Clarity reveals a more protracted temporal course of axon swelling and disconnection than previously described following traumatic brain injury

Weber, Maura T.; Arena, John D.; Xiao, Rui; Wolf, John A.; Johnson, Victoria E.

doi:10.1111/bpa.12677

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Clarity reveals a more protracted temporal course of axon swelling and disconnection than previously described following traumatic brain injury
Citation	Weber MT, Arena JD, Xiao R, Wolf JA, Johnson VE. Brain Pathol. 2019; 29(3): 437-450.
Affiliation	Department of Neurosurgery, Penn Center for Brain Injury and Repair, Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA, 19104, USA.
Copyright	(Copyright © 2019, John Wiley and Sons)
DOI	10.1111/bpa.12677
PMID	30444552
Abstract	Diffuse axonal injury (DAI) is an important consequence of traumatic brain injury (TBI). At the moment of trauma, axons rarely disconnect, but undergo cytoskeletal disruption and transport interruption leading to protein accumulation within swellings. The amyloid precursor protein (APP) accumulates rapidly and the standard histological evaluation of axonal pathology relies upon its detection. APP+ swellings first appear as varicosities along intact axons, which can ultimately undergo secondary disconnection to leave a terminal "axon bulb" at the disconnected, proximal end. However, sites of disconnection are difficult to determine with certainty using standard, thin tissue-sections, thus limiting the comprehensive evaluation of axon degeneration. The tissue-clearing technology, CLARITY, permits three-dimensional visualization of axons that would otherwise be out of plane in standard tissue sections. Here, we examined the morphology and connection status of APP+ swellings using CLARITY at 6h, 24h, 1-week and 1-month following the controlled cortical impact (CCI) model of TBI in mice. Remarkably, many APP+ swellings that appeared as terminal bulbs when viewed in standard 8μm-thick regions of tissue, were instead revealed to be varicose swellings along intact axons when three-dimensions were fully-visible. Moreover, the percentage of these potentially-viable axon swellings differed with survival from injury and may represent the delayed-onset of distinct mechanisms of degeneration. Even at 1-month post-CCI, ~10% of apparently terminal bulbs were revealed as connected by CLARITY and are thus potentially salvageable. Intriguingly, the diameter of swellings decreased with survival, including varicosities along intact axons, and may reflect reversal of, or reduced, axonal transport interruption in the chronic setting. These data indicate that APP immunohistochemistry on standard-thickness tissue sections overestimates axon disconnection, particularly acutely post-injury. Evaluating cleared tissue demonstrates a surprisingly delayed process of axon disconnection and thus longer window of therapeutic opportunity than previously appreciated. Intriguingly, a subset of axon swellings may also be capable of recovery. This article is protected by copyright. All rights reserved. This article is protected by copyright. All rights reserved. Language: en