatomy & Physiology
                Keywords: cd13, mesenchymal stem cells, adhesion, cell transplantation, hindlimb ischemia

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