Human Traumatic Brain Injury Alters Circulating L-Arginine and Its Metabolite Levels: Possible Link to Cerebral Blood Flow, Extracellular Matrix Remodeling, and Energy Status

Jeter, Cameron B.; Hergenroeder, Georgene W.; Ward, Norman H.; Moore, Anthony N.; Dash, Pramod K.

doi:10.1089/neu.2011.2029

Cited by 38 publications

(38 citation statements)

References 38 publications

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“…It is possible that ischemic brain injury per se can impair again the small bowel function and structure. Indeed, Jeter et al (30) identified that patients with severe traumatic brain injury had lower plasma citrulline concentrations than patients with mild traumatic brain injury and controls, even in the absence of shock. In addition, Hernández et al (31) found that acute brain injury was associated with increased gut permeability compared with controls.…”

Section: Discussionmentioning

confidence: 99%

“…In our opinion, enterocyte biomarkers could be integrative markers of global ischemia, taking into account both duration and severity of ischemia, but this hypothesis requires further studies. Third, it is possible that ischemic brain injury itself is responsible for additional small bowel dysfunction (30,31). According to this hypothesis, patients with a poor neurological outcome, being those with the worst brain ischemia, could have more gut injury than patients with neurological recovery.…”

Section: Discussionmentioning

confidence: 99%

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Enterocyte Damage

Piton

Belin

Barrot

et al. 2015

Shock

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Cardiac arrest is considered to be a cause of small bowel ischemia, but the consequences of cardiac arrest on the human small bowel have been rarely studied. Plasma citrulline concentration is a marker of functional enterocyte mass, and plasma intestinal fatty acid-binding protein (I-FABP) concentration is a marker of enterocyte damage. We aimed to measure enterocyte biomarkers after cardiac arrest and to study the prognostic value of biomarker abnormalities. This is a prospective, observational, single-center study of patients admitted to the intensive care unit (ICU) for cardiac arrest, evaluating plasma citrulline and I-FABP concentrations at admission and after 24 h and variables according to the Utstein criteria. Variables according to 28-day Cerebral Performance Category score of 1 to 2 (good neurological outcome) versus 3 to 5 (poor neurological outcome) were compared. Sixty-nine patients with cardiac arrest of both cardiac and hypoxic origin were included. At ICU admission, plasma citrulline concentration was low in 65% and plasma I-FABP was elevated in 82% of the patients. After 24 h, plasma citrulline was low in 82% and I-FABP was normal in 60% of the patients. Patients with a poor neurological outcome had a lower plasma citrulline concentration and a higher I-FABP concentration at ICU admission. By multivariate analysis, plasma citrulline levels of 13.1 μmol L or less and I-FABP more than 260 pg mL were independently associated with a poor neurological outcome (odds ratio, 21.9 [2.2-215], and odds ratio, 13.6 [1.4-129], respectively). Cardiac arrest resuscitation is associated with evidence of small bowel mucosal damage in most patients, with a short and intense I-FABP elevation at admission and a decrease in citrulline concentration during the first day. In this study, low plasma citrulline and high I-FABP concentrations at ICU admission were predictive of a poor neurological outcome. This study confirms that cardiac arrest is a model of small bowel mucosal ischemia and suggests that enterocyte damage is a piece in the puzzle of post-cardiac arrest syndrome.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Enterocyte Damage

Piton

Belin

Barrot

et al. 2015

Shock

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“…Second, an assessment of L-arginine which was not determined in the current study, would have provided more insight into NOS function than ADMA itself. It has been demonstrated that TBI alters L-arginine levels and therefore it is possible that CSF L-arginine depletion may account for the observed altered ADMA levels (55, 56). Finally, the control subjects in this study were diagnosed with meningoencephalitis and pulmonary hypertension which potentially could have an influence on ADMA levels.…”

Section: Discussionmentioning

confidence: 99%

Hypothermia Decreases Cerebrospinal Fluid Asymmetric Dimethylarginine Levels in Children With Traumatic Brain Injury

Thampatty

Klamerus²,

Oberly³

et al. 2013

Pediatric Critical Care Medicine

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Objectives Pathological increases in asymmetric dimethylarginine (ADMA), an endogenous nitric oxide synthase (NOS) inhibitor, have been implicated in endothelial dysfunction and vascular diseases. Reduced NO early after traumatic brain injury (TBI) may contribute to hypoperfusion. Currently, methods to quantify ADMA in the cerebrospinal fluid (CSF) have not been fully explored. We aimed to develop and validate a method to determine ADMA in the CSF of a pediatric TBI population and to use this method to assess the effects of (i) TBI and (ii) therapeutic hypothermia (TH) on this mediator. Design, Setting, Patients An ancillary study to a prospective, phase II randomized clinical trial (RCT) of early hypothermia in a tertiary care pediatric intensive care unit for children with TBI admitted to Children's Hospital of Pittsburgh. Interventions None Measurements and Main Results A UPLC-MS/MS method was developed and validated to quantitate ADMA. A total of 56 samples collected over 3 days starting with injury onset were analyzed from the CSF of consented therapeutic hypothermia (n=9) and normothermia (n=10) children. Children undergoing diagnostic lumbar puncture (n=5) were controls. ADMA was present at a quantifiable level in all samples. Mean ADMA levels were significantly increased in normothermic TBI children compared to control (0.19± 0.08 μmol/L and 0.11± 0.02μmol/L respectively, p=0.01), and hypothermic children had significantly reduced mean ADMA levels (0.11 ± 0.05 μmol/L) vs. normothermic (p=0.03) measured on day 3. Patient demographics including age, gender, and NO levels (measured as nitrite and nitrate using liquid chromatography coupled with Griess reaction) did not significantly differ between normothermia and hypothermia groups. Also, NO levels did not correlate with ADMA concentrations. Conclusions ADMA levels were significantly increased in the CSF of TBI children. Early hypothermia attenuated this increase. The implications of attenuated ADMA on NOS activity and regional cerebral blood flow after TBI by TH deserve future attention.

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“…Jeter et al (2012) used chromatography and mass spectrometry to assess L-arginine and its metabolic products in the plasma (<24 h) of mTBI patients, but did not observe changes as compared to controls. The same group also assessed branched chain amino acids (BCAA) in plasma (<24) of mTBI patients (Jeter et al, 2013b).…”

Section: The Hypothesis-driven Approachmentioning

confidence: 99%

Current status of fluid biomarkers in mild traumatic brain injury

Kulbe

Geddes

2016

Experimental Neurology

109

111

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Mild traumatic brain injury (mTBI) affects millions of people annually and is difficult to diagnose. Mild injury is insensitive to conventional imaging techniques and diagnoses are often made using subjective criteria such as self-reported symptoms. Many people who sustain a mTBI develop persistent post-concussive symptoms. Athletes and military personnel are at great risk for repeat injury which can result in second impact syndrome or chronic traumatic encephalopathy. An objective and quantifiable measure, such as a serum biomarker, is needed to aid in mTBI diagnosis, prognosis, return to play/duty assessments, and would further elucidate mTBI pathophysiology. The majority of TBI biomarker research focuses on severe TBI with few studies specific to mild injury. Most studies use a hypothesis-driven approach, screening biofluids for markers known to be associated with TBI pathophysiology. This approach has yielded limited success in identifying markers that can be used clinically, additional candidate biomarkers are needed. Innovative and unbiased methods such as proteomics, microRNA arrays, urinary screens, autoantibody identification and phage display would complement more traditional approaches to aid in the discovery of novel mTBI biomarkers.

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Human Traumatic Brain Injury Alters Circulating L-Arginine and Its Metabolite Levels: Possible Link to Cerebral Blood Flow, Extracellular Matrix Remodeling, and Energy Status

Cited by 38 publications

References 38 publications

Enterocyte Damage

Enterocyte Damage

Hypothermia Decreases Cerebrospinal Fluid Asymmetric Dimethylarginine Levels in Children With Traumatic Brain Injury

Current status of fluid biomarkers in mild traumatic brain injury

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