Your search keyword '"Stenzel-Poore MP"' showing total 96 results

1. GDF10 is a signal for axonal sprouting and functional recovery after stroke

Author

Li, S, Nie, EH, Yin, Y, Benowitz, LI, Tung, S, Vinters, HV, Bahjat, FR, Stenzel-Poore, MP, Kawaguchi, R, Coppola, G, and Carmichael, ST

Subjects

Neurology & Neurosurgery, Neurosciences, Psychology, Cognitive Sciences

Abstract

Stroke produces a limited process of neural repair. Axonal sprouting in cortex adjacent to the infarct is part of this recovery process, but the signal that initiates axonal sprouting is not known. Growth and differentiation factor 10 (GDF10) is induced in peri-infarct neurons in mice, non-human primates and humans. GDF10 promotes axonal outgrowth in vitro in mouse, rat and human neurons through TGFβRI and TGFβRII signaling. Using pharmacogenetic gain- and loss-of-function studies, we found that GDF10 produced axonal sprouting and enhanced functional recovery after stroke; knocking down GDF10 blocked axonal sprouting and reduced recovery. RNA sequencing from peri-infarct cortical neurons revealed that GDF10 downregulated PTEN, upregulated PI3 kinase signaling and induced specific axonal guidance molecules. Using unsupervised genome-wide association analysis of the GDF10 transcriptome, we found that it was not related to neurodevelopment, but may partially overlap with other CNS injury patterns. Thus, GDF10 is a stroke-induced signal for axonal sprouting and functional recovery.

Published

2015

2. Overproduction of corticotropin-releasing factor in transgenic mice: a genetic model of anxiogenic behavior

Author

Stenzel-Poore, MP, primary, Heinrichs, SC, additional, Rivest, S, additional, Koob, GF, additional, and Vale, WW, additional

Published

1994

3. Preconditioning reprograms the response to ischemic injury and primes the emergence of unique endogenous neuroprotective phenotypes: a speculative synthesis.

Author

Stenzel-Poore MP, Stevens SL, King JS, Simon RP, Stenzel-Poore, Mary P, Stevens, Susan L, King, Jeffrey S, and Simon, Roger P

Published

2007

4. Mice deficient in corticotropin-releasing factor receptor type 2 exhibit normal ethanol-associated behaviors [corrected] [published erratum appears in ALCOHOLISM 2008 Nov;32(11):2028].

Author

Sharpe AL, Coste SC, Burkhart-Kasch S, Li N, Stenzel-Poore MP, and Phillips TJ

Abstract

BACKGROUND: Stress is believed to influence alcohol use and relapse in alcoholics. Animal studies suggest an interaction between corticotropin-releasing factor (CRF) and its receptors and the behavioral effects and consumption of alcohol. The objective of these studies was to examine the effect of corticotropin-releasing factor receptor type 2 (CRF2) on ethanol consumption, conditioned taste aversion, sedation, and hypothermia. METHODS: CRF2-null mutant or knock-out (KO), and wild-type (WT) mice were used to assess consumption of increasing concentrations of ethanol in a two-bottle, 24-hr test and during daily limited-access sessions. Ethanol-induced conditioned taste aversion (CTA), loss of righting reflex (LORR), hypothermia, and ethanol metabolism kinetics were also examined in the CRF2 KO and WT mice. RESULTS: CRF2 KO mice did not differ from WT mice in sensitivity to ethanol-induced CTA, LORR, hypothermia, or ethanol metabolism kinetics. There was no genotypic difference in ethanol intake or preference in the 24-hr, two-bottle choice procedure, and only modestly reduced consumption of the 7.5 and 10% ethanol solutions in KO versus WT mice in the limited-access procedure. CONCLUSIONS: CRF2 deficiency had little effect on several ethanol-associated behaviors in CRF2-null mutant compared with WT mice, suggesting that this receptor does not have a primary role in modulating these behaviors. Evidence of a role for this receptor in neural circuits subserving stress-coping behaviors suggest that future studies should focus on the role of endogenous CRF2 in ethanol-associated behaviors in mice that are stressed or withdrawing from dependence on ethanol. [ABSTRACT FROM AUTHOR]

Published

2005

5. Identification and Characterization of Small-Molecule IRF3-Dependent Immune Activators for Pharmaceutical Development.

Author

Foss MH, Stevens SL, Jin H, Allen EM, Nelson D, DeFilippis V, Nilsen A, and Stenzel-Poore MP

Subjects

Animals, Antiviral Agents pharmacology, Drug Development, Macrophages metabolism, Mice, Interferon Regulatory Factor-3 metabolism, Signal Transduction

Abstract

We sought to develop a small-molecule activator of interferon regulatory factor 3 (IRF3), an essential innate immune transcription factor, which could potentially be used therapeutically in multiple disease settings. Using a high-throughput screen, we identified small-molecule entities that activate a type I interferon response, with minimal off-target NFκB activation. We identified 399 compounds at a hit rate of 0.24% from singlicate primary screening. Secondary screening included the primary hits and additional compounds with similar chemical structures obtained from other library sources and resulted in 142 candidate compounds. The hit compounds were sorted and ranked to identify compound groups with activity in both human and mouse backgrounds to facilitate animal model engagement for translational development. Chemical modifications within two groups of small molecules produced leads with improved activity over original hits. Furthermore, these leads demonstrated activity in ex vivo cytokine release assays from human blood- and mouse bone marrow-derived macrophages. Dependence on IRF3 was demonstrated using bone marrow-derived macrophages from IRF3-deficient mice, which were not responsive to the molecules. To identify the upstream pathway leading to IRF3 activation, we used a library of CRISPR knockout cell lines to test the key innate immune adaptor and receptor molecules. These studies indicated a surprising toll-interleukin-1 receptor-domain-containing-adapter-inducing interferon-β-dependent but TLR3/4-independent mechanism of IRF3 activation.

Published

2022

6. CpG preconditioning reduces accumulation of lysophosphatidylcholine in ischemic brain tissue after middle cerebral artery occlusion.

Author

Mavroudakis L, Stevens SL, Duncan KD, Stenzel-Poore MP, Laskin J, and Lanekoff I

Subjects

Animals, Disease Models, Animal, Infarction, Middle Cerebral Artery pathology, Male, Mass Spectrometry, Mice, Inbred C57BL, Oligodeoxyribonucleotides administration & dosage, Mice, Brain pathology, Brain Chemistry, Infarction, Middle Cerebral Artery therapy, Lysophosphatidylcholines analysis, Oligodeoxyribonucleotides therapeutic use

Abstract

Ischemic stroke is one of the major causes of death and permanent disability in the world. However, the molecular mechanisms surrounding tissue damage are complex and further studies are needed to gain insights necessary for development of treatment. Prophylactic treatment by administration of cytosine-guanine (CpG) oligodeoxynucleotides has been shown to provide neuroprotection against anticipated ischemic injury. CpG binds to Toll-like receptor 9 (TLR9) causing initialization of an inflammatory response that limits visible ischemic damages upon subsequent stroke. Here, we use nanospray desorption electrospray ionization (nano-DESI) mass spectrometry imaging (MSI) to characterize molecular effects of CpG preconditioning prior to middle cerebral artery occlusion (MCAO) and reperfusion. By doping the nano-DESI solvent with appropriate internal standards, we can study and compare distributions of phosphatidylcholine (PC) and lysophosphatidylcholine (LPC) in the ischemic hemisphere of the brain despite the large changes in alkali metal abundances. Our results show that CpG preconditioning not only reduces the infarct size but it also decreases the degradation of PC and accumulation of LPC species, which indicates reduced cell membrane breakdown and overall ischemic damage. Our findings show that molecular mechanisms of PC degradation are intact despite CpG preconditioning but that these are limited due to the initialized inflammatory response.

Published

2021

7. Preconditioning in the Rhesus Macaque Induces a Proteomic Signature Following Cerebral Ischemia that Is Associated with Neuroprotection.

Author

Stevens SL, Liu T, Bahjat FR, Petyuk VA, Schepmoes AA, Sontag RL, Gritsenko MA, Wu C, Wang S, Shukla AK, Jacobs JM, Smith RD, Rodland KD, Alexander West G, Kohama SG, Glynn C, and Stenzel-Poore MP

Subjects

Animals, Brain Ischemia pathology, Macaca mulatta, Male, Neuroprotection drug effects, Toll-Like Receptor 9 agonists, Brain Ischemia cerebrospinal fluid, Brain Ischemia prevention & control, Ischemic Preconditioning methods, Neuroprotection physiology, Proteomics methods

Abstract

Each year, thousands of patients are at risk of cerebral ischemic injury, due to iatrogenic responses to surgical procedures. Prophylactic treatment of these patients as standard care could minimize potential neurological complications. We have shown that protection of brain tissue, in a non-human primate model of cerebral ischemic injury, is possible through pharmacological preconditioning using the immune activator D192935. We postulate that preconditioning with D192935 results in neuroprotective reprogramming that is evident in the brain following experimentally induced cerebral ischemia. We performed quantitative proteomic analysis of cerebral spinal fluid (CSF) collected post-stroke from our previously published efficacy study to determine whether CSF protein profiles correlated with induced protection. Four groups of animals were examined: naïve animals (no treatment or stroke); animals treated with vehicle prior to stroke; D192935 treated and stroked animals, further delineated into two groups, ones that were protected (small infarcts) and those that were not protected (large infarcts). We found that distinct protein clusters defined the protected and non-protected animal groups, with a 16-member cluster of proteins induced exclusively in D192935 protected animals. Seventy percent of the proteins induced in the protected animals have functions that would enhance neuroprotection and tissue repair, including several members associated with M2 macrophages, a macrophage phenotype shown to contribute to neuroprotection and repair during ischemic injury. These studies highlight the translational importance of CSF biomarkers in defining mechanism and monitoring responses to treatment in development of stroke therapeutics.

Published

2019

8. Translational Stroke Research: Vision and Opportunities.

Author

Bosetti F, Koenig JI, Ayata C, Back SA, Becker K, Broderick JP, Carmichael ST, Cho S, Cipolla MJ, Corbett D, Corriveau RA, Cramer SC, Ferguson AR, Finklestein SP, Ford BD, Furie KL, Hemmen TM, Iadecola C, Jakeman LB, Janis S, Jauch EC, Johnston KC, Kochanek PM, Kohn H, Lo EH, Lyden PD, Mallard C, McCullough LD, McGavern LM, Meschia JF, Moy CS, Perez-Pinzon MA, Ramadan I, Savitz SI, Schwamm LH, Steinberg GK, Stenzel-Poore MP, Tymianski M, Warach S, Wechsler LR, Zhang JH, and Koroshetz W

Subjects

Age Factors, Animals, Chronic Disease, Comorbidity, Disease Models, Animal, Humans, Recovery of Function, Sex Factors, Stroke epidemiology, Stroke physiopathology, Research, Stroke therapy, Thrombectomy methods, Thrombolytic Therapy methods, Translational Research, Biomedical

Published

2017

9. Preclinical Development of a Prophylactic Neuroprotective Therapy for the Preventive Treatment of Anticipated Ischemia-Reperfusion Injury.

Author

Bahjat FR, Alexander West G, Kohama SG, Glynn C, Urbanski HF, Hobbs TR, Earl E, Stevens SL, and Stenzel-Poore MP

Subjects

Analysis of Variance, Animals, Brain Infarction diagnostic imaging, Brain Infarction drug therapy, Brain Infarction etiology, Disease Models, Animal, Dose-Response Relationship, Drug, Macaca mulatta, Male, Mice, Mice, Inbred C57BL, Neurologic Examination, Neuroprotective Agents chemistry, Oligodeoxyribonucleotides chemistry, Physical Conditioning, Animal physiology, Reperfusion Injury complications, Time Factors, Brain Ischemia prevention & control, Cytokines metabolism, Drug Evaluation, Preclinical, Neuroprotective Agents therapeutic use, Oligodeoxyribonucleotides therapeutic use, Reperfusion Injury prevention & control

Abstract

Ischemia-reperfusion brain injury can be iatrogenically induced secondary to life-saving procedures. Prophylactic treatment of these patients offers a promising prevention for lifelong complications. We postulate that a cytosine-guanine (CpG) oligodeoxynucleotide (ODN) can provide robust antecedent protection against cerebral ischemic injury with minimal release of pro-inflammatory cytokines, making it an ideal candidate for further clinical development. Mouse and nonhuman primate (NHP) models of cerebral ischemic injury were used to test whether an A-type CpG ODN, which induces minimal systemic inflammatory cytokine responses, can provide prophylactic protection. Extent of injury in the mouse was measured by histological staining of live tissue. In the NHP, injury was assessed 2 and 7 days post-occlusion from T2-weighted magnetic resonance images and neurological and motor deficits were cataloged daily. Plasma cytokine levels were measured using species-specific Luminex assays. Prophylactic administration of an A-type CpG ODN provided robust protection against cerebral ischemic injury in the mouse with minimal systemic inflammation. Rhesus macaques treated with D192935, a mixture of human optimized A-type CpG ODNs, had smaller infarcts and demonstrated significantly less neurological and motor deficits following ischemic injury. Our findings demonstrate the translational potential of D192935 as a prophylactic treatment for patients at risk of cerebral ischemic injury.

Published

2017

10. Cytosolic Receptor Melanoma Differentiation-Associated Protein 5 Mediates Preconditioning-Induced Neuroprotection Against Cerebral Ischemic Injury.

Author

Gesuete R, Christensen SN, Bahjat FR, Packard AE, Stevens SL, Liu M, Salazar AM, and Stenzel-Poore MP

Subjects

Animals, Carboxymethylcellulose Sodium analogs & derivatives, Carboxymethylcellulose Sodium metabolism, Carboxymethylcellulose Sodium therapeutic use, Interferon-Induced Helicase, IFIH1, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Neuroprotective Agents metabolism, Neuroprotective Agents therapeutic use, Poly I-C metabolism, Poly I-C therapeutic use, Polylysine analogs & derivatives, Polylysine metabolism, Polylysine therapeutic use, Brain Ischemia metabolism, Brain Ischemia prevention & control, DEAD-box RNA Helicases metabolism, Ischemic Preconditioning methods, Stroke metabolism, Stroke prevention & control

Abstract

Background and Purpose: Preconditioning with poly-l-lysine and carboxymethylcellulose (ICLC) provides robust neuroprotection from cerebral ischemia in a mouse stroke model. However, the receptor that mediates neuroprotection is unknown. As a synthetic double-stranded RNA, poly-ICLC may bind endosomal Toll-like receptor 3 or one of the cytosolic retinoic acid-inducible gene-I-like receptor family members, retinoic acid-inducible gene-I, or melanoma differentiation-associated protein 5. Activation of these receptors culminates in type I interferons (IFN-α/β) induction-a response required for poly-ICLC-induced neuroprotection. In this study, we investigate the receptor required for poly-ICLC-induced neuroprotection., Methods: Toll-like receptor 3, melanoma differentiation-associated protein 5-, and IFN-promoter stimulator 1-deficient mice were treated with poly-ICLC 24 hours before middle cerebral artery occlusion. Infarct volume was measured 24 hours after stroke to identify the receptor signaling pathways involved in protection. IFN-α/β induction was measured in plasma samples collected 6 hours after poly-ICLC treatment. IFN-β-deficient mice were used to test the requirement of IFN-β for poly-ICLC-induced neuroprotection. Mice were treated with recombinant IFN-α-A to test the role of IFN-α as a potential mediator of neuroprotection., Results: Poly-ICLC induction of both neuroprotection and systemic IFN-α/β requires the cytosolic receptor melanoma differentiation-associated protein 5 and the adapter molecule IFN-promoter stimulator 1, whereas it is independent of Toll-like receptor 3. IFN-β is not required for poly-ICLC-induced neuroprotection. IFN-α treatment protects against stroke., Conclusions: Poly-ICLC preconditioning is mediated by melanoma differentiation-associated protein 5 and its adaptor molecule IFN-promoter stimulator 1. This is the first evidence that a cytosolic receptor can mediate neuroprotection, providing a new target for the development of therapeutic agents to protect the brain from ischemic injury., (© 2015 American Heart Association, Inc.)

Published

2016

11. Role of Circulating Immune Cells in Stroke and Preconditioning-Induced Protection.

Author

Gesuete R, Stevens SL, and Stenzel-Poore MP

Subjects

Animals, Humans, Ischemic Preconditioning, Lymphocytes immunology, Macrophages immunology, Neuroprotection immunology, Neutrophils immunology, Stroke immunology

Abstract

Stroke activates an inflammatory response that results in the infiltration of peripheral immune cells into the ischemic area, contributing to exacerbation of tissue damage. However, evidence indicates that inflammatory cell infiltration can also promote neuroprotection through regulatory immune cells that mitigate injury. These immune regulatory cells may also be important mediators of neuroprotection associated with preconditioning, a phenomenon whereby small exposure to a potential harmful stimulus is able to induce protection against a subsequent ischemic event. The elucidation of mechanisms that allow these immune cells to confer neuroprotection is critical to developing new therapeutic strategies against acute stroke. In the present review, we discuss the dual role of peripheral immune cells in stroke-related brain injury and neuroprotection. Furthermore, we report new data from our laboratory that supports the important role of peripheral cells and their interaction with the brain endothelium for the establishment of the protective phenotype in preconditioning.

Published

2016

12. CpG preconditioning regulates miRNA expression that modulates genomic reprogramming associated with neuroprotection against ischemic injury.

Author

Vartanian KB, Mitchell HD, Stevens SL, Conrad VK, McDermott JE, and Stenzel-Poore MP

Subjects

Adjuvants, Immunologic pharmacology, Animals, Brain Ischemia metabolism, Male, Mice, Oligonucleotide Array Sequence Analysis, Stroke metabolism, Stroke pathology, Brain Ischemia drug therapy, Gene Expression Regulation drug effects, MicroRNAs biosynthesis, Neuroprotective Agents pharmacology, Oligodeoxyribonucleotides pharmacology, Stroke drug therapy

Abstract

Cytosine-phosphate-guanine (CpG) preconditioning reprograms the genomic response to stroke to protect the brain against ischemic injury. The mechanisms underlying genomic reprogramming are incompletely understood. MicroRNAs (miRNAs) regulate gene expression; however, their role in modulating gene responses produced by CpG preconditioning is unknown. We evaluated brain miRNA expression in response to CpG preconditioning before and after stroke using microarray. Importantly, we have data from previous gene microarrays under the same conditions, which allowed integration of miRNA and gene expression data to specifically identify regulated miRNA gene targets. CpG preconditioning did not significantly alter miRNA expression before stroke, indicating that miRNA regulation is not critical for the initiation of preconditioning-induced neuroprotection. However, after stroke, differentially regulated miRNAs between CpG- and saline-treated animals associated with the upregulation of several neuroprotective genes, implicating these miRNAs in genomic reprogramming that increases neuroprotection. Statistical analysis revealed that the miRNA targets were enriched in the gene population regulated in the setting of stroke, implying that miRNAs likely orchestrate this gene expression. These data suggest that miRNAs regulate endogenous responses to stroke and that manipulation of these miRNAs may have the potential to acutely activate novel neuroprotective processes that reduce damage.

Published

2015

13. Reprogramming the response to stroke by preconditioning.

Author

Stevens SL, Vartanian KB, and Stenzel-Poore MP

Subjects

Brain Ischemia physiopathology, Humans, Stroke physiopathology, Brain blood supply, Brain Ischemia therapy, Ischemic Preconditioning, Stroke therapy

Published

2014

14. Matrix effects in biological mass spectrometry imaging: identification and compensation.

Author

Lanekoff I, Stevens SL, Stenzel-Poore MP, and Laskin J

Subjects

Animals, Infarction, Middle Cerebral Artery diagnosis, Mice, Mice, Inbred C57BL, Optical Imaging methods, Phosphatidylcholines analysis, Potassium analysis, Sodium analysis, Brain blood supply, Brain pathology, Brain Chemistry, Infarction, Middle Cerebral Artery pathology, Spectrometry, Mass, Electrospray Ionization methods

Abstract

Matrix effects in mass spectrometry imaging (MSI) may affect the observed molecular distribution in chemical and biological systems. In this study, we use mouse brain tissue of a middle cerebral artery occlusion (MCAO) stroke model to examine matrix effects in nanospray desorption electrospray ionization MSI (nano-DESI MSI). This is achieved by normalizing the intensity of the sodium and potassium adducts of endogenous phosphatidylcholine (PC) species to the intensity of the corresponding adduct of the PC standard supplied at a constant rate with the nano-DESI solvent. The use of MCAO model with an ischemic region localized to one hemisphere of the brain enables immediate comparison of matrix effects within one ion image. Furthermore, significant differences in sodium and potassium concentrations in the ischemic region in comparison with the healthy tissue allowed us to distinguish between two types of matrix effects. Specifically, we discuss matrix effects originating from variations in alkali metal concentrations and matrix effects originating from variations in the molecular composition of the tissue. Compensation for both types of matrix effects was achieved by normalizing the signals corresponding to endogenous PC to the signals of the standards. This approach, which does not introduce any complexity in sample preparation, efficiently compensates for signal variations resulting from differences in the local concentrations of sodium and potassium in tissue sections and from the complexity of the extracted analyte mixture derived from local variations in molecular composition.

Published

2014

15. Toll-like receptors and ischemic brain injury.

Author

Gesuete R, Kohama SG, and Stenzel-Poore MP

Subjects

Animals, Humans, Neuroprotective Agents metabolism, Brain Ischemia metabolism, Brain Ischemia prevention & control, Signal Transduction physiology, Toll-Like Receptors metabolism

Abstract

Toll-like receptors (TLRs) are master regulators of innate immunity and play an integral role in the activation of inflammatory response during infections. In addition, TLRs influence the body's response to numerous forms of injury. Recent data have shown that TLRs play a modulating role in ischemic brain damage after stroke. Interestingly, their stimulation before ischemia induces a tolerant state that is neuroprotective. This phenomenon, referred to as TLR preconditioning, is the result of the reprogramming of TLR response to ischemic injury. This review addresses the role of TLRs in brain ischemia and the activation of endogenous neuroprotective pathways in the setting of preconditioning. We highlight the protective role of interferon-related response and the potential site of action for TLR preconditioning involving the blood-brain barrier. Pharmacologic modulation of TLR activation to promote protection against stroke is a promising approach for the development of prophylactic and immediate therapies targeting ischemic brain injury.

Published

2014

16. Steps to translate preconditioning from basic research to the clinic.

Author

Bahjat FR, Gesuete R, and Stenzel-Poore MP

Subjects

Animals, Blood-Brain Barrier physiology, Brain Ischemia therapy, Disease Models, Animal, Drug Evaluation, Preclinical, Humans, Mice, Rats, Brain Ischemia drug therapy, Ischemic Preconditioning, Neuroprotective Agents therapeutic use, Translational Research, Biomedical

Abstract

Efforts to treat cardiovascular and cerebrovascular diseases often focus on the mitigation of ischemia-reperfusion (I/R) injury. Many treatments or "preconditioners" are known to provide substantial protection against the I/R injury when administered prior to the event. Brief periods of ischemia itself have been validated as a means to achieve neuroprotection in many experimental disease settings, in multiple organ systems, and in multiple species suggesting a common pathway leading to tolerance. In addition, pharmacological agents that act as potent preconditioners have been described. Experimental induction of neuroprotection using these various preconditioning paradigms has provided a unique window into the brain's endogenous protective mechanisms. Moreover, preconditioning agents themselves hold significant promise as clinical-stage therapies for prevention of I/R injury. The aim of this article is to explore several key steps involved in the preclinical validation of preconditioning agents prior to the conduct of clinical studies in humans. Drug development is difficult, expensive and relies on multi-factorial analysis of data from diverse disciplines. Importantly, there is no single path for the preclinical development of a novel therapeutic and no proven strategy to ensure success in clinical translation. Rather, the conduct of a diverse array of robust preclinical studies reduces the risk of clinical failure by varying degrees depending upon the relevance of preclinical models and drug pharmacology to humans. A strong sense of urgency and high tolerance of failure are often required to achieve success in the development of novel treatment paradigms for complex human conditions.

Published

2013

17. TLR9 bone marrow chimeric mice define a role for cerebral TNF in neuroprotection induced by CpG preconditioning.

Author

Packard AE, Leung PY, Vartanian KB, Stevens SL, Bahjat FR, and Stenzel-Poore MP

Subjects

Animals, Brain Injuries genetics, Brain Injuries metabolism, Brain Injuries physiopathology, Brain Ischemia genetics, Brain Ischemia pathology, Hematopoietic Stem Cells metabolism, Hematopoietic Stem Cells pathology, Mice, Mice, Knockout, Toll-Like Receptor 9 genetics, Transplantation Chimera genetics, Transplantation, Homologous, Tumor Necrosis Factor-alpha genetics, Adjuvants, Immunologic pharmacology, Bone Marrow Transplantation, Brain Ischemia metabolism, Oligodeoxyribonucleotides pharmacology, Toll-Like Receptor 9 biosynthesis, Transplantation Chimera metabolism, Tumor Necrosis Factor-alpha metabolism

Abstract

Systemic preconditioning with the TLR9 ligand CpG induces neuroprotection against brain ischemic injury through a tumor necrosis factor (TNF)-dependent mechanism. It is unclear how systemic administration of CpG engages the brain to induce the protective phenotype. To address this, we created TLR9-deficient reciprocal bone marrow chimeric mice lacking TLR9 on either hematopoietic cells or radiation-resistant cells of nonhematopoietic origin. We report that wild-type mice reconstituted with TLR9-deficient hematopoietic cells failed to show neuroprotection after systemic CpG preconditioning. Further, while hematopoietic expression of TLR9 is required for CpG-induced neuroprotection it is not sufficient to restore protection to TLR9-deficient mice that are reconstituted with hematopoietic cells bearing TLR9. To determine whether the absence of protection was associated with TNF, we examined TNF levels in the systemic circulation and the brain. We found that although TNF is required for CpG preconditioning, systemic TNF levels did not correlate with the protective phenotype. However, induction of cerebral TNF mRNA required expression of TLR9 on both hematopoietic and nonhematopoietic cells and correlated with neuroprotection. In accordance with these results, we show the therapeutic potential of intranasal CpG preconditioning, which induces brain TNF mRNA and robust neuroprotection with no concomitant increase in systemic levels of TNF.

Published

2012

18. Poly-ICLC preconditioning protects the blood-brain barrier against ischemic injury in vitro through type I interferon signaling.

Author

Gesuete R, Packard AE, Vartanian KB, Conrad VK, Stevens SL, Bahjat FR, Yang T, and Stenzel-Poore MP

Subjects

Analysis of Variance, Animals, Animals, Newborn, Blood-Brain Barrier metabolism, Brain Infarction drug therapy, Brain Infarction etiology, Carboxymethylcellulose Sodium administration & dosage, Carboxymethylcellulose Sodium pharmacology, Cells, Cultured, Disease Models, Animal, Enzyme-Linked Immunosorbent Assay methods, Gene Expression Regulation drug effects, Gene Expression Regulation genetics, Glucose deficiency, Hypoxia drug therapy, Hypoxia metabolism, Infarction, Middle Cerebral Artery complications, Infarction, Middle Cerebral Artery genetics, Interferon Regulatory Factor-1 deficiency, Interferon-beta genetics, Interferon-beta metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Neuroglia drug effects, Poly I-C pharmacology, Polylysine administration & dosage, Polylysine pharmacology, RNA, Messenger metabolism, Tight Junctions drug effects, Tight Junctions pathology, Time Factors, Blood-Brain Barrier drug effects, Carboxymethylcellulose Sodium analogs & derivatives, Infarction, Middle Cerebral Artery prevention & control, Interferon Regulatory Factor-1 metabolism, Ischemic Preconditioning methods, Neuroprotective Agents administration & dosage, Poly I-C administration & dosage, Polylysine analogs & derivatives, Signal Transduction drug effects

Abstract

Preconditioning with a low dose of harmful stimulus prior to injury induces tolerance to a subsequent ischemic challenge resulting in neuroprotection against stroke. Experimental models of preconditioning primarily focus on neurons as the cellular target of cerebral protection, while less attention has been paid to the cerebrovascular compartment, whose role in the pathogenesis of ischemic brain injury is crucial. We have shown that preconditioning with polyinosinic polycytidylic acid (poly-ICLC) protects against cerebral ischemic damage. To delineate the mechanism of poly-ICLC protection, we investigated whether poly-ICLC preconditioning preserves the function of the blood-brain barrier (BBB) in response to ischemic injury. Using an in vitro BBB model, we found that poly-ICLC treatment prior to exposure to oxygen-glucose deprivation maintained the paracellular and transcellular transport across the endothelium and attenuated the drop in transendothelial electric resistance. We found that poly-ICLC treatment induced interferon (IFN) β mRNA expression in astrocytes and microglia and that type I IFN signaling in brain microvascular endothelial cells was required for protection. Importantly, this implicates a potential mechanism underlying neuroprotection in our in vivo experimental stroke model, where type I IFN signaling is required for poly-ICLC-induced neuroprotection against ischemic injury. In conclusion, we are the first to show that preconditioning with poly-ICLC attenuates ischemia-induced BBB dysfunction. This mechanism is likely an important feature of poly-ICLC-mediated neuroprotection and highlights the therapeutic potential of targeting BBB signaling pathways to protect the brain against stroke., (© 2012 The Authors Journal of Neurochemistry © International Society for Neurochemistry.)

Published

2012

19. Toll-like receptor 7 preconditioning induces robust neuroprotection against stroke by a novel type I interferon-mediated mechanism.

Author

Leung PY, Stevens SL, Packard AE, Lessov NS, Yang T, Conrad VK, van den Dungen NN, Simon RP, and Stenzel-Poore MP

Subjects

Animals, Brain Infarction pathology, Interferon Regulatory Factor-7 deficiency, Interferon Regulatory Factor-7 genetics, Interferon Regulatory Factor-7 physiology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Models, Animal, Receptor, Interferon alpha-beta deficiency, Receptor, Interferon alpha-beta genetics, Signal Transduction physiology, Stroke physiopathology, Tumor Necrosis Factor-alpha deficiency, Tumor Necrosis Factor-alpha genetics, Tumor Necrosis Factor-alpha physiology, Aminoquinolines therapeutic use, Brain blood supply, Imidazoles therapeutic use, Ischemic Preconditioning methods, Membrane Glycoproteins agonists, Neuroprotective Agents therapeutic use, Receptor, Interferon alpha-beta physiology, Stroke prevention & control, Toll-Like Receptor 7 agonists

Abstract

Background and Purpose: Systemic administration of Toll-like receptor (TLR) 4 and TLR9 agonists before cerebral ischemia have been shown to reduce ischemic injury by reprogramming the response of the brain to stroke. Our goal was to explore the mechanism of TLR-induced neuroprotection by determining whether a TLR7 agonist also protects against stroke injury., Methods: C57Bl/6, TNF(-/-), interferon (IFN) regulatory factor 7(-/-), or type I IFN receptor (IFNAR)(-/-) mice were subcutaneously administered the TLR7 agonist Gardiquimod (GDQ) 72 hours before middle cerebral artery occlusion. Infarct volume and functional outcome were determined after reperfusion. Plasma cytokine responses and induction of mRNA for IFN-related genes in the brain were measured. IFNAR(-/-) mice also were treated with the TLR4 agonist (lipopolysaccharide) or the TLR9 agonist before middle cerebral artery occlusion and infarct volumes measured., Results: The results show that GDQ reduces infarct volume as well as functional deficits in mice. GDQ pretreatment provided robust neuroprotection in TNF(-/-) mice, indicating that TNF was not essential. GDQ induced a significant increase in plasma IFNα levels and both IRF7(-/-) and IFNAR(-/-) mice failed to be protected, implicating a role for IFN signaling in TLR7-mediated protection., Conclusions: Our studies provide the first evidence that TLR7 preconditioning can mediate neuroprotection against ischemic injury. Moreover, we show that the mechanism of protection is unique from other TLR preconditioning ligands in that it is independent of TNF and dependent on IFNAR.

Published

2012

20. Poly-IC preconditioning protects against cerebral and renal ischemia-reperfusion injury.

Author

Packard AE, Hedges JC, Bahjat FR, Stevens SL, Conlin MJ, Salazar AM, and Stenzel-Poore MP

Subjects

Animals, Brain drug effects, Brain physiopathology, Brain Ischemia physiopathology, Cells, Cultured, Cytokines blood, Kidney drug effects, Kidney physiopathology, Kidney Diseases physiopathology, Male, Mice, Mice, Inbred C57BL, Neuroprotective Agents therapeutic use, Reperfusion Injury physiopathology, Brain Ischemia prevention & control, Interferon Inducers therapeutic use, Ischemic Preconditioning methods, Kidney Diseases prevention & control, Poly I-C therapeutic use, Reperfusion Injury prevention & control

Abstract

Preconditioning induces ischemic tolerance, which confers robust protection against ischemic damage. We show marked protection with polyinosinic polycytidylic acid (poly-IC) preconditioning in three models of murine ischemia-reperfusion injury. Poly-IC preconditioning induced protection against ischemia modeled in vitro in brain cortical cells and in vivo in models of brain ischemia and renal ischemia. Further, unlike other Toll-like receptor (TLR) ligands, which generally induce significant inflammatory responses, poly-IC elicits only modest systemic inflammation. Results show that poly-IC is a new powerful prophylactic treatment that offers promise as a clinical therapeutic strategy to minimize damage in patient populations at risk of ischemic injury.

Published

2012

21. Corticotropin-releasing factor acting on corticotropin-releasing factor receptor type 1 is critical for binge alcohol drinking in mice.

Author

Kaur S, Li J, Stenzel-Poore MP, and Ryabinin AE

Subjects

Animals, Central Nervous System Depressants blood, Ethanol blood, Female, Gene Deletion, Ligands, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Sucrose, Urocortins genetics, Alcoholism genetics, Alcoholism psychology, Corticotropin-Releasing Hormone genetics, Receptors, Corticotropin-Releasing Hormone genetics

Abstract

Background: The corticotropin-releasing factor (CRF) system has been implicated in the regulation of alcohol consumption. However, previous mouse knockout (KO) studies using continuous ethanol access have failed to conclusively confirm this. Recent studies have shown that CRF receptor type 1 (CRFR1) antagonists attenuate alcohol intake in the limited access "drinking in the dark" (DID) model of binge drinking. To avoid the potential nonspecific effects of antagonists, in this study, we tested alcohol drinking in CRFR1, CRFR2, CRF, and urocortin 1 (Ucn1) KO and corresponding wild-type (WT) littermates using the DID paradigm., Methods: On days 1 to 3, the CRFR1, CRFR2, Ucn1, and CRF KO mice and their respective WT littermates were provided with 20% ethanol or 10% sucrose for 2 hours with water available at all other times. On day 4, access to ethanol or sucrose was increased to 4 hours. At the end of each drinking session, the volume of ethanol consumed was recorded, and at the conclusion of the last session, blood was also collected for blood ethanol concentration (BEC) analysis., Results: CRFR1 KO mice had lower alcohol intakes and BECs and higher intakes of sucrose compared with WTs. In contrast, CRFR2 KO mice, while having reduced intakes initially, had similar alcohol intakes on days 2 to 4 and similar BECs as the WTs. To determine the ligand responsible, Ucn1 and CRF KO and WT mice were tested next. While Ucn1 KOs had similar alcohol intakes and BECs to their WTs, CRF KO mice showed reduced alcohol consumption and lower BECs compared with WTs., Conclusions: Our results confirm that CRFR1 plays a key role in binge drinking and identify CRF as the ligand critically involved in excessive alcohol consumption., (Copyright © 2011 by the Research Society on Alcoholism.)

Published

2012

22. Dissociation of corticotropin-releasing factor receptor subtype involvement in sensitivity to locomotor effects of methamphetamine and cocaine.

Author

Giardino WJ, Mark GP, Stenzel-Poore MP, and Ryabinin AE

Subjects

Aminopyridines pharmacology, Animals, Cocaine administration & dosage, Female, Gene Deletion, Male, Methamphetamine administration & dosage, Mice, Mice, Inbred C57BL, Mice, Knockout, Motor Activity drug effects, Receptors, Corticotropin-Releasing Hormone genetics, Cocaine pharmacology, Methamphetamine pharmacology, Receptors, Corticotropin-Releasing Hormone metabolism

Abstract

Rationale: Enhanced sensitivity to the euphoric and locomotor-activating effects of psychostimulants may influence an individual's predisposition to drug abuse and addiction. While drug-induced behaviors are mediated by the actions of several neurotransmitter systems, past research revealed that the corticotropin-releasing factor (CRF) system is important in driving the acute locomotor response to psychostimulants., Objectives: We previously reported that genetic deletion of the CRF type-2 receptor (CRF-R2), but not the CRF type-1 receptor (CRF-R1) dampened the acute locomotor stimulant response to methamphetamine (1 mg/kg). These results contrasted with previous studies implicating CRF-R1 in the locomotor effects of psychostimulants. Since the majority of previous studies focused on cocaine, rather than methamphetamine, we set out to test the hypothesis that these drugs differentially engage CRF-R1 and CRF-R2., Methods: We expanded our earlier findings by first replicating our previous experiments at a higher dose of methamphetamine (2 mg/kg), and by assessing the effects of the CRF-R1-selective antagonist CP-376,395 (10 mg/kg) on methamphetamine-induced locomotor activity. Next, we used both genetic and pharmacological tools to examine the specific components of the CRF system underlying the acute locomotor response to cocaine (5-10 mg/kg)., Results: While genetic deletion of CRF-R2 dampened the locomotor response to methamphetamine (but not cocaine), genetic deletion and pharmacological blockade of CRF-R1 dampened the locomotor response to cocaine (but not methamphetamine)., Conclusions: These findings highlight the differential involvement of CRF receptors in acute sensitivity to two different stimulant drugs of abuse, providing an intriguing basis for the development of more targeted therapeutics for psychostimulant addiction.

Published

2012

23. Modeling dynamic regulatory processes in stroke.

Author

McDermott JE, Jarman K, Taylor R, Lancaster M, Shankaran H, Vartanian KB, Stevens SL, Stenzel-Poore MP, and Sanfilippo A

Subjects

Algorithms, Animals, Brain Ischemia genetics, Brain Ischemia metabolism, Computer Simulation, Gene Expression Profiling, Gene Expression Regulation, Mice, Mice, Inbred C57BL, Multigene Family, Reproducibility of Results, Gene Regulatory Networks, Models, Genetic, Stroke genetics, Stroke metabolism, Transcriptome

Abstract

The ability to examine the behavior of biological systems in silico has the potential to greatly accelerate the pace of discovery in diseases, such as stroke, where in vivo analysis is time intensive and costly. In this paper we describe an approach for in silico examination of responses of the blood transcriptome to neuroprotective agents and subsequent stroke through the development of dynamic models of the regulatory processes observed in the experimental gene expression data. First, we identified functional gene clusters from these data. Next, we derived ordinary differential equations (ODEs) from the data relating these functional clusters to each other in terms of their regulatory influence on one another. Dynamic models were developed by coupling these ODEs into a model that simulates the expression of regulated functional clusters. By changing the magnitude of gene expression in the initial input state it was possible to assess the behavior of the networks through time under varying conditions since the dynamic model only requires an initial starting state, and does not require measurement of regulatory influences at each time point in order to make accurate predictions. We discuss the implications of our models on neuroprotection in stroke, explore the limitations of the approach, and report that an optimized dynamic model can provide accurate predictions of overall system behavior under several different neuroprotective paradigms.

Published

2012

24. Identification and validation of Ifit1 as an important innate immune bottleneck.

Author

McDermott JE, Vartanian KB, Mitchell H, Stevens SL, Sanfilippo A, and Stenzel-Poore MP

Subjects

Adaptor Proteins, Signal Transducing, Animals, Carrier Proteins genetics, Cell Line, Immunity, Innate drug effects, Immunity, Innate genetics, Lipopolysaccharides pharmacology, Macrophages drug effects, Macrophages metabolism, Mice, RNA-Binding Proteins, Reverse Transcriptase Polymerase Chain Reaction, Toll-Like Receptors genetics, Toll-Like Receptors metabolism, Carrier Proteins metabolism, Immunity, Innate immunology

Abstract

The innate immune system plays important roles in a number of disparate processes. Foremost, innate immunity is a first responder to invasion by pathogens and triggers early defensive responses and recruits the adaptive immune system. The innate immune system also responds to endogenous damage signals that arise from tissue injury. Recently it has been found that innate immunity plays an important role in neuroprotection against ischemic stroke through the activation of the primary innate immune receptors, Toll-like receptors (TLRs). Using several large-scale transcriptomic data sets from mouse and mouse macrophage studies we identified targets predicted to be important in controlling innate immune processes initiated by TLR activation. Targets were identified as genes with high betweenness centrality, so-called bottlenecks, in networks inferred from statistical associations between gene expression patterns. A small set of putative bottlenecks were identified in each of the data sets investigated including interferon-stimulated genes (Ifit1, Ifi47, Tgtp and Oasl2) as well as genes uncharacterized in immune responses (Axud1 and Ppp1r15a). We further validated one of these targets, Ifit1, in mouse macrophages by showing that silencing it suppresses induction of predicted downstream genes by lipopolysaccharide (LPS)-mediated TLR4 activation through an unknown direct or indirect mechanism. Our study demonstrates the utility of network analysis for identification of interesting targets related to innate immune function, and highlights that Ifit1 can exert a positive regulatory effect on downstream genes.

Published

2012

25. Ethanol concentration-dependent effects and the role of stress on ethanol drinking in corticotropin-releasing factor type 1 and double type 1 and 2 receptor knockout mice.

Author

Pastor R, Reed C, Burkhart-Kasch S, Li N, Sharpe AL, Coste SC, Stenzel-Poore MP, and Phillips TJ

Subjects

Alcohol Drinking epidemiology, Alcohol Drinking genetics, Animals, Disease Models, Animal, Dose-Response Relationship, Drug, Female, Genotype, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Quinine administration & dosage, Saccharin administration & dosage, Stress, Psychological genetics, Swimming, Time, Ethanol administration & dosage, Receptors, Corticotropin-Releasing Hormone genetics, Stress, Psychological complications

Abstract

Rationale: Exposure to stressors promotes ethanol (EtOH) consumption and enhances drug craving during abstinence. Corticotropin-releasing factor (CRF), and in particular, CRF actions via type 1 CRF receptors (CRF(1)) are critical in behavioral responses to stressors. CRF(1) play a role in EtOH-induced behavioral neuroadaptation, in binge-like EtOH consumption, and in heightened EtOH consumption in dependent animals., Objectives: We investigated the involvement of CRF(1) in swim-stress-induced changes in EtOH consumption and in baseline consumption as a function of EtOH concentration. The role of CRF(2) in adapting to effects of the stressor was also examined., Methods: Wild-type mice and knockout mice lacking CRF(1) were tested for two-bottle choice EtOH consumption at concentrations of 3-20%. Also, intake of 10% EtOH was examined in wild-type mice and knockout mice lacking CRF(1), or lacking both CRF(1) and CRF(2), before and after acute or repeated swim stress exposures., Results: EtOH intake was reduced in CRF(1) compared with wild-type mice when presented at a concentration of 20% but not when presented at lower concentrations. No genotype-dependent effects were found for saccharin or quinine drinking. Acute swim stress had no effect, but repeated swim stress resulted in higher levels of EtOH consumption in wild-type mice, compared with both types of knockout mice. Stress effects on EtOH drinking were longer lasting in double knockout mice., Conclusions: These data suggest a prominent role of CRF(1) in stressor-induced changes in EtOH consumption, with involvement of CRF(2) in recovery from stressor effects.

Published

2011

26. LPS preconditioning redirects TLR signaling following stroke: TRIF-IRF3 plays a seminal role in mediating tolerance to ischemic injury.

Author

Vartanian KB, Stevens SL, Marsh BJ, Williams-Karnesky R, Lessov NS, and Stenzel-Poore MP

Subjects

Adaptor Proteins, Vesicular Transport genetics, Animals, Chemokines blood, Chemokines immunology, Cytokines blood, Cytokines immunology, Gene Expression Profiling, Humans, Infarction, Middle Cerebral Artery, Interferon Regulatory Factor-3 genetics, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Microarray Analysis, NF-kappa B immunology, Adaptor Proteins, Vesicular Transport immunology, Brain Ischemia blood, Brain Ischemia immunology, Brain Ischemia pathology, Interferon Regulatory Factor-3 immunology, Ischemic Preconditioning, Lipopolysaccharides pharmacology, Signal Transduction drug effects, Signal Transduction immunology, Stroke blood, Stroke immunology, Stroke pathology, Toll-Like Receptor 4 immunology

Abstract

Background: Toll-like receptor 4 (TLR4) is activated in response to cerebral ischemia leading to substantial brain damage. In contrast, mild activation of TLR4 by preconditioning with low dose exposure to lipopolysaccharide (LPS) prior to cerebral ischemia dramatically improves outcome by reprogramming the signaling response to injury. This suggests that TLR4 signaling can be altered to induce an endogenously neuroprotective phenotype. However, the TLR4 signaling events involved in this neuroprotective response are poorly understood. Here we define several molecular mediators of the primary signaling cascades induced by LPS preconditioning that give rise to the reprogrammed response to cerebral ischemia and confer the neuroprotective phenotype., Methods: C57BL6 mice were preconditioned with low dose LPS prior to transient middle cerebral artery occlusion (MCAO). Cortical tissue and blood were collected following MCAO. Microarray and qtPCR were performed to analyze gene expression associated with TLR4 signaling. EMSA and DNA binding ELISA were used to evaluate NFκB and IRF3 activity. Protein expression was determined using Western blot or ELISA. MyD88-/- and TRIF-/- mice were utilized to evaluate signaling in LPS preconditioning-induced neuroprotection., Results: Gene expression analyses revealed that LPS preconditioning resulted in a marked upregulation of anti-inflammatory/type I IFN-associated genes following ischemia while pro-inflammatory genes induced following ischemia were present but not differentially modulated by LPS. Interestingly, although expression of pro-inflammatory genes was observed, there was decreased activity of NFκB p65 and increased presence of NFκB inhibitors, including Ship1, Tollip, and p105, in LPS-preconditioned mice following stroke. In contrast, IRF3 activity was enhanced in LPS-preconditioned mice following stroke. TRIF and MyD88 deficient mice revealed that neuroprotection induced by LPS depends on TLR4 signaling via TRIF, which activates IRF3, but does not depend on MyD88 signaling., Conclusion: Our results characterize several critical mediators of the TLR4 signaling events associated with neuroprotection. LPS preconditioning redirects TLR4 signaling in response to stroke through suppression of NFκB activity, enhanced IRF3 activity, and increased anti-inflammatory/type I IFN gene expression. Interestingly, this protective phenotype does not require the suppression of pro-inflammatory mediators. Furthermore, our results highlight a critical role for TRIF-IRF3 signaling as the governing mechanism in the neuroprotective response to stroke.

Published

2011

27. Multiple preconditioning paradigms converge on interferon regulatory factor-dependent signaling to promote tolerance to ischemic brain injury.

Author

Stevens SL, Leung PY, Vartanian KB, Gopalan B, Yang T, Simon RP, and Stenzel-Poore MP

Subjects

Animals, Brain blood supply, Brain drug effects, Brain Ischemia genetics, Gene Expression drug effects, Interferon Regulatory Factors genetics, Lipopolysaccharides immunology, Male, Mice, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction drug effects, Signal Transduction immunology, Toll-Like Receptors genetics, Brain immunology, Brain Ischemia immunology, Interferon Regulatory Factors immunology, Ischemic Preconditioning methods, Lipopolysaccharides pharmacology, Toll-Like Receptors immunology

Abstract

Ischemic tolerance can be induced by numerous preconditioning stimuli, including various Toll-like receptor (TLR) ligands. We have shown previously that systemic administration of the TLR4 ligand LPS or the TLR9 ligand unmethylated CpG oligodeoxynucleotide before transient brain ischemia in mice confers substantial protection against ischemic damage. To elucidate the molecular mechanisms of preconditioning, we compared brain genomic profiles in response to preconditioning with these TLR ligands and with preconditioning via exposure to brief ischemia. We found that exposure to the TLR ligands and brief ischemia induced genomic changes in the brain characteristic of a TLR pathway-mediated response. Interestingly, all three preconditioning stimuli resulted in a reprogrammed response to stroke injury that converged on a shared subset of 13 genes not evident in the genomic profile from brains that were subjected to stroke without prior preconditioning. Analysis of the promoter region of these shared genes showed sequences required for interferon regulatory factor (IRF)-mediated transcription. The importance of this IRF gene network was tested using mice deficient in IRF3 or IRF7. Our data show that both transcription factors are required for TLR-mediated preconditioning and neuroprotection. These studies are the first to discover a convergent mechanism of neuroprotection induced by preconditioning--one that potentially results in reprogramming of the TLR-mediated response to stroke and requires the presence of IRF3 and IRF7.

Published

2011

28. Proof of concept: pharmacological preconditioning with a Toll-like receptor agonist protects against cerebrovascular injury in a primate model of stroke.

Author

Bahjat FR, Williams-Karnesky RL, Kohama SG, West GA, Doyle KP, Spector MD, Hobbs TR, and Stenzel-Poore MP

Subjects

Animals, DNA therapeutic use, Disease Models, Animal, Macaca mulatta, Male, Mice, Mice, Inbred C57BL, Recovery of Function drug effects, Stroke pathology, Ischemic Preconditioning methods, Oligodeoxyribonucleotides therapeutic use, Stroke prevention & control, Toll-Like Receptors agonists

Abstract

Cerebral ischemic injury is a significant portion of the burden of disease in developed countries; rates of mortality are high and the costs associated with morbidity are enormous. Recent therapeutic approaches have aimed at mitigating the extent of damage and/or promoting repair once injury has occurred. Often, patients at high risk of ischemic injury can be identified in advance and targeted for antecedent neuroprotective therapy. Agents that stimulate the innate pattern recognition receptor, Toll-like receptor 9, have been shown to induce tolerance (precondition) to ischemic brain injury in a mouse model of stroke. Here, we demonstrate for the first time that pharmacological preconditioning against cerebrovascular ischemic injury is also possible in a nonhuman primate model of stroke in the rhesus macaque. The model of stroke used is a minimally invasive transient vascular occlusion, resulting in brain damage that is primarily localized to the cortex and as such, represents a model with substantial clinical relevance. Finally, K-type (also referred to as B-type) cytosine-guanine-rich DNA oligonucleotides, the class of agents employed in this study, are currently in use in human clinical trials, underscoring the feasibility of this treatment in patients at risk of cerebral ischemia.

Published

2011

29. CRF receptor antagonist astressin-B reverses and prevents alopecia in CRF over-expressing mice.

Author

Wang L, Million M, Rivier J, Rivier C, Craft N, Stenzel-Poore MP, and Taché Y

Subjects

Alopecia genetics, Animals, Corticotropin-Releasing Hormone administration & dosage, Corticotropin-Releasing Hormone pharmacology, Corticotropin-Releasing Hormone therapeutic use, Drug Evaluation, Preclinical, Female, Hair drug effects, Hair growth & development, Hormone Antagonists administration & dosage, Hormone Antagonists pharmacology, Hormone Antagonists therapeutic use, Injections, Intraperitoneal, Injections, Subcutaneous, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Peptide Fragments administration & dosage, Receptors, Corticotropin-Releasing Hormone antagonists & inhibitors, Up-Regulation, Alopecia drug therapy, Alopecia prevention & control, Corticotropin-Releasing Hormone genetics, Peptide Fragments pharmacology, Peptide Fragments therapeutic use

Abstract

Corticotropin-releasing factor (CRF) signaling pathways are involved in the stress response, and there is growing evidence supporting hair growth inhibition of murine hair follicle in vivo upon stress exposure. We investigated whether the blockade of CRF receptors influences the development of hair loss in CRF over-expressing (OE)-mice that display phenotypes of Cushing's syndrome and chronic stress, including alopecia. The non-selective CRF receptors antagonist, astressin-B (5 µg/mouse) injected peripherally once a day for 5 days in 4-9 months old CRF-OE alopecic mice induced pigmentation and hair re-growth that was largely retained for over 4 months. In young CRF-OE mice, astressin-B prevented the development of alopecia that occurred in saline-treated mice. Histological examination indicated that alopecic CRF-OE mice had hair follicle atrophy and that astressin-B revived the hair follicle from the telogen to anagen phase. However, astressin-B did not show any effect on the elevated plasma corticosterone levels and the increased weights of adrenal glands and visceral fat in CRF-OE mice. The selective CRF₂ receptor antagonist, astressin₂-B had moderate effect on pigmentation, but not on hair re-growth. The commercial drug for alopecia, minoxidil only showed partial effect on hair re-growth. These data support the existence of a key molecular switching mechanism triggered by blocking peripheral CRF receptors with an antagonist to reset hair growth in a mouse model of alopecia associated with chronic stress.

Published

2011

30. Dissection of corticotropin-releasing factor system involvement in locomotor sensitivity to methamphetamine.

Author

Giardino WJ, Pastor R, Anacker AM, Spangler E, Cote DM, Li J, Stenzel-Poore MP, Phillips TJ, and Ryabinin AE

Subjects

Animals, Corticotropin-Releasing Hormone genetics, Female, Gene Deletion, Immunohistochemistry, Male, Mice, Mice, Inbred DBA, Mice, Knockout, Mutation genetics, Mutation physiology, Proto-Oncogene Proteins c-fos metabolism, Receptors, Corticotropin-Releasing Hormone antagonists & inhibitors, Receptors, Corticotropin-Releasing Hormone genetics, Urocortins genetics, Central Nervous System Stimulants pharmacology, Corticotropin-Releasing Hormone physiology, Methamphetamine pharmacology, Motor Activity drug effects, Motor Activity physiology

Abstract

Sensitivity to the euphoric and locomotor-activating effects of drugs of abuse may contribute to risk for excessive use and addiction. Repeated administration of psychostimulants such as methamphetamine (MA) can result in neuroadaptive consequences that manifest behaviorally as a progressive escalation of locomotor activation, termed psychomotor sensitization. The present studies addressed the involvement of specific components of the corticotropin-releasing factor (CRF) system in locomotor activation and psychomotor sensitization induced by MA (1, 2 mg/kg) by utilizing pharmacological approaches, as well as a series of genetic knockout (KO) mice, each deficient for a single component of the CRF system: CRF-R1, CRF-R2, CRF, or the CRF-related peptide Urocortin 1 (Ucn1). CRF-R1 KO mice did not differ from wild-type mice in sensitization to MA, and pharmacological blockade of CRF-R1 with CP-154,526 (15, 30 mg/kg) in DBA/2J mice did not selectively attenuate either the acquisition or expression of MA-induced sensitization. Deletion of either of the endogenous ligands of CRF-R1 (CRF, Ucn1) either enhanced or had no effect on MA-induced sensitization, providing further evidence against a role for CRF-R1 signaling. Interestingly, deletion of CRF-R2 attenuated MA-induced locomotor activation, elucidating a novel contribution of the CRF system to MA sensitivity, and suggesting the participation of the endogenous urocortin peptides Ucn2 and Ucn3. Immunohistochemistry for Fos was used to visualize neural activation underlying CRF-R2-dependent sensitivity to MA, identifying the basolateral and central nuclei of the amygdala as neural substrates involved in this response. Our results support further examination of CRF-R2 involvement in neural processes associated with MA addiction., (© 2010 The Authors. Genes, Brain and Behavior © 2010 Blackwell Publishing Ltd and International Behavioural and Neural Genetics Society.)

Published

2011

31. Corticotropin-releasing hormone (CRH) transgenic mice display hyperphagia with increased Agouti-related protein mRNA in the hypothalamic arcuate nucleus.

Author

Nakayama S, Nishiyama M, Iwasaki Y, Shinahara M, Okada Y, Tsuda M, Okazaki M, Tsugita M, Taguchi T, Makino S, Stenzel-Poore MP, Hashimoto K, and Terada Y

Subjects

Adipose Tissue metabolism, Animals, Body Weight genetics, Corticosterone blood, Cushing Syndrome physiopathology, Disease Models, Animal, Eating drug effects, Eating genetics, Male, Mice, Mice, Transgenic, Neuropeptide Y metabolism, Pro-Opiomelanocortin metabolism, RNA, Messenger metabolism, Agouti-Related Protein genetics, Arcuate Nucleus of Hypothalamus metabolism, Corticotropin-Releasing Hormone genetics, Glucocorticoids pharmacology, Hyperphagia chemically induced

Abstract

Although glucocorticoid-induced hyperphagia is observed in the patients with glucocorticoid treatment or Cushing's syndrome, its molecular mechanism is not clear. We thus explored the expression of neuropeptide mRNAs in the hypothalamus related to appetite regulation in CRH over-expressing transgenic mice (CRH-Tg), a model of Cushing's syndrome. We measured food intake, body weight (including body fat weight) and plasma corticosterone levels in CRH-Tg and their wild-type littermates (WT) at 6 and 14 weeks old. We also examined neuropeptide Y (NPY), proopiomelanocortin (POMC) and Agouti-related protein (AgRP) mRNAs in the arcuate nucleus (ARC) using in situ hybridization. Circulating corticosterone levels in CRH-Tg were markedly elevated at both 6 and 14 weeks old. Body fat weight in CRH-Tg was significantly increased at 14 weeks old, which is considered as an effect of chronic glucocorticoid excess. At both 6 and 14 weeks old, CRH-Tg mice showed significant hyperphagia compared with WT (14w old: WT 3.9±0.1, CRH-Tg 5.1±0.7 g/day, p<0.05). Unexpectedly, NPY mRNA levels in CRH-Tg were significantly decreased at 14 weeks old (WT: 1571.5±111.2, CRH-Tg: 949.1±139.3 dpm/mg, p<0.05), and there were no differences in POMC mRNA levels between CRH-Tg and WT. On the other hand, AgRP mRNA levels in CRH-Tg were significantly increased compared with WT at both ages (14w old: WT 365.6±88.6, CRH-Tg 660.1±87.2 dpm/ mg, p<0.05). These results suggest that glucocorticoid-induced hyperphagia is associated with increased hypothalamic AgRP. Our results also indicate that hypothalamic NPY does not have an essential role in the increased food intake during glucocorticoid excess.

Published

2011

32. Defining the players in higher-order networks: predictive modeling for reverse engineering functional influence networks.

Author

McDermott JE, Archuleta M, Stevens SL, Stenzel-Poore MP, and Sanfilippo A

Subjects

Algorithms, Animals, Artificial Intelligence, Biomedical Engineering, Computational Biology, Disease Models, Animal, Mice, Oligonucleotide Array Sequence Analysis statistics & numerical data, Stroke genetics, Stroke prevention & control, Systems Biology statistics & numerical data, Gene Expression Profiling statistics & numerical data, Gene Regulatory Networks, Models, Genetic

Abstract

Determining biological network dependencies that can help predict the behavior of a system given prior observations from high-throughput data is a very valuable but difficult task, especially in the light of the ever-increasing volume of experimental data. Such an endeavor can be greatly enhanced by considering regulatory influences on co-expressed groups of genes representing functional modules, thus constraining the number of parameters in the system. This allows development of network models that are predictive of system dynamics. We first develop a predictive network model of the transcriptomics of whole blood from a mouse model of neuroprotection in ischemic stroke, and show that it can accurately predict system behavior under novel conditions. We then use a network topology approach to expand the set of regulators considered and show that addition of topological bottlenecks improves the performance of the predictive model. Finally, we explore how improvements in definition of functional modules may be achieved through an integration of inferred network relationships and functional relationships defined using Gene Ontology similarity. We show that appropriate integration of these two types of relationships can result in models with improved performance.

Published

2011

33. Toll-like receptor tolerance as a mechanism for neuroprotection.

Author

Vartanian K and Stenzel-Poore M

Abstract

It has been discovered recently that toll-like receptors (TLRs) are key mediators of tissue injury in response to stroke. This revelation has identified a new target critical to understanding the underlying mechanisms of stroke injury and potential therapies. Much of the interest in TLRs centers around their ability to self regulate - a process commonly referred to as "tolerance," wherein prior exposure to low level TLR activation induces protection against a subsequent challenge that would otherwise cause damage. This endogenous process has been exploited in the setting of stroke. Recent studies show that TLR pathways can be reprogrammed via prior exposure to TLR ligands leading to decreased infarct size and improved neurological outcomes in response to ischemic injury. Efforts to understand the molecular mechanisms of TLR reprogramming have led to the identification of multiple routes of TLR regulation including inhibitors that target signaling mediators, microRNAs that suppress genes post-transcriptionally, and epigenetic changes in chromatin remodeling that affect global gene regulation. In this review, we discuss the role of TLRs in mediating injury due to stroke, evidence for TLR preconditioning-induced TLR reprogramming in response to stroke, and possible mechanisms of TLR-induced neuroprotection.

Published

2010

34. Adenosine and stroke: maximizing the therapeutic potential of adenosine as a prophylactic and acute neuroprotectant.

Author

Williams-Karnesky RL and Stenzel-Poore MP

Abstract

Stroke is a leading cause of morbidity and mortality in the United States. Despite intensive research into the development of treatments that lessen the severity of cerebrovascular injury, no major therapies exist. Though the potential use of adenosine as a neuroprotective agent in the context of stroke has long been realized, there are currently no adenosine-based therapies for the treatment of cerebral ischemia and reperfusion. One of the major obstacles to developing adenosine-based therapies for the treatment of stroke is the prevalence of functional adenosine receptors outside the central nervous system. The activities of peripheral immune and vascular endothelial cells are particularly vulnerable to modulation via adenosine receptors. Many of the pathophysiological processes in stroke are a direct result of peripheral immune infiltration into the brain. Ischemic preconditioning, which can be induced by a number of stimuli, has emerged as a promising area of focus in the development of stroke therapeutics. Reprogramming of the brain and immune responses to adenosine signaling may be an underlying principle of tolerance to cerebral ischemia. Insight into the role of adenosine in various preconditioning paradigms may lead to new uses for adenosine as both an acute and prophylactic neuroprotectant.

Published

2009

35. Systemic lipopolysaccharide protects the brain from ischemic injury by reprogramming the response of the brain to stroke: a critical role for IRF3.

Author

Marsh B, Stevens SL, Packard AE, Gopalan B, Hunter B, Leung PY, Harrington CA, and Stenzel-Poore MP

Subjects

Animals, Brain drug effects, Brain metabolism, Cell Death drug effects, Cell Hypoxia drug effects, Gene Expression drug effects, Glucose deficiency, Interferon Regulatory Factor-3 genetics, Interferon-beta genetics, Interferon-beta metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Neurons drug effects, Neurons physiology, Oligonucleotide Array Sequence Analysis, Infarction, Middle Cerebral Artery drug therapy, Interferon Regulatory Factor-3 metabolism, Interferon-beta therapeutic use, Lipopolysaccharides administration & dosage, Neuroprotective Agents administration & dosage, Reperfusion Injury prevention & control

Abstract

Lipopolysaccharide (LPS) preconditioning provides neuroprotection against subsequent cerebral ischemic injury through activation of its receptor, Toll-like receptor 4 (TLR4). Paradoxically, TLR activation by endogenous ligands after ischemia worsens stroke damage. Here, we define a novel, protective role for TLRs after ischemia in the context of LPS preconditioning. Microarray analysis of brains collected 24 h after stroke revealed a unique set of upregulated genes in LPS-pretreated animals. Promoter analysis of the unique gene set identified an overrepresentation of type I interferon (IFN)-associated transcriptional regulatory elements. This finding suggested the presence of type I IFNs or interferon regulatory factors (IRFs), which upregulate interferon-stimulated genes. Upregulation of IFNbeta was confirmed by real-time reverse transcription-PCR. Direct administration of IFNbeta intracerebroventricularly at the time of stroke was sufficient for neuroprotection. TLR4 can induce both IFNbeta and interferon-stimulated genes through its adapter molecule Toll/interleukin receptor domain-containing adaptor-inducing IFNbeta (TRIF) and the IRF3 transcription factor. We show in oxygen glucose deprivation of cortical neurons, an in vitro model of stroke, that activation of TRIF after stroke reduces neuronal death. Furthermore, mice lacking IRF3 were not protected by LPS preconditioning in our in vivo model. Our studies constitute the first demonstration of the neuroprotective capacity of TRIF/IRF3 signaling and suggest that interferon-stimulated genes, whether induced by IFNbeta or by enhanced TLR signaling to IRF3, are a potent means of protecting the brain against ischemic damage.

Published

2009

36. CRF enhancement of GIRK channel-mediated transmission in dopamine neurons.

Author

Beckstead MJ, Gantz SC, Ford CP, Stenzel-Poore MP, Phillips PE, Mark GP, and Williams JT

Subjects

Animals, Central Nervous System Stimulants pharmacology, Corticotropin-Releasing Hormone metabolism, Female, G Protein-Coupled Inwardly-Rectifying Potassium Channels metabolism, Inhibitory Postsynaptic Potentials drug effects, Inhibitory Postsynaptic Potentials physiology, Male, Mice, Mice, Inbred C57BL, Neural Inhibition drug effects, Neural Inhibition physiology, Neurons metabolism, Receptors, Corticotropin-Releasing Hormone drug effects, Receptors, Corticotropin-Releasing Hormone metabolism, Receptors, Dopamine D2 drug effects, Receptors, Dopamine D2 metabolism, Receptors, GABA-B drug effects, Receptors, GABA-B metabolism, Recurrence, Restraint, Physical physiology, Restraint, Physical psychology, Stress, Psychological metabolism, Substance Withdrawal Syndrome metabolism, Substance Withdrawal Syndrome physiopathology, Substance-Related Disorders metabolism, Substance-Related Disorders physiopathology, Synaptic Transmission drug effects, Synaptic Transmission physiology, Ventral Tegmental Area metabolism, Corticotropin-Releasing Hormone pharmacology, G Protein-Coupled Inwardly-Rectifying Potassium Channels drug effects, Neurons drug effects, Reinforcement, Psychology, Stress, Psychological physiopathology, Ventral Tegmental Area drug effects

Abstract

Dopamine neurons in the ventral midbrain contribute to learning and memory of natural and drug-related rewards. Corticotropin-releasing factor (CRF), a stress-related peptide, is thought to be involved in aspects of relapse following drug withdrawal, but the cellular actions are poorly understood. This study investigates the action of CRF on G-protein-linked inhibitory postsynaptic currents (IPSCs) mediated by GIRK (Kir3) channels in dopamine neurons. CRF enhanced the amplitude and slowed the kinetics of IPSCs following activation of D2-dopamine and GABA(B) receptors. This action was postsynaptic and dependent on the CRF(1) receptor. The enhancement induced by CRF was attenuated by repeated in vivo exposures to psychostimulants or restraint stress. The results indicate that CRF influences dopamine- and GABA-mediated inhibition in the midbrain, suggesting implications for the chronic actions of psychostimulants and stress on dopamine-mediated behaviors.

Published

2009

37. A new model of cortical stroke in the rhesus macaque.

Author

West GA, Golshani KJ, Doyle KP, Lessov NS, Hobbs TR, Kohama SG, Pike MM, Kroenke CD, Grafe MR, Spector MD, Tobar ET, Simon RP, and Stenzel-Poore MP

Subjects

Animals, Benzoxazines, Brain Ischemia blood, Brain Ischemia surgery, Magnetic Resonance Imaging, Male, Oxazines, Brain Ischemia pathology, Disease Models, Animal, Macaca mulatta surgery

Abstract

Primate models are essential tools for translational research in stroke but are reportedly inconsistent in their ability to produce cortical infarcts of reproducible size. Here, we report a new stroke model using a transorbital, reversible, two-vessel occlusion approach in male rhesus macaques that produces consistent and reproducible cortical infarcts. The right middle cerebral artery (distal to the orbitofrontal branch) and both anterior cerebral arteries were occluded with vascular clips. Bilateral occlusion of the anterior cerebral artery was critical for reducing collateral flow to the ipsilateral cortex. Reversible ischemia was induced for 45, 60, or 90 mins (n=2/timepoint) and infarct volume and neurologic outcome were evaluated. The infarcts were located predominantly in the cortex and increased in size with extended duration of ischemia determined by T(2)-weighted magnetic resonance imaging . Infarct volume measured by 2,3,5-triphenyl tetrazolium chloride and cresyl violet staining corroborated magnetic resonance imaging results. Neurologic deficit scores worsened gradually with longer occlusion times. A subset of animals (n=5) underwent 60 mins of ischemia resulting in consistent infarct volumes primarily located to the cortex that correlated well with neurologic deficit scores. This approach offers promise for evaluating therapeutic interventions in stroke.

Published

2009

38. Inflammation and the emerging role of the toll-like receptor system in acute brain ischemia.

Author

Marsh BJ, Stevens SL, Hunter B, and Stenzel-Poore MP

Subjects

Acute Disease, Animals, Arterial Occlusive Diseases pathology, Arterial Occlusive Diseases physiopathology, Arterial Occlusive Diseases prevention & control, Brain Ischemia pathology, Cerebral Arteries metabolism, Cerebral Arteries pathology, Cerebral Arteries physiopathology, Dinucleoside Phosphates pharmacology, Disease Models, Animal, Encephalitis metabolism, Encephalitis pathology, GATA3 Transcription Factor metabolism, Interferon Type I metabolism, Killer Cells, Natural drug effects, Killer Cells, Natural metabolism, Killer Cells, Natural pathology, Male, Mice, Mice, Inbred C57BL, Stroke pathology, Stroke physiopathology, Stroke prevention & control, Brain Ischemia physiopathology, Brain Ischemia prevention & control, Encephalitis physiopathology, Ischemic Preconditioning, Toll-Like Receptors physiology

Abstract

Background and Purpose: Systemic administration of cytosine-guanine (CpG) oligodeoxynucleotides provides neuroprotection against subsequent cerebral ischemic injury. We examined the genomic response of leukocytes and brain cells after ischemia in the context of CpG preconditioning., Methods: RNA was isolated from circulating leukocytes and ischemic cortex 3 and 24 hours after middle cerebral artery occlusion after CpG or saline pretreatment and subjected to microarray analysis. Genes uniquely upregulated in CpG-pretreated mice were examined for overrepresented transcriptional regulatory elements., Results: CpG preconditioning induced a novel response to middle cerebral artery occlusion within circulating leukocytes that was dominated by natural killer cell-associated genes and the GATA-3 transcriptional regulatory element. Preconditioning also caused a novel brain response to stroke that was dominated by Type I interferon, interferon-associated genes, and transcriptional regulatory elements., Conclusions: CpG preconditioning invokes novel leukocyte and brain responses to stroke. In this, CpG may be a unique preconditioning agent, coordinating peripheral and brain responses to protect against ischemic injury.

Published

2009

39. Toll-like receptor signaling in endogenous neuroprotection and stroke.

Author

Marsh BJ, Williams-Karnesky RL, and Stenzel-Poore MP

Subjects

Animals, Brain Infarction genetics, Brain Infarction immunology, Brain Ischemia genetics, Brain Ischemia immunology, Cytoprotection genetics, Cytoprotection immunology, Encephalitis genetics, Encephalitis immunology, Gene Expression Regulation genetics, Gene Expression Regulation immunology, Humans, Immune Tolerance genetics, Immune Tolerance immunology, Nerve Degeneration genetics, Nerve Degeneration immunology, Signal Transduction genetics, Signal Transduction immunology, Toll-Like Receptors genetics, Brain Infarction metabolism, Brain Ischemia metabolism, Encephalitis metabolism, Nerve Degeneration metabolism, Toll-Like Receptors metabolism

Abstract

Stroke and other cerebral vascular diseases are a leading cause of morbidity and mortality in the United States. Despite intensive research to identify interventions that lessen cerebrovascular injury, no major therapies exist. Development of stroke prophylaxis involves an understanding of the mechanisms of damage following cerebral ischemia, and elucidation of the endogenous mechanisms that combat further brain injury. Toll-like receptors (TLRs) are critical components of the innate immune system that have been shown recently to mediate ischemic injury. Paradoxically, TLR ligands administered systemically induce a state of tolerance to subsequent ischemic injury. Herein we suggest that stimulation of TLRs prior to ischemia reprograms TLR signaling that occurs following ischemic injury. Such reprogramming leads to suppressed expression of pro-inflammatory molecules and enhanced expression of numerous anti-inflammatory mediators that collectively confer robust neuroprotection. Our findings indicate that numerous preconditioning stimuli lead to TLR activation, an event that occurs prior to ischemia and ultimately leads to TLR reprogramming. Thus genomic reprogramming of TLR signaling may be a unifying principle of tolerance to cerebral ischemia.

Published

2009

40. Plasma adiponectin levels are increased despite insulin resistance in corticotropin-releasing hormone transgenic mice, an animal model of Cushing syndrome.

Author

Shinahara M, Nishiyama M, Iwasaki Y, Nakayama S, Noguchi T, Kambayashi M, Okada Y, Tsuda M, Stenzel-Poore MP, Hashimoto K, and Terada Y

Subjects

Adiponectin biosynthesis, Animals, Corticosterone blood, Disease Models, Animal, Male, Mice, Mice, Transgenic, Adiponectin blood, Corticotropin-Releasing Hormone genetics, Cushing Syndrome blood, Insulin Resistance physiology

Abstract

Adiponectin (AdN), an adipokine derived from the adipose tissue, has an insulin-sensitizing effect, and plasma AdN is shown to be decreased in obesity and/or insulin resistant state. To clarify whether changes in AdN are also responsible for the development of glucocorticoid-induced insulin resistance, we examined AdN concentration in plasma and AdN expression in the adipose tissue, using corticotropin-releasing hormone (CRH) transgenic mouse (CRH-Tg), an animal model of Cushing syndrome. We found, unexpectedly, that plasma AdN levels in CRHTg were significantly higher than those in wild-type littermates (wild-type: 19.7+/-2.5, CRH-Tg: 32.4+/-3.1 microg/mL, p<0.01). On the other hand, AdN mRNA and protein levels were significantly decreased in the adipose tissue of CRH-Tg. Bilateral adrenalectomy in CRH-Tg eliminated both their Cushing's phenotype and their increase in plasma AdN levels (wild-type/sham: 9.4+/-0.5, CRH-Tg/sham: 15.7+/-2.0, CRH-Tg/ADX: 8.5+/-0.4 microg/mL). These results strongly suggest that AdN is not a major factor responsible for the development of insulin resistance in Cushing syndrome. Our data also suggest that glucocorticoid increases plasma AdN levels but decreases AdN expression in adipocytes, the latter being explained possibly by the decrease in AdN metabolism in the Cushing state.

Published

2009

41. It's all in the family: multiple Toll-like receptors offer promise as novel therapeutic targets for stroke neuroprotection.

Author

Leung PY, Packard AE, and Stenzel-Poore MP

Abstract

Ischemic tolerance is a biological process that can be utilized to unlock the brain's own endogenous protection mechanisms and, as such, holds true promise for patients at risk of ischemic injury. Experimentally, preconditioning with various Toll-like receptor (TLR) agonists has now been demonstrated to successfully attenuate ischemic damage, partly through genomic reprogramming of the body's response to stroke. This treatment diminishes the inflammatory response to stroke and at the same time enhances the production of anti-inflammatory cytokines and neuroprotective mediators. This review discusses recent discoveries about the role of TLRs in preconditioning and ischemic tolerance.

Published

2009

42. Corticotropin-releasing factor-overexpressing mice exhibit reduced neuronal activation in the arcuate nucleus and food intake in response to fasting.

Author

Stengel A, Goebel M, Million M, Stenzel-Poore MP, Kobelt P, Mönnikes H, Taché Y, and Wang L

Subjects

Animals, Arcuate Nucleus of Hypothalamus drug effects, Cholecystokinin pharmacology, Eating drug effects, Gastric Emptying drug effects, Gastric Emptying physiology, Gene Expression Regulation, Genes, fos, Ghrelin pharmacology, Hyperphagia physiopathology, Hypothalamus, Middle drug effects, Hypothalamus, Middle physiology, Mice, Nootropic Agents pharmacology, Sincalide analogs & derivatives, Sincalide pharmacology, Arcuate Nucleus of Hypothalamus physiology, Corticotropin-Releasing Hormone genetics, Eating physiology, Energy Intake drug effects, Fasting physiology, Neurons physiology

Abstract

Corticotropin-releasing factor (CRF) overexpressing (OE) mice are a genetic model that exhibits features of chronic stress. We investigated whether the adaptive feeding response to a hypocaloric challenge induced by food deprivation is impaired under conditions of chronic CRF overproduction. Food intake response to a 16-h overnight fast and ip injection of gut hormones regulating food intake were compared in CRF-OE and wild type (WT) littermate mice along with brain Fos expression, circulating ghrelin levels, and gastric emptying of a nonnutrient meal. CRF-OE mice injected ip with saline showed a 47 and 44% reduction of 30-min and 4-h cumulative food intake response to an overnight fast, respectively, compared with WT. However, the 30-min food intake decrease induced by ip cholecystokinin (3 microg/kg) and increase by ghrelin (300 microg/kg) were similar in CRF-OE and WT mice. Overnight fasting increased the plasma total ghrelin to similar levels in CRF-OE and WT mice, although CRF-OE mice had a 2-fold reduction of nonfasting ghrelin levels. The number of Fos-immunoreactive cells induced by fasting in the arcuate nucleus was reduced by 5.9-fold in CRF-OE compared with WT mice whereas no significant changes were observed in other hypothalamic nuclei. In contrast, fasted CRF-OE mice displayed a 5.6-fold increase in Fos-immunoreactive cell number in the dorsal motor nucleus of the vagus nerve and a 34% increase in 20-min gastric emptying. These findings indicate that sustained overproduction of hypothalamic CRF in mice interferes with fasting-induced activation of arcuate nucleus neurons and the related hyperphagic response.

Published

2009

43. Mechanisms of ischemic brain damage.

Author

Doyle KP, Simon RP, and Stenzel-Poore MP

Subjects

Animals, Apoptosis physiology, Brain physiopathology, Brain Ischemia physiopathology, Humans, Inflammation pathology, Inflammation physiopathology, Oxidative Stress physiology, Reactive Nitrogen Species physiology, Stroke pathology, Stroke physiopathology, Brain pathology, Brain Ischemia pathology

Abstract

In the United States stroke is the third leading cause of death and the leading cause of disability. Brain injury following stroke results from the complex interplay of multiple pathways including excitotoxicity, acidotoxicity, ionic imbalance, peri-infarct depolarization, oxidative and nitrative stress, inflammation and apoptosis. There are very few treatments for stroke and the development of new treatments requires a comprehensive understanding of the diverse mechanisms of ischemic brain damage that are responsible for neuronal death. Here, we discuss the underlying pathophysiology of this devastating disease and reveal the intertwined pathways that are the target of therapeutic intervention.

Published

2008

44. Corticotropin-releasing factor-1 receptor involvement in behavioral neuroadaptation to ethanol: a urocortin1-independent mechanism.

Author

Pastor R, McKinnon CS, Scibelli AC, Burkhart-Kasch S, Reed C, Ryabinin AE, Coste SC, Stenzel-Poore MP, and Phillips TJ

Subjects

Adrenocorticotropic Hormone blood, Animals, Ethanol administration & dosage, Gene Deletion, Mice, Mice, Inbred C57BL, Mice, Knockout, Mifepristone pharmacology, Psychomotor Performance drug effects, Pyrimidines pharmacology, Pyrroles pharmacology, Urocortins metabolism, Adaptation, Biological drug effects, Behavior, Animal drug effects, Ethanol pharmacology, Nervous System Physiological Phenomena drug effects, Receptors, Corticotropin-Releasing Hormone metabolism

Abstract

A common expression of neuroadaptations induced by repeated exposure to addictive drugs is a persistent sensitized behavioral response to their stimulant properties. Neuroplasticity underlying drug-induced sensitization has been proposed to explain compulsive drug pursuit and consumption characteristic of addiction. The hypothalamic-pituitary-adrenal (HPA) axis-activating neuropeptide, corticotropin-releasing factor (CRF), may be the keystone in drug-induced neuroadaptation. Corticosterone-activated glucocorticoid receptors (GRs) mediate the development of sensitization to ethanol (EtOH), implicating the HPA axis in this process. EtOH-induced increases in corticosterone require CRF activation of CRF1 receptors. We posited that CRF1 signaling pathways are crucial for EtOH-induced sensitization. We demonstrate that mice lacking CRF1 receptors do not show psychomotor sensitization to EtOH, a phenomenon that was also absent in CRF1 + 2 receptor double-knockout mice. Deletion of CRF2 receptors alone did not prevent sensitization. A blunted endocrine response to EtOH was found only in the genotypes showing no sensitization. The CRF1 receptor antagonist CP-154,526 attenuated the acquisition and prevented the expression of EtOH-induced psychomotor sensitization. Because CRF1 receptors are also activated by urocortin-1 (Ucn1), we tested Ucn1 knockout mice for EtOH sensitization and found normal sensitization in this genotype. Finally, we show that the GR antagonist mifepristone does not block the expression of EtOH sensitization. CRF and CRF1 receptors, therefore, are involved in the neurobiological adaptations that underlie the development and expression of psychomotor sensitization to EtOH. A CRF/CRF1-mediated mechanism involving the HPA axis is proposed for acquisition, whereas an extrahypothalamic CRF/CRF1 participation is suggested for expression of sensitization to EtOH.

Published

2008

45. Nasal administration of osteopontin peptide mimetics confers neuroprotection in stroke.

Author

Doyle KP, Yang T, Lessov NS, Ciesielski TM, Stevens SL, Simon RP, King JS, and Stenzel-Poore MP

Subjects

Administration, Intranasal, Amino Acid Sequence, Animals, Biomimetic Materials chemistry, Biomimetic Materials therapeutic use, Cells, Cultured, Cytoprotection drug effects, Female, Humans, Integrins metabolism, Male, Mice, Molecular Sequence Data, Neuroprotective Agents administration & dosage, Neuroprotective Agents chemistry, Neuroprotective Agents pharmacology, Osteopontin chemistry, Peptides administration & dosage, Peptides chemistry, Peptides therapeutic use, Phosphorylation drug effects, Protein Binding, Rats, Stroke pathology, Thrombin pharmacology, Time Factors, Biomimetic Materials administration & dosage, Neurons drug effects, Neuroprotective Agents therapeutic use, Osteopontin administration & dosage, Osteopontin therapeutic use, Stroke drug therapy

Abstract

Osteopontin (OPN), a large secreted glycoprotein with an arginine, glycine, aspartate (RGD) motif, can bind and signal through cellular integrin receptors. We have shown previously that OPN enhances neuronal survival in the setting of ischemia. Here, we sought to increase the neuroprotective potency of OPN and improve the method of delivery with the goal of identifying a treatment for stroke in humans. We show that thrombin cleavage of OPN improves its ability to ligate integrin receptors and its neuroprotective capacity in models of ischemia. Thrombin-cleaved OPN is a twofold more effective neuroprotectant than the untreated molecule. We also tested whether OPN could be administered intranasally and found that it is efficiently targeted to the brain via intranasal delivery. Furthermore, intranasal administration of thrombin-treated OPN confers protection against ischemic brain injury. Osteopontin mimetics based on the peptide sequences located either N or C terminal to the thrombin cleavage site were generated and tested in models of ischemia. Treatment with successively shorter N-terminal peptides and a phosphorylated C-terminal peptide provided significant neuroprotection against ischemic injury. These findings show that OPN mimetics offer promise for development into new drugs for the treatment of stroke.

Published

2008

46. Toll-like receptor 9: a new target of ischemic preconditioning in the brain.

Author

Stevens SL, Ciesielski TM, Marsh BJ, Yang T, Homen DS, Boule JL, Lessov NS, Simon RP, and Stenzel-Poore MP

Subjects

Animals, Brain Ischemia pathology, Cell Death drug effects, Disease Models, Animal, Infarction, Middle Cerebral Artery drug therapy, Infarction, Middle Cerebral Artery metabolism, Infarction, Middle Cerebral Artery pathology, Ligands, Male, Mice, Mice, Inbred C57BL, Neurons pathology, Oligodeoxyribonucleotides pharmacology, Tumor Necrosis Factor-alpha metabolism, Brain Ischemia drug therapy, Brain Ischemia metabolism, Ischemic Preconditioning methods, Lipopolysaccharides pharmacology, Neuroprotective Agents pharmacology, Toll-Like Receptor 9 metabolism

Abstract

Preconditioning with lipopolysaccharide (LPS), a toll-like receptor 4 (TLR4) ligand, provides neuroprotection against subsequent cerebral ischemic brain injury, through a tumor necrosis factor (TNF)alpha-dependent process. Here, we report the first evidence that another TLR, TLR9, can induce neuroprotection. We show that the TLR9 ligand CpG oligodeoxynucleotide (ODN) can serve as a potent preconditioning stimulus and provide protection against ischemic brain injury. Our studies show that systemic administration of CpG ODN 1826 in advance of brain ischemia (middle cerebral artery occlusion (MCAO)) reduces ischemic damage up to 60% in a dose- and time-dependent manner. We also offer evidence that CpG ODN preconditioning can provide direct protection to cells of the central nervous system, as we have found marked neuroprotection in modeled ischemia in vitro. Finally, we show that CpG preconditioning significantly increases serum TNFalpha levels before MCAO and that TNFalpha is required for subsequent reduction in damage, as mice lacking TNFalpha are not protected against ischemic injury by CpG preconditioning. Our studies show that preconditioning with a TLR9 ligand induces neuroprotection against ischemic injury through a mechanism that shares common elements with LPS preconditioning via TLR4.

Published

2008

47. Toll-like receptors: novel pharmacological targets for the treatment of neurological diseases.

Author

Marsh BJ and Stenzel-Poore MP

Subjects

Animals, Brain Diseases prevention & control, Humans, Immune Tolerance, Signal Transduction, Toll-Like Receptor 3 agonists, Toll-Like Receptor 9 agonists, Brain Diseases drug therapy, Toll-Like Receptors physiology

Abstract

Toll-like receptors (TLRs) are a family of evolutionarily conserved molecules that directly detect pathogen invasion or tissue damage and initiate a biological response. TLRs can signal through two primary intracellular pathways and as such can induce either immuno-stimulatory or immuno-modulatory molecules. Both sides of this twin-edged sword are being examined for their therapeutic potential in combating neurological disease. The immuno-stimulatory properties of TLRs are being used to generate tumor-specific immune responses to CNS tumors while the immuno-modulatory properties are being used to suppress damaging inflammatory responses to stroke. Recently, a third component of TLR signaling has begun to emerge--that of direct neuroprotection. Hence, the TLRs offer novel targets for the treatment of neurological disease.

Published

2008

48. Endotoxin preconditioning protects against the cytotoxic effects of TNFalpha after stroke: a novel role for TNFalpha in LPS-ischemic tolerance.

Author

Rosenzweig HL, Minami M, Lessov NS, Coste SC, Stevens SL, Henshall DC, Meller R, Simon RP, and Stenzel-Poore MP

Subjects

Animals, Antibodies immunology, Brain Ischemia chemically induced, Brain Ischemia genetics, Brain Ischemia pathology, Cells, Cultured, Cerebrovascular Disorders chemically induced, Cerebrovascular Disorders genetics, Cerebrovascular Disorders metabolism, Cerebrovascular Disorders pathology, Disease Models, Animal, Male, Mice, Mice, Knockout, Rats, Signal Transduction, Solubility, Tumor Necrosis Factor-alpha deficiency, Tumor Necrosis Factor-alpha genetics, Brain Ischemia metabolism, Ischemic Preconditioning, Lipopolysaccharides pharmacology, Tumor Necrosis Factor-alpha metabolism, Tumor Necrosis Factor-alpha toxicity

Abstract

Lipopolysaccharide (LPS) preconditioning provides neuroprotection against subsequent cerebral ischemic injury. Tumor necrosis factor-alpha (TNFalpha) is protective in LPS-induced preconditioning yet exacerbates neuronal injury in ischemia. Here, we define dual roles of TNFalpha in LPS-induced ischemic tolerance in a murine model of stroke and in primary neuronal cultures in vitro, and show that the cytotoxic effects of TNFalpha are attenuated by LPS preconditioning. We show that LPS preconditioning significantly increases circulating levels of TNFalpha before middle cerebral artery occlusion in mice and show that TNFalpha is required to establish subsequent neuroprotection against ischemia, as mice lacking TNFalpha are not protected from ischemic injury by LPS preconditioning. After stroke, LPS preconditioned mice have a significant reduction in the levels of TNFalpha (approximately threefold) and the proximal TNFalpha signaling molecules, neuronal TNF-receptor 1 (TNFR1), and TNFR-associated death domain (TRADD). Soluble TNFR1 (s-TNFR1) levels were significantly increased after stroke in LPS-preconditioned mice (approximately 2.5-fold), which may neutralize the effect of TNFalpha and reduce TNFalpha-mediated injury in ischemia. Importantly, LPS-preconditioned mice show marked resistance to brain injury caused by intracerebral administration of exogenous TNFalpha after stroke. We establish an in vitro model of LPS preconditioning in primary cortical neuronal cultures and show that LPS preconditioning causes significant protection against injurious TNFalpha in the setting of ischemia. Our studies suggest that TNFalpha is a twin-edged sword in the setting of stroke: TNFalpha upregulation is needed to establish LPS-induced tolerance before ischemia, whereas suppression of TNFalpha signaling during ischemia confers neuroprotection after LPS preconditioning.

Published

2007

49. Novel thyroxine derivatives, thyronamine and 3-iodothyronamine, induce transient hypothermia and marked neuroprotection against stroke injury.

Author

Doyle KP, Suchland KL, Ciesielski TM, Lessov NS, Grandy DK, Scanlan TS, and Stenzel-Poore MP

Subjects

Animals, Behavior, Animal physiology, Body Temperature, Brain Ischemia pathology, Cells, Cultured, Humans, Ischemic Preconditioning, Male, Mice, Mice, Inbred C57BL, Molecular Structure, Neurons cytology, Neurons metabolism, Stroke prevention & control, Hypothermia chemically induced, Neuroprotective Agents chemistry, Neuroprotective Agents metabolism, Neuroprotective Agents pharmacology, Stroke pathology, Thyronines chemistry, Thyronines metabolism, Thyronines pharmacology, Thyroxine analogs & derivatives

Abstract

Background and Purpose: Mild hypothermia confers profound neuroprotection in ischemia. We recently discovered 2 natural derivatives of thyroxine, 3-iodothyronamine (T(1)AM) and thyronamine (T(0)AM), that when administered to rodents lower body temperature for several hours without induction of a compensatory homeostatic response. We tested whether T(1)AM- and T(0)AM-induced hypothermia protects against brain injury from experimental stroke., Methods: We tested T(1)AM and T(0)AM 1 hour after and 2 days before stroke in a mouse model of focal ischemia. To determine whether T(1)AM and T(0)AM require hypothermia to protect against stroke injury, the induction of hypothermia was prevented., Results: T(1)AM and T(0)AM administration reduced body temperature from 37 degrees C to 31 degrees C. Mice given T(1)AM or T(0)AM after the ischemic period had significantly smaller infarcts compared with controls. Mice preconditioned with T(1)AM before ischemia displayed significantly smaller infarcts compared with controls. Pre- and postischemia treatments required the induction of hypothermia. T(1)AM and T(0)AM treatment in vitro failed to confer neuroprotection against ischemia., Conclusions: T(1)AM and T(0)AM, are potent neuroprotectants in acute stroke and T(1)AM can be used as antecedent treatment to induce neuroprotection against subsequent ischemia. Hypothermia induced by T(1)AM and T(0)AM may underlie neuroprotection. T(1)AM and T(0)AM offer promise as treatments for brain injury.

Published

2007

50. Expression profiling identifies the CRH/CRH-R1 system as a modulator of neurovascular gene activity.

Author

Deussing JM, Kühne C, Pütz B, Panhuysen M, Breu J, Stenzel-Poore MP, Holsboer F, and Wurst W

Subjects

Alkaline Phosphatase metabolism, Animals, Behavior, Animal physiology, Brain metabolism, Cerebrovascular Circulation physiology, Gene Expression Profiling, Glucocorticoids metabolism, Hypothalamo-Hypophyseal System physiology, In Situ Hybridization, Male, Mice, Mice, Knockout, Microcirculation, Molecular Sequence Data, Oligonucleotide Array Sequence Analysis, Pituitary-Adrenal System physiology, Receptors, Corticotropin-Releasing Hormone genetics, Reproducibility of Results, Signal Transduction physiology, Brain blood supply, Corticotropin-Releasing Hormone metabolism, Gene Expression Regulation, Receptors, Corticotropin-Releasing Hormone metabolism

Abstract

Corticotropin-releasing hormone receptor type 1 (CRH-R1)-deficient mice display reduced anxiety-like behavior, a chronic corticosterone deficit, and an impaired neuroendocrine stress response caused by disruption of the hypothalamic-pituitary-adrenocortical (HPA) axis. The molecular substrates and pathways of CRH/CRH-R1-dependent signaling mechanisms underlying the behavioral phenotype as well as the consequences of lifelong glucocorticoid deficit remain largely obscure. To dissect involved neuronal circuitries, we performed comparative expression profiling of brains of CRH-R1 mutant and wild-type mice using our custom made MPIP (Max Planck Institute of Psychiatry) 17k cDNA microarray. Microarray analysis yielded 107 genes showing altered expression levels when comparing CRH-R1 knockout mice with wild-type littermates. A significant proportion of differentially expressed genes was related to control of HPA and hypothalamic-pituitary-thyroid (HPT) axes reflecting not only the disturbance of the HPA axis in CRH-R1 mutant mice but also the interplay of both neuroendocrine systems. The spatial analysis of regulated genes revealed a prevalence for genes expressed in the cerebral microvasculature. This phenotype was confirmed by the successful cross-validation of regulated genes in CRH overexpressing mice. Analysis of the cerebral vasculature of CRH-R1 mutant and CRH overexpressing mice revealed alterations of functional rather than structural properties. A direct role of the CRH/CRH-R1 system was supported by demonstrating Crhr1 expression in the adult murine cerebral vasculature. In conclusion, these data suggest a novel, previously unknown role of the CRH/CRH-R1 system in modulating neurovascular gene expression and function.

Published

2007