Biodistribution of Neural Stem Cells After Intravascular Therapy for Hypoxic–Ischemia

Author:

Pendharkar Arjun V.1,Chua Josh Y.1,Andres Robert H.1,Wang Nancy1,Gaeta Xavier1,Wang Hui1,De Abhijit1,Choi Raymond1,Chen Shawn1,Rutt Brian K.1,Gambhir Sanjiv S.1,Guzman Raphael1

Affiliation:

1. From the Department of Neurosurgery (A.V.P., J.Y.C., R.H.A., N.W., X.G., R.C., R.G.), Stanford University School of Medicine, Stanford, Calif; the Molecular Imaging Program at Stanford (MIPS; H.W., A.D., S.C., B.K.R., S.S.G.), Stanford University School of Medicine, Stanford, Calif; and the Department of Radiology (S.C., B.K.R., S.S.G.), Stanford University School of Medicine, Stanford, Calif.

Abstract

Background and Purpose— Intravascular transplantation of neural stem cells represents a minimally invasive therapeutic approach for the treatment of central nervous system diseases. The cellular biodistribution after intravascular injection needs to be analyzed to determine the ideal delivery modality. We studied the biodistribution and efficiency of targeted central nervous system delivery comparing intravenous and intra-arterial (IA) administration of neural stem cells after brain ischemia. Methods— Mouse neural stem cells were transduced with a firefly luciferase reporter gene for bioluminescence imaging (BLI). Hypoxic–ischemia was induced in adult mice and reporter neural stem cells were transplanted IA or intravenous at 24 hours after brain ischemia. In vivo BLI was used to track transplanted cells up to 2 weeks after transplantation and ex vivo BLI was used to determine single organ biodistribution. Results— Immediately after transplantation, BLI signal from the brain was 12 times higher in IA versus intravenous injected animals ( P <0.0001). After IA injection, 69% of the total luciferase activity arose from the brain early after transplantation and 93% at 1 week. After intravenous injection, 94% of the BLI signal was detected in the lungs ( P =0.004) followed by an overall 94% signal loss at 1 week, indicating lack of cell survival outside the brain. Ex vivo single organ analysis showed a significantly higher BLI signal in the brain than in the lungs, liver, and kidneys at 1 week ( P <0.0001) and 2 weeks in IA ( P =0.007). Conclusion— IA transplantation results in superior delivery and sustained presence of neural stem cells in the ischemic brain in comparison to intravenous infusion.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Advanced and Specialised Nursing,Cardiology and Cardiovascular Medicine,Clinical Neurology

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