Chronic traumatic encephalopathy-integration of canonical traumatic brain injury secondary injury mechanisms with tau pathology

Kulbe, Jacqueline R.; Hall, Edward D.

doi:10.1016/j.pneurobio.2017.08.003

Cited by 49 publications

(34 citation statements)

References 363 publications

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“…Considering all the studies presented above, there is a strong basis to assume that the administration of GM1 ganglioside can inhibit the AOI mechanism following traumatic brain injury, thereby serving as a neuroprotective agent in various brain injuries. Since in the past decade or even earlier, TBI has been established as a major cause to CTE (chronic traumatic encephalopathy) 44 – 46 new and novel potential treatments are needed to address this destructive process. Although GM1 have previously been used as a potential treatment for neurodegenerative diseases like PD and HD 40 , 47 , it is important to emphasize that in contrast to these reports where a high dose of GM1 or a longer range of treatment was needed to obtain desired results, this low-single dose was sufficient to prevent cognitive and biochemical damage.…”

Section: Discussionmentioning

confidence: 99%

GM1 ganglioside prevents axonal regeneration inhibition and cognitive deficits in a mouse model of traumatic brain injury

Benady

Freidin

Pick

et al. 2018

Sci Rep

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Traumatic Brain Injury (TBI) is one of the most common causes of neurological damage in young populations. It has been previously suggested that one of the mechanisms that underlie brain injury is Axonal Outgrowth Inhibition (AOI) that is caused by altered composition of the gangliosides on the axon surface. In the present study, we have found a significant reduction of GM1 ganglioside levels in the cortex in a closed head traumatic brain injury model of a mouse, induced by a weight drop device. In addition, axonal regeneration in the brains of the injured mice was affected as seen by the expression of the axonal marker pNF-H and the growth cones (visualized by F-actin and β-III-tubulin). NeuN immunostaining revealed mTBI-induced damage to neuronal survival. Finally, as expected, spatial and visual memories (measured by the Y-maze and the Novel Object Recognition tests, respectively) were also damaged 7 and 30 days post injury. A single low dose of GM1 shortly after the injury (2 mg/kg; IP) prevented all of the deficits mentioned above. These results reveal additional insights into the neuroprotective characteristics of GM1 in prevention of biochemical, cellular and cognitive changes caused by trauma, and may suggest a potential intervention for mTBI.

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Section: Discussionmentioning

confidence: 99%

GM1 ganglioside prevents axonal regeneration inhibition and cognitive deficits in a mouse model of traumatic brain injury

Benady

Freidin

Pick

et al. 2018

Sci Rep

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“…Excessive p-tau is a major contributor to CTE. 36 This has been seen in sports such as boxing and football. 37 p-GSK-3b is the primary kinase that phosphorylates tau, and p-tau is known to increase following a TBI.…”

Section: Blocking Gsk-3b Prevents Memory Deficits Post-tbi 1873mentioning

confidence: 99%

Inhibition of Glycogen Synthase Kinase 3β as a Treatment for the Prevention of Cognitive Deficits after a Traumatic Brain Injury

Farr

Niehoff

Kumar

et al. 2019

Journal of Neurotrauma

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Traumatic brain injury (TBI) has many long-term consequences, including impairment in memory and changes in mood. Glycogen synthase kinase 3b (GSK-3b) in its phosphorylated form (p-GSK-3b) is considered to be a major contributor to memory problems that occur post-TBI. We have developed an antisense that targets the GSK-3b (G AO) gene. Using a model of closed-head concussive TBI, we subjected mice to TBI and injected G AO or a random antisense (R AO) 15 min post-injury. One week post-injury, mice were tested in object recognition with 24 h delay. At 4 weeks post-injury, mice were tested with a T-maze foot shock avoidance memory test and a second object recognition test with 24 h delay using different objects. Mice that received G AO show improved memory in both object recognition and T-maze compared with R AO-treated mice that were subjected to TBI. Next, we verified that G AO blocked the surge in phosphorylated GSK-3b post-TBI. Mice were subjected to TBI and injected with antisense 15 min post-TBI with G AO or R AO. Mice were euthanized at 4 and 72 h post-TBI. Analysis of p-ser9GSK-3b, p-tyr216GSK-3b, and phospho-tau (p-tau) 404 showed that mice that received a TBI+ R AO had significantly higher p-ser9GSK-3b, p-tyr216GSK-3b, and p-tau 404 levels than the mice that received TBI+ G AO and the Sham+ R AO mice. The current finding suggests that inhibiting GSK-3b increase after TBI with an antisense directed at GSK-3b prevents learning and memory impairments.

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“…In 2016, the first NINDS/NIBIB consensus meeting defined the neuropathological criteria of CTE and confirmed that the pathognomonic lesions in CTE are accumulations of abnormally hyperphosphorylated tau (p-tau) in astrocytes and neurons located around small blood vessels and at the depths of the cortical sulci (10). CTE, a new neurodegenerative tauopathy, was reported in athletes who played soccer, baseball, ice hockey, and rugby, as well as in military personnel exposed to explosive blasts (5)(6)(7)11). Clinical presentation of CTE was divided into three phases: behavioral/psychiatric, cognitive, and motor (12,13).…”

Section: Introductionmentioning

confidence: 99%

“…Traumatic brain injury (TBI) was long recognized as a risk factor for dementia (1)(2)(3)(4)(5). Chronic traumatic encephalopathy (CTE) refers to the neuropathological changes resulting from repeated episodes of TBI (3,(5)(6)(7). In the early twentieth century, the terms "punch-drunk" or "dementia pugilistica" were used to describe the clinical features of a distinct neuropsychiatric syndrome that affected boxers.…”

Section: Introductionmentioning

confidence: 99%

A Clinicopathological Report of a 93-Year-Old Former Street Boxer With Coexistence of Chronic Traumatic Encephalopathy, Alzheimer's Disease, Dementia With Lewy Bodies, and Hippocampal Sclerosis With TDP-43 Pathology

et al. 2020

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Chronic traumatic encephalopathy (CTE) was recently recognized as a new tauopathy in which multifocal perivascular phosphorylated tau aggregates accumulate in neurons, astrocytes, and neurites at the depths of the cortical sulci. Traumatic brain injury (TBI) in early or mid-life is known to be associated with an increased risk of dementia in late life. This case report describes a 93-year-old former street boxer with a premortem diagnosis of severe dementia, who showed pathological evidence of the coexistence of Alzheimer's disease, CTE, dementia with Lewy bodies, and hippocampal sclerosis with TDP-43 pathology. These findings suggest that TBI may trigger a variety of misfolded proteins leading to dementia. Currently, clear clinical diagnostic criteria for CTE have not been established. Therefore, clinicians should be aware that TBI is a risk factor for dementia and that CTE can overlap with other neurodegenerative diseases.

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Chronic traumatic encephalopathy-integration of canonical traumatic brain injury secondary injury mechanisms with tau pathology

Cited by 49 publications

References 363 publications

GM1 ganglioside prevents axonal regeneration inhibition and cognitive deficits in a mouse model of traumatic brain injury

GM1 ganglioside prevents axonal regeneration inhibition and cognitive deficits in a mouse model of traumatic brain injury

Inhibition of Glycogen Synthase Kinase 3β as a Treatment for the Prevention of Cognitive Deficits after a Traumatic Brain Injury

A Clinicopathological Report of a 93-Year-Old Former Street Boxer With Coexistence of Chronic Traumatic Encephalopathy, Alzheimer's Disease, Dementia With Lewy Bodies, and Hippocampal Sclerosis With TDP-43 Pathology

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