characteristics of the early immune response following transplantation of mouse es cell derived insulin-producing cell clusters特征的早期免疫反应移植后小鼠es细胞衍生胰岛素生产细胞集群.pdfVIP

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characteristics of the early immune response following transplantation of mouse es cell derived insulin-producing cell clusters特征的早期免疫反应移植后小鼠es细胞衍生胰岛素生产细胞集群.pdf

characteristics of the early immune response following transplantation of mouse es cell derived insulin-producing cell clusters特征的早期免疫反应移植后小鼠es细胞衍生胰岛素生产细胞集群

Characteristics of the Early Immune Response Following Transplantation of Mouse ES Cell Derived Insulin- Producing Cell Clusters 1,2 1 Ashleigh S. Boyd *, Kathryn J. Wood * 1Transplantation Research Immunology Group, Nuffield Department of Surgery, John Radcliffe Hospital, University of Oxford, Oxford, United Kingdom, 2 NIH Center of Biomedical Research Excellence (COBRE) in Tissue Repair and Stem Cell Biology, Roger Williams Hospital, Boston University School of Medicine, Providence, Rhode Island, United States of America Abstract Background: The fully differentiated progeny of ES cells (ESC) may eventually be used for cell replacement therapy (CRT). However, elements of the innate immune system may contribute to damage or destruction of these tissues when transplanted. Methodology/Principal Findings: Herein, we assessed the hitherto ill-defined contribution of the early innate immune response in CRT after transplantation of either ESC derived insulin producing cell clusters (IPCCs) or adult pancreatic islets. Ingress of neutrophil or macrophage cells was noted immediately at the site of IPCC transplantation, but this infiltration was attenuated by day three. Gene profiling identified specific inflammatory cytokines and chemokines that were either absent or sharply reduced by three days after IPCC transplantation. Thus, IPCC transplantation provoked less of an early immune response than pancreatic islet transplantation. Conclusions/Significance: Our study offers insights into the characteristics of the immune response of an ESC derived tissue in the incipient stages following transplantation and suggests potential strategies to inhibit cell damage to ensure their long-term perpetuation and functionality in CRT. Citation: Boyd AS, Wood KJ (

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