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Open AccessJournal ArticleDOI

Transsynaptic tracing and its emerging use to assess graft-reconstructed neural circuits

Andrew F. Adler, +2 more
- 01 Jun 2020 - 
- Vol. 38, Iss: 6, pp 716-726
TLDR
Evidence is reviewed suggesting that the new contacts established between host and graft neurons may indeed be cell‐type specific, and how transsynaptic tracing can be used in the future to further elucidate the mechanisms of graft‐mediated functional recovery in spinal cord injury and Parkinson's disease.
Abstract
Fetal neural progenitor grafts have been evaluated in preclinical animal models of spinal cord injury and Parkinson's disease for decades, but the initial reliance on primary tissue as a cell source limited the scale of their clinical translatability. With the development of robust methods to differentiate human pluripotent stem cells to specific neural subtypes, cell replacement therapy holds renewed promise to treat a variety of neurodegenerative diseases and injuries at scale. As these cell sources are evaluated in preclinical models, new transsynaptic tracing methods are making it possible to study the connectivity between host and graft neurons with greater speed and detail than was previously possible. To date, these studies have revealed that widespread, long-lasting, and anatomically appropriate synaptic contacts are established between host and graft neurons, as well as new aspects of host-graft connectivity which may be relevant to clinical cell replacement therapy. It is not yet clear, however, whether the synaptic connectivity between graft and host neurons is as cell-type specific as it is in the endogenous nervous system, or whether that connectivity is responsible for the functional efficacy of cell replacement therapy. Here, we review evidence suggesting that the new contacts established between host and graft neurons may indeed be cell-type specific, and how transsynaptic tracing can be used in the future to further elucidate the mechanisms of graft-mediated functional recovery in spinal cord injury and Parkinson's disease.

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Citations
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Supporting data for 3D Printed Stem-Cell Derived Neural Progenitors Generate Spinal Cord Scaffolds

TL;DR: Successful bioprinting of OPCs in combination with sNPCs demonstrates a multicellular neural tissue engineering approach, where the ability to direct the patterning and combination of transplanted neuronal and glial cells can be beneficial in rebuilding functional axonal connections across areas of central nervous system tissue damage.
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Transplanting neural progenitor cells to restore connectivity after spinal cord injury.

TL;DR: The use of neural progenitor cell transplants to restore connectivity in key neural systems following spinal damage is described and focused here on the use of neurons obtained or derived from different sources to promote connectivity in sensory, motor and autonomic systems.
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Retinal Ganglion Cell Transplantation: Approaches for Overcoming Challenges to Functional Integration

TL;DR: The current state of experimental RGC transplantation is summarized in this paper, and a set of standard approaches to quantifying and reporting experimental outcomes is proposed to guide a collective effort toward functional RGC replacement and optic nerve regeneration.
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Dopamine Cell Therapy: From Cell Replacement to Circuitry Repair.

TL;DR: In this article, homotopic transplantation of mDA neurons into the substantia nigra was investigated in rodent PD models as a way to achieve more complete circuitry repair, and the afferent connectivity of grafts implanted in the nigra matched closely that of the intrinsic mDA system.
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Transneuronal tracing to map connectivity in injured and transplanted spinal networks

TL;DR: A review of advances in neuronal tracing using pseudorabies virus (PRV) and its use in the intact, injured, and transplanted spinal cord can be found in this article .
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