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Open AccessJournal ArticleDOI

Modality-specific axonal regeneration: toward selective regenerative neural interfaces.

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TLDR
This study demonstrates the guided enrichment of sensory axons in specific regenerative chambers, and supports the notion that neurotrophic factors can be used to segregate sensory and perhaps motor axons from transected peripheral nerves into separate compartments.
Abstract
Regenerative peripheral nerve interfaces have been proposed as viable alternatives for the natural control of robotic prosthetic devices. However, sensory and motor axons at the neural interface are of mixed submodality types, which difficult the specific recording from motor axons and the eliciting of precise sensory modalities through selective stimulation. Here we evaluated the possibility of using type-specific neurotrophins to preferentially entice the regeneration of defined axonal populations from transected peripheral nerves into separate compartments. Segregation of mixed sensory fibers from dorsal root ganglion neurons was evaluated in vitro by compartmentalized diffusion delivery of nerve growth factor (NGF) and neurotrophin-3 (NT-3), to preferentially entice the growth of TrkA+ nociceptive and TrkC+ proprioceptive subsets of sensory neurons, respectively. The average axon length in the NGF channel increased 2.5 fold compared to that in saline or NT-3, whereas the number of branches increased 3 fold in the NT-3 channels. These results were confirmed using a 3-D “Y”-shaped in vitro assay showing that the arm containing NGF was able to entice a 5-fold increase in axonal length of unbranched fibers. To address if such segregation can be enticed in vivo, a “Y”-shaped tubing was used to allow regeneration of the transected adult rat sciatic nerve into separate compartments filled with either NFG or NT-3. A significant increase in the number of CGRP+ pain fibers were attracted towards the sural nerve, while N-52+ large diameter axons were observed in the tibial and NT-3 compartments. This study demonstrates the guided enrichment of sensory axons in specific regenerative chambers, and supports the notion that neurotrophic factors can be used to segregate sensory and perhaps motor axons in separate peripheral interfaces.

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Journal ArticleDOI

Specificity of peripheral nerve regeneration: interactions at the axon level.

TL;DR: The aim of this review is to understand if some of these molecular factors implicated in axonal regeneration and pathfinding after injury are specific for motor and sensory neuron growth, and provide the basic knowledge for potential strategies to enhance and guide axonal regenerate and reinnervation of adequate target organs.
Journal ArticleDOI

Biomimetic approaches to bionic touch through a peripheral nerve interface.

TL;DR: This work describes devices that can be chronically implanted in the nerve to electrically activate nerve fibers and offers a blueprint for how these codes could be implemented in a neuroprosthetic device to deliver rich, natural, and versatile tactile sensations.
Journal ArticleDOI

Interfacing the somatosensory system to restore touch and proprioception: essential considerations.

TL;DR: The purpose of this review is to outline practical considerations for the design of a somatosensory interface based on present knowledge of the anatomy and physiology, prior attempts to elicit somatic sensations using electrical stimulation, and lessons learned from successful sensory neuroprostheses such as the cochlear implant.
Journal ArticleDOI

Foreign Body Reaction to Implanted Biomaterials and Its Impact in Nerve Neuroprosthetics.

TL;DR: In this paper, the authors provide an overview of the material-cell interactions leading to the development of FBR and discuss how material properties (such as stiffness and size), pharmacological therapies, or use of biodegradable materials may be exploited to minimize FBR to nerve neuroprosthetic implants and improve their long-term stability.
Book ChapterDOI

Interfaces with the peripheral nerve for the control of neuroprostheses.

TL;DR: This chapter provides a general overview of nerve electrodes as well as the state-of-the-art of their biomedical applications in neuroprosthetic systems.
References
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Journal ArticleDOI

Neuronal ensemble control of prosthetic devices by a human with tetraplegia

TL;DR: Initial results for a tetraplegic human using a pilot NMP suggest that NMPs based upon intracortical neuronal ensemble spiking activity could provide a valuable new neurotechnology to restore independence for humans with paralysis.
Journal ArticleDOI

Cortical control of a prosthetic arm for self-feeding

TL;DR: A system that permits embodied prosthetic control is described and monkeys (Macaca mulatta) use their motor cortical activity to control a mechanized arm replica in a self-feeding task, and this demonstration of multi-degree-of-freedom embodied prosthetics control paves the way towards the development of dexterous prosthetic devices that could ultimately achieve arm and hand function at a near-natural level.
Journal ArticleDOI

Neuronal cell loss accompanies the brain tissue response to chronically implanted silicon microelectrode arrays

TL;DR: Persistent ED1 up-regulation and neuronal loss was not observed in microelectrode stab controls indicating that the phenotype did not result from the initial mechanical trauma of electrode implantation, but was associated with the foreign body response.

Conduction velocityisrelated to morphological cell typeinrat dorsal root ganglion neurones

A. Harper, +1 more
TL;DR: Combining intracellular recording and dye‐injection techniques permitted direct correlation of neuronal soma size with peripheral nerve conduction velocity in individual neurones of the L4 dorsal root ganglion of the anaesthetized 5‐8‐week‐old rat.
Journal ArticleDOI

Conduction velocity is related to morphological cell type in rat dorsal root ganglion neurones.

TL;DR: In this article, an intracellular recording and dye-injection technique was used to study the relationship between neuronal cell size and axonal conduction velocity in the L4 dorsal root ganglion.
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