Blockade of adrenoreceptors inhibits the splenic response to stroke

Ajmo, Craig T.; Collier, Lisa A.; Leonardo, Christopher C.; Hall, Aaron A.; Green, Suzanne M.; Womble, Tracy; Cuevas, Javier; Willing, Alison E.; Pennypacker, Keith R.

doi:10.1016/j.expneurol.2009.03.044

Cited by 128 publications

(129 citation statements)

References 49 publications

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“…Separate experiments completed by Offner et al have shown a peripheral increase in production of the pro inflammatory cytokines TNF , IFN , IL-6, MCP-1, and IL-2 after ischemic stroke . Further work completed by Ajmo et al has shown that ischemic stroke is associated with adrenergic output that stimulates the spleen to release immune (T and B cells) into the systemic circulation that ultimately lead to increased cavity size after MCAO stroke in a rodent model (Ajmo, et al, 2009). Furthermore, Verdrame et al have shown similar results indicating the release of immune cells (CD8+ T cells) is correlated with a reduction in splenic mass.…”

Section: Discussionmentioning

confidence: 99%

Intravenous multipotent adult progenitor cell therapy for traumatic brain injury: Preserving the blood brain barrier via an interaction with splenocytes

Walker¹,

Jiménez²,

Shah³

et al. 2010

Journal of the American College of Surgeons

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Recent investigation has shown an interaction between transplanted progenitor cells and resident splenocytes leading to modulation of the immunologic response in neurological injury. We hypothesize that the intravenous injection of multipotent adult progenitor cells (MAPC) confers neurovascular protection after traumatic brain injury through an interaction with resident splenocytes, subsequently leading to preservation of the blood brain barrier.Four groups of rats underwent controlled cortical impact injury (3 groups) or sham injury (1 group). MAPC were injected via the tail vein at two doses (2*10 6 MAPC/kg or 10*10 6 MAPC/kg) 2 and 24 hours after injury. Blood brain barrier permeability was assessed by measuring Evans blue dye extravasation (n=6/group). Additionally, splenic mass was measured (n=12/group) followed by splenocyte characterization (n=9/group) including: cell cycle analysis (n=6/group), apoptosis index (n=6/group), cell proliferation (n=6/group), and inflammatory cytokine measurements (n=6/group). Vascular architecture was determined by immunohistochemistry (n=3/ group). Traumatic brain injury results in a decrease in splenic mass and increased blood brain barrier permeability. Intravenous infusion of MAPC preserved splenic mass and returned blood brain

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Section: Discussionmentioning

confidence: 99%

Intravenous multipotent adult progenitor cell therapy for traumatic brain injury: Preserving the blood brain barrier via an interaction with splenocytes

Walker¹,

Jiménez²,

Shah³

et al. 2010

Journal of the American College of Surgeons

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“…By these molecules, infiltrating neutrophils amplify a cerebral inflammatory response that may exacerbate post-ischemic brain damage (49,51,52). Furthermore, infiltrating neutrophils are the primary source of enhanced matrix metalloproteinase 9 activity in the ischemic brain, which is a critical mechanism underlying the breakdown of the BBB and the exacerbation of neurological injury (53).…”

Section: Microglia-innate Immune Cells Of the Brainmentioning

confidence: 99%

Inflammatory mechanisms involved in brain injury following cardiac arrest and cardiopulmonary resuscitation

et al. 2016

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Abstract. Cardiac arrest (CA) is a leading cause of fatality and long-term disability worldwide. Recent advances in cardiopulmonary resuscitation (CPR) have improved survival rates; however, the survivors are prone to severe neurological injury subsequent to successful CPR following CA. Effective therapeutic options to protect the brain from CA remain limited, due to the complexities of the injury cascades caused by global cerebral ischemia/reperfusion (I/R). Although the precise mechanisms of neurological impairment following CA-initiated I/R injury require further clarification, evidence supports that one of the key cellular pathways of cerebral injury is inflammation. The inflammatory response is orchestrated by activated glial cells in response to I/R injury. Increased release of danger-associated molecular pattern molecules and cellular dysfunction in activated microglia and astrocytes contribute to ischemia-induced cytotoxic and pro-inflammatory cytokines generation, and ultimately to delayed death of neurons. Furthermore, cytokines and adhesion molecules generated within activated microglia, as well as astrocytes, are involved in the innate immune response; modulate influx of peripheral immune and inflammatory cells into the brain, resulting in neurological injury. The present review discusses the molecular aspects of immune and inflammatory mechanisms in global cerebral I/R injury following CA and CPR, and the potential therapeutic strategies that target neuroinflammation and the innate immune system.

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“…14 It has further been demonstrated in experimental stroke models that pre or immediate poststroke surgical removal or irradiation of the spleen attenuates these responses, and results in reduced stroke lesion size and enhanced recovery. 5,[14][15][16][17][18][19] The pre-clinical body of evidence raises an exciting possibility that novel therapies can be designed to target the spleen as an approach to modulate post-stroke inflammation and dampen secondary brain injury. [20][21][22][23][24] However, the road to translation of these findings in the clinical setting is beset with challenges.…”

Section: Introductionmentioning

confidence: 99%

Acute splenic responses in patients with ischemic stroke and intracerebral hemorrhage

Vahidy

Parsha

Rahbar

et al. 2015

J Cereb Blood Flow Metab

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Animal models provide evidence of spleen mediated post-stroke activation of the peripheral immune system. Translation of these findings to stroke patients requires estimation of pre-stroke spleen volume along with quantification of its dayto-day variation. We enrolled a cohort of 158 healthy volunteers and measured their spleen volume over the course of five consecutive days. We also enrolled a concurrent cohort of 158 stroke patients, measured initial spleen volume within 24 h of stroke symptom onset followed by daily assessments. Blood samples for cytokine analysis were collected from a subset of patients. Using data from healthy volunteers, we fit longitudinal quantile regression models to construct gender and body surface area based normograms of spleen volume. We quantified day-to-day variation and defined splenic contraction. Based on our criteria, approximately 40% of stroke patients experienced substantial post-stroke reduction in splenic volume. African Americans, older patients, and patients with past history of stroke have significantly higher odds of post-stroke splenic contraction. All measured cytokine levels were elevated in patients with splenic contraction, with significant differences for interferon gamma, interleukin 6, 10, 12, and 13. Our work provides reference standards for further work, validation of pre-clinical findings, and characterization of patients with post-stroke splenic contraction.

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Blockade of adrenoreceptors inhibits the splenic response to stroke

Cited by 128 publications

References 49 publications

Intravenous multipotent adult progenitor cell therapy for traumatic brain injury: Preserving the blood brain barrier via an interaction with splenocytes

Intravenous multipotent adult progenitor cell therapy for traumatic brain injury: Preserving the blood brain barrier via an interaction with splenocytes

Inflammatory mechanisms involved in brain injury following cardiac arrest and cardiopulmonary resuscitation

Acute splenic responses in patients with ischemic stroke and intracerebral hemorrhage

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