Inflammatory Cell Infiltration after Endothelin-1-Induced Cerebral Ischemia: Histochemical and Myeloperoxidase Correlation with Temporal Changes in Brain Injury

Weston, Robert M.; Jones, Nicole M.; Jarrott, Bevyn; Callaway, Jennifer K.

doi:10.1038/sj.jcbfm.9600324

Cited by 124 publications

(114 citation statements)

References 97 publications

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“…We found that MPO, a key enzyme secreted in the inflammatory response to tissue injury, is widely distributed in the ischemic tissues, and correlated positively with infarct size. The peak level of MPO activity, determined by activation of the MPO-sensing agent in vivo and confirmed by MPO activity assays and qRT-PCR analyses, occurred on day 3 after ischemia in our model, similar to previous ex vivo findings (5). Both neutrophils and macrophages/microglia contribute to secrete MPO in the ischemic brain, although neutrophils peak earlier (days 1-3), whereas macrophages/microglia are most abundant later (days 3-7).…”

Section: Discussionsupporting

confidence: 74%

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Tracking the inflammatory response in stroke in vivo by sensing the enzyme myeloperoxidase

Breckwoldt

Chen

Stangenberg³

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

275

240

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Inflammation can extend ischemic brain injury and adversely affect outcome in experimental animal models. A key difficulty in translating animal studies to humans is the lack of a definitive method to confirm and track inflammation in the brain in vivo. Myeloperoxidase (MPO), a key inflammatory enzyme secreted by activated neutrophils and macrophages/microglia, can generate highly reactive oxygen species to cause additional damage in cerebral ischemia. We report here that a functional, enzyme-activatable MRI agent can accurately track the oxidative activity of MPO noninvasively in stroke in living animals. We found that MPO is widely distributed in ischemic tissues, correlates positively with infarct size, and is detected even 3 weeks postinfarction. The peak level of MPO activity, determined by activation of the MPO-sensing agent in vivo and confirmed by MPO activity and quantitative RT-PCR assays, occurred on day 3 after ischemia. Both neutrophils and macrophages/microglia contribute to secrete MPO in the ischemic brain, although neutrophils peak earlier (days 1-3) whereas macrophages/microglia are most abundant later (days 3-7). In contrast to the conventional MRI agent diethylenetriaminepentatacetate gadolinium, which reports blood-brain barrier disruption, MPO imaging is able to additionally track MPO activity and confirm inflammation on the molecular level in vivo, information that was previously only possible to obtain on ex vivo brain sections and impossible to assess in living human patients. Our findings could allow efficient noninvasive serial screening of therapies targeting inflammation and the use of MPO imaging as an imaging biomarker to risk-stratify patients.inflammation ͉ ischemia ͉ molecular imaging ͉ MRI ͉ brain

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Section: Discussionsupporting

confidence: 74%

“…Inflammation in stroke has been traditionally identified on histopathology as neutrophil infiltration, which correlates positively with ischemic damage (5). Myeloperoxidase (MPO) is the most abundant component in azurophilic granules in neutrophils and has often been used as a histopathological marker for neutrophils (6).…”

mentioning

confidence: 99%

Tracking the inflammatory response in stroke in vivo by sensing the enzyme myeloperoxidase

Breckwoldt

Chen

Stangenberg³

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

275

240

View full text Add to dashboard Cite

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“…29 Neutrophil accumulation peaked at 3 days and persisted for at least 15 days. 8 The present human data are consistent with these results: neonates with abnormal neurologic outcome had significantly higher peripheral WBC and ANC by 12 to 24 h of life compared to neonates with good long-term neurologic outcome. Because neutrophils produce reactive and toxic metabolites such as reactive oxygen species and hypochlorous acid via two enzymes, membrane-associated nicotinamide adenine dinucleotide phosphate (NADPH) oxidase and myeloperoxidase, respectively, continued and prolonged accumulation of neutrophils in the injured area exacerbates hypoxic-ischemic-induced brain injury.…”

supporting

confidence: 81%

“…5 Hypoxia increases white blood cell (WBC) production and the number of circulating neutrophils, 6 while cytokines increase vascular permeability 7 and upregulate expression of intercellular adhesion molecules (ICAM), mediators that induce migration of leukocytes and promote local inflammatory reactions. 8 In addition, cytokines increase the affinity of neutrophil integrins to ICAMs 8,9 promoting transendothelial migration. 7,10,11 Inflammation-induced cell injury occurs due to the 'oxidation burst' that involves neutrophil production of reactive and toxic metabolites such as hydrogen peroxide, superoxide anion and hypochlorous acid.…”

Section: Introductionmentioning

confidence: 99%

Elevated total peripheral leukocyte count may identify risk for neurological disability in asphyxiated term neonates

et al. 2007

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Objective: The present study investigated the relationship between neurologic outcome and total circulating white blood cell (WBC) and absolute neutrophil counts (ANCs) in the first week of life in term infants with hypoxic-ischemic encephalopathy (HIE).Study design: Long-term neurologic outcome at 18 months was measured retrospectively in 30 term neonates with HIE using the Pediatric Cerebral Performance Category Scale (PCPCS) score with outcomes dichotomized as either good or poor. We then compared white blood cell and ANC levels during the first 4 days of life and magnetic resonance imaging (MRI) obtained within the first month life between the two PCPCS groups. MRI was quantified using a validated scoring system. Results:Neonates with good long-term outcomes had significantly lower MRI scores (indicating lesser injury) than neonates with poor outcomes. More importantly, neonates with poor outcomes had significantly higher WBC and ANC levels as early as12 h after birth and up to 96 h after birth compared to those with good outcomes. These data suggest that elevated peripheral neutrophil counts in the first 96 h of life may signal or predict adverse long-term outcome.Conclusions: Our findings suggest that elevated peripheral neutrophil counts in the first 96 h of life in term infants with HIE may contribute to abnormal neurodevelopmental outcome.

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“…8 These infiltrating cells include neutrophils, monocytes, macrophages, dendritic cells, T and B lymphocytes, and natural killer cells. 8 For example, clinical and experimental data suggest that neutrophils are a key immune cell to enter the brain after ischemia, and neutrophil number correlates with the severity of an ischemic lesion, 9,10 although there is some controversy as to whether this is an early event or is delayed by up to 3 days. 8 It is also remains controversial as to whether neutrophils contribute directly to secondary brain damage or are merely bystanders that mainly assist in promoting tissue repair and recovery.…”

Section: Introductionmentioning

confidence: 99%

Immune Cell Infiltration in Malignant Middle Cerebral Artery Infarction: Comparison with Transient Cerebral Ischemia

Chu

Kim

Lee

et al. 2013

J Cereb Blood Flow Metab

178

175

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We tested whether significant leukocyte infiltration occurs in a mouse model of permanent cerebral ischemia. C57BL6/J male mice underwent either permanent (3 or 24 hours) or transient (1 or 2 hours þ 22-to 23-hour reperfusion) middle cerebral artery occlusion (MCAO). Using flow cytometry, we observed B15,000 leukocytes (CD45 þ high cells) in the ischemic hemisphere as early as 3 hours after permanent MCAO (pMCAO), comprising B40% lymphoid cells and B60% myeloid cells. Neutrophils were the predominant cell type entering the brain, and were increased to B5,000 as early as 3 hours after pMCAO. Several cell types (monocytes, macrophages, B lymphocytes, CD8þ T lymphocytes, and natural killer cells) were also increased at 3 hours to levels sustained for 24 hours, whereas others (CD4 þ T cells, natural killer T cells, and dendritic cells) were unchanged at 3 hours, but were increased by 24 hours after pMCAO. Immunohistochemical analysis revealed that leukocytes typically had entered and widely dispersed throughout the parenchyma of the infarct within 3 hours. Moreover, compared with pMCAO, there were B50% fewer infiltrating leukocytes at 24 hours after transient MCAO (tMCAO), independent of infarct size. Microglial cell numbers were bilaterally increased in both models. These findings indicate that a profound infiltration of inflammatory cells occurs in the brain early after focal ischemia, especially without reperfusion.

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Inflammatory Cell Infiltration after Endothelin-1-Induced Cerebral Ischemia: Histochemical and Myeloperoxidase Correlation with Temporal Changes in Brain Injury

Cited by 124 publications

References 97 publications

Tracking the inflammatory response in stroke in vivo by sensing the enzyme myeloperoxidase

Tracking the inflammatory response in stroke in vivo by sensing the enzyme myeloperoxidase

Elevated total peripheral leukocyte count may identify risk for neurological disability in asphyxiated term neonates

Immune Cell Infiltration in Malignant Middle Cerebral Artery Infarction: Comparison with Transient Cerebral Ischemia

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