Statins in Traumatic Brain Injury

Wible, Elissa Fory; Laskowitz, Daniel T.

doi:10.1016/j.nurt.2009.11.003

Cited by 76 publications

(47 citation statements)

References 97 publications

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“…17 Lastly, statins counteract the procoagulant cascade promoted by infl ammation through the following mechanisms: blunting monocytic expression of tissue factor, increasing thrombomodulin availability (important in the activation of protein C), and reducing levels of plasminogen activator inhibitor-1, which impairs the fi brinolytic system. 15 Though no studies to date have evaluated the effect of statins on delirium in patients in the ICU, this drug class has been examined in models of traumatic brain injury (TBI), 18 which involves pathophysiologic changes (eg, neuronal damage and apoptosis, neuroinfl ammation, and BBB injury) similar to those observed in other types of critical illness, including sepsis and acute respiratory distress syndrome. The benefi ts of statins observed in animal studies of TBI include increased hippocampal neuron survival and improved neurologic function.…”

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confidence: 99%

“…The benefi ts of statins observed in animal studies of TBI include increased hippocampal neuron survival and improved neurologic function. [18][19][20][21][22] In humans, one clinical trial reported a reduction in amnesia and increased orientation in patients with TBI who were treated with rosuvastatin. 23 Studies investigating the effect of statins on patients with postoperative delirium, a population with different clinical profi les than patients in the ICU, have yielded inconsistent results.…”

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Statins and Brain Dysfunction

Morandi

Hughes

Girard

et al. 2011

Chest

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Delirium is a manifestation of acute brain dysfunction that occurs in up to 80% of patients who are critically ill and is associated with higher mortality and long-term cognitive impairment (LTCI), which is akin to a dementia-like cognitive disability. [1][2][3][4][5][6][7] This acquired cognitive impairment-critical illness brain injury-has important public health implications for both younger and older patients (the latter an increasingly larger proportion of the population), threatening the functional independence and quality of life of millions of ICU survivors in the coming decades. Given that delirium in the ICU represents early brain dysfunction during critical illness and can be easily assessed using validated bedside instruments, 1,8 novel therapies that prevent or treat delirium may prevent its associated immediate and long-term sequelae.Findings from animal and human studies suggest a neuroinfl ammatory pathogenesis of delirium and longterm brain dysfunction associated with critical illness. We propose a testable hypothesis, based on existing data, that the pleiotropic effects of statin medications can mitigate the mechanisms of delirium and LTCI associated with critical illness. Specifi cally, that statins may modify two processes leading to brain injury: neuroinfl ammation and activation of proinfl ammatory microglia. Effects on Neuroinflammation During Critical IllnessAn intense systemic infl ammatory response to illness or injury is a key mediator of organ dysfunction during critical illness. Several conditions that often lead to an ICU admission are examples of the deleterious effects of systemic infl ammation (eg, severe sepsis, trauma, acute respiratory distress syndrome). Proinfl ammatory cytokines (eg, tumor necrosis factor [TNF]-a and IL-1 b ) and chemokines (eg, monocytic chemoattractant protein [MCP]-1) activate leukocytes and endothelial cells (which express leukocyteDelirium is a frequent form of acute brain dysfunction in patients who are critically ill and is associated with poor clinical outcomes, including a critical illness brain injury that may last for months to years. Despite widespread recognition of signifi cant adverse outcomes, pharmacologic approaches to prevent or treat delirium during critical illness remain unproven. We hypothesize that commonly prescribed statin medications may prevent and treat delirium by targeting molecular pathways of infl ammation (peripheral and central) and microglial activation that are central to the pathogenesis of delirium. Systemic infl ammation, a principal mechanism of injury, for example, in sepsis, acute respiratory distress syndrome, and other critical illnesses, can cause neuronal apoptosis, blood-brain barrier injury, brain ischemia, and microglial activation. We hypothesize that the known pleiotropic effects of statins, which attenuate such neuroinfl ammation, may redirect microglial activation and promote an antiinfl ammatory phenotype, thereby offering the potential to reduce the public health burden of delirium and its associated l...

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Statins and Brain Dysfunction

Morandi

Hughes

Girard

et al. 2011

Chest

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“…Total 44 100 P E R S P E C T I V E (27), and brain injury (28,29). A search of the literature reveals no systematic neuroPK studies in any mouse strain that would enable direct comparisons of CNS exposure across the various statins.…”

Section: Databases and Repurposingmentioning

confidence: 99%

Data gaps limit the translational potential of preclinical research

Kleiman

Ehlers

2016

Sci. Transl. Med.

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“…Statin therapy has also been investigated in patients with ALI; it was shown to be safe and associated with a significant decrease in bronchoalveolar lavage interleukin-8, but had no other effects compared to placebo [101]. Although preclinical studies have shown benefits from statins in models of TBI and related disease processes, including cerebral ischemia, ICH, and subarachnoid hemorrhage, clinical studies have been shortcoming [102]. The use of statins in patients with aneurysmal subarachnoid hemorrhage has been investigated in several small clinical trials.…”

Section: Statinsmentioning

confidence: 99%

Antioxidant Strategies in Neurocritical Care

Hanafy

Selim

2012

Neurotherapeutics

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An increase in oxidative stress and overproduction of oxidizing reactive species plays an important role in the pathophysiology of several conditions encountered in the neurocritical care setting including: ischemic and hemorrhagic strokes, traumatic brain injury, acute respiratory distress syndrome, sepsis, and organ failure. The presence of oxidative stress in these conditions is supported by a large body of preclinical and clinical studies, and provides a rationale to support a potential therapeutic role for antioxidants. The purpose of this article is to briefly review the basic mechanisms and molecular biology of oxidative stress, summarize its role in critically ill neurological patients, and review available data regarding the potential role of antioxidant strategies in neurocritical care and future directions.

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Statins in Traumatic Brain Injury

Cited by 76 publications

References 97 publications

Statins and Brain Dysfunction

Statins and Brain Dysfunction

Data gaps limit the translational potential of preclinical research

Antioxidant Strategies in Neurocritical Care

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