<scp>IL</scp>‐1β associations with posttraumatic epilepsy development: A genetics and biomarker cohort study

Diamond, Matthew L.; Ritter, Anne C.; Failla, Michelle D.; Boles, Jennifer A.; Conley, Yvette P.; Kochanek, Patrick M.; Wagner, Amy K.

doi:10.1111/epi.12628

Cited by 129 publications

(77 citation statements)

References 53 publications

(47 reference statements)

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“…Many studies have shown that genetic variation is associated with outcomes and conditions following TBI (Hoh et al, 2010;Weaver et al, 2012;Wagner et al, 2012;Garringer et al, 2013;Diamond et al, 2014;Failla et al, 2014). Of note, an IL-6 polymorphism (À174 G/C) has been reported as associated with mortality after severe TBI (Dalla Libera et al, 2011) and the development of Alzheimer's disease in non-TBI populations (Qi et al, 2012).…”

Section: Discussionmentioning

confidence: 99%

Acute CSF interleukin-6 trajectories after TBI: Associations with neuroinflammation, polytrauma, and outcome

Kumar

Diamond

Boles

et al. 2015

Brain, Behavior, and Immunity

126

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Section: Discussionmentioning

confidence: 99%

Acute CSF interleukin-6 trajectories after TBI: Associations with neuroinflammation, polytrauma, and outcome

Kumar

Diamond

Boles

et al. 2015

Brain, Behavior, and Immunity

126

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“…Moreover, compared to the existent traumatic brain injury model [54, 55], parenchymal brain calcified cysticerci have the advantage of being much more homogeneous and predictable in their structure and evolution than are traumatic brain lesions. Knowledge provided from these suggested cohort studies might also allow the development of novel interventions to prevent chronic epilepsy in NCC and perhaps in other forms of acquired epilepsy.…”

Section: Future Directions For Researchmentioning

confidence: 99%

Update on Cysticercosis Epileptogenesis: the Role of the Hippocampus

Brutto

Engel

Eliashiv

et al. 2015

Curr Neurol Neurosci Rep

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Neurocysticercosis (NCC) is the most common helminthic infection of the nervous system and a frequent cause of reactive seizures and epilepsy worldwide. In many cases, multiple episodes of focal seizures related to an identifiable parenchymal brain cyst (and likely attributable to local damage) continue for years after the cyst resolves. However, cases where seizure semiology, interictal EEG abnormalities, and parasites location do not correlate raise concerns about the causal relationship between NCC and either reactive seizures or epilepsy, as well as the epileptogenic potential of parasites. Neurosurgical series of patients with intractable epilepsy and cross-sectional population-based studies have shown a robust association between NCC and hippocampal sclerosis (HS), which might contribute to the above-referred inconsistencies. Current information does not allow to define whether in patients with NCC, HS could result from recurrent seizure activity from a local or distant focus or from chronic recurrent inflammation. In either case, HS may become the pathological substrate of subsequent mesial temporal lobe epilepsy (MTLE). Longitudinal clinical- and population-based cohort studies are needed to evaluate the causal relationship between NCC and HS and to characterize this association with the occurrence of MTLE. If a cause-and-effect relationship between NCC and HS is demonstrated, NCC patients could be assessed to examine neuronal mechanisms of hippocampal epileptogenesis in comparison with animal models, to identify biomarkers of hippocampal epileptogenesis, and to develop novel interventions to prevent epilepsy in NCC and perhaps in other forms of acquired epilepsy.

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“…Studies have characterized certain candidate cytokines, chemokines, cell-surface markers, and microglia as elevated early after injury compared to uninjured controls (Woodcock and Morganti-Kossmann, 2013). Contemporary concepts contend that controlled inflammation is necessary to clear debris and damaged cells early following TBI, while sustained elevations of inflammatory markers, such as IL-1β, TNFα, and IL-6, are deleterious if not physiologically regulated and can lead to an increased risk of depression (Juengst et al , 2014), epilepsy (Diamond et al , 2014), cognitive deficits (Clausen et al , 2009, 2011) and poor global outcomes (Kumar et al , 2014). …”

Section: Introductionmentioning

confidence: 99%

Principal components derived from CSF inflammatory profiles predict outcome in survivors after severe traumatic brain injury

Kumar

Rubin

Berger

et al. 2016

Brain, Behavior, and Immunity

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Studies have characterized absolute levels of multiple inflammatory agents as significant risk factors for poor outcomes after traumatic brain injury (TBI). However, inflammatory marker concentrations are highly inter-related, and production of one may result in the production or regulation of another. Therefore, a more comprehensive characterization of the inflammatory response post-TBI should consider relative levels of markers in the inflammatory pathway. We used principal component analysis (PCA) as a dimension-reduction technique to characterize the sets of markers that contribute independently to variability in cerebrospinal (CSF) inflammatory profiles after TBI. Using PCA results, we defined groups (or clusters) of individuals (n=111) with similar patterns of acute CSF inflammation that were then evaluated in the context of outcome and other relevant CSF and serum biomarkers collected days 0-3 and 4-5 post-injury. We identified four significant principal components (PC1-PC4) for CSF inflammation from days 0-3, and PC1 accounted for the greatest (31%) percentage of variance. PC1 was characterized by relatively higher CSF sICAM-1, sFAS, IL-10, IL-6, sVCAM-1, IL-5, and IL-8 levels. Cluster analysis then defined two distinct clusters, such that individuals in cluster 1 had highly positive PC1 scores and relatively higher levels of CSF cortisol, progesterone, estradiol, testosterone, brain derived neurotrophic factor (BDNF), and S100b; this group also had higher serum cortisol and lower serum BDNF. Multinomial logistic regression analyses showed that individuals in cluster 1 had a 10.9 times increased likelihood of GOS scores of 2/3 versus 4/5 at 6 months compared to cluster 2, after controlling for covariates. Cluster group did not discriminate between mortality compared to GOS scores of 4/5 after controlling for age and other covariates. Cluster groupings also did not discriminate mortality or 12 month outcomes in multivariate models. PCA and cluster analysis establish that a subset of CSF inflammatory markers measured in days 0-3 post-TBI may distinguish individuals with poor 6-month outcome, and future studies should prospectively validate these findings. PCA of inflammatory mediators after TBI could aid in prognostication and in identifying patient subgroups for therapeutic interventions.

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IL‐1β associations with posttraumatic epilepsy development: A genetics and biomarker cohort study

Cited by 129 publications

References 53 publications

Acute CSF interleukin-6 trajectories after TBI: Associations with neuroinflammation, polytrauma, and outcome

Acute CSF interleukin-6 trajectories after TBI: Associations with neuroinflammation, polytrauma, and outcome

Update on Cysticercosis Epileptogenesis: the Role of the Hippocampus

Principal components derived from CSF inflammatory profiles predict outcome in survivors after severe traumatic brain injury

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