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      Imaging Neural Stem Cell Graft-Induced Structural Repair in Stroke

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          Abstract

          Stem cell therapy ameliorates motor deficits in experimental stroke model. Multimodal molecular imaging enables real-time longitudinal monitoring of infarct location, size, and transplant survival. In the present study, we used magnetic resonance imaging (MRI) and positron emission tomography (PET) to track the infarct evolution, tissue repair, and the fate of grafted cells. We genetically engineered embryonic stem cell-derived neural stem cells (NSCs) with a triple fusion reporter gene to express monomeric red fluorescence protein and herpes simplex virus-truncated thymidine kinase for multimodal molecular imaging and SPIO labeled for MRI. The infarct size as well as fate and function of grafted cells were tracked in real time for 3 months using MRI and PET. We report that grafted NSCs reduced the infarct size in animals with less than 0.1 cm 3 initial infarct in a dose-dependent manner, while larger stroke was not amenable to such beneficial effects. PET imaging revealed increased metabolic activity in grafted animals and visualized functioning grafted cells in vivo. Immunohistopathological analysis demonstrated that, after a 3-month survival period, grafted NSCs dispersed in the stroke-lesioned parenchyma and differentiated into neurons, astrocytes, and oligodendrocytes. Longitudinal multimodal imaging provides insights into time course dose-dependent interactions between NSC grafts and structural changes in infarcted tissue.

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          Author and article information

          Journal
          9208854
          8477
          Cell Transplant
          Cell Transplant
          Cell transplantation
          0963-6897
          1555-3892
          16 February 2018
          2013
          22 February 2018
          : 22
          : 5
          : 881-892
          Affiliations
          [* ]Department of Neurosurgery, Stanford Stroke Center and Stanford Institute for Neuro-Innovation and Translational Neurosciences, Stanford, CA, USA
          []Molecular Medicine Research Institute, Sunnyvale, CA, USA
          []Department of Medicine and Radiology (Molecular Imaging Program at Stanford), Stanford University School of Medicine, Stanford, CA, USA
          Author notes
          Address correspondence to Marcel Daadi, Ph.D., Department of Neurosurgery, Stanford University, MSLS P304, 1201 Welch Rd., Stanford, CA 94305-5487, USA. Tel: +1-650-724-9998; Fax: +1-650-498-4134; mdaadi@ 123456stanford.edu
          Article
          PMC5823270 PMC5823270 5823270 nihpa942826
          10.3727/096368912X656144
          5823270
          23044338
          9b89de9d-ab2e-44cb-84fc-f9b4d144728f
          History
          Categories
          Article

          Magnetic resonance imaging (MRI),Human neural stem cells (NSCs),Molecular imaging,Position emission tomography (PET),Cell therapy

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