Your search keyword '"Heijnen CJ"' showing total 461 results

101. Longitudinal changes in glucocorticoid receptor exon 1 F methylation and psychopathology after military deployment.

Author

Schür RR, Boks MP, Rutten BPF, Daskalakis NP, de Nijs L, van Zuiden M, Kavelaars A, Heijnen CJ, Joëls M, Kahn RS, Geuze E, Vermetten E, and Vinkers CH

Subjects

Adolescent, Adult, Afghan Campaign 2001-, Epigenesis, Genetic, Exons, Humans, Longitudinal Studies, Male, Mental Health, Middle Aged, Military Personnel, Prospective Studies, Psychiatric Status Rating Scales, Stress Disorders, Post-Traumatic genetics, Stress, Psychological, Young Adult, DNA Methylation, Exposure to Violence, Mental Disorders genetics, Receptors, Glucocorticoid genetics

Abstract

Several cross-sectional studies have demonstrated the relevance of DNA methylation of the glucocorticoid receptor exon 1 F region (GR-1 F ) for trauma-related psychopathology. We conducted a longitudinal study to examine GR-1 F methylation changes over time in relation to trauma exposure and the development of post-deployment psychopathology. GR-1 F methylation (52 loci) was quantified using pyrosequencing in whole blood of 92 military men 1 month before and 6 months after a 4-month deployment period to Afghanistan. GR-1 F methylation overall (mean methylation and the number of methylated loci) and functional methylation (methylation at loci associated with GR exon 1 F expression) measures were examined. We first investigated the effect of exposure to potentially traumatic events during deployment on these measures. Subsequently, changes in GR-1 F methylation were related to changes in mental health problems (total Symptom Checklist-90 score) and posttraumatic stress disorder (PTSD) symptoms (Self-Report Inventory for PTSD). Trauma exposure during deployment was associated with an increase in all methylation measures, but development of mental health problems 6 months after deployment was only significantly associated with an increased functional methylation. Emergence of post-deployment PTSD symptoms was not related to increased functional methylation over time. Pre-deployment methylation levels did not predict post-deployment psychopathology. To our knowledge, this is the first study to prospectively demonstrate trauma-related increases in GR-1 F methylation, and it shows that only increases at specific functionally relevant sites predispose for post-deployment psychopathology.

Published

2017

102. HDAC6 inhibition effectively reverses chemotherapy-induced peripheral neuropathy.

Author

Krukowski K, Ma J, Golonzhka O, Laumet GO, Gutti T, van Duzer JH, Mazitschek R, Jarpe MB, Heijnen CJ, and Kavelaars A

Subjects

Animals, Antineoplastic Agents administration & dosage, Male, Mice, Mice, Inbred C57BL, Pain diagnosis, Peripheral Nervous System Diseases diagnosis, Rats, Rats, Sprague-Dawley, Treatment Outcome, Cisplatin adverse effects, Histone Deacetylase 6 antagonists & inhibitors, Hydroxamic Acids administration & dosage, Pain chemically induced, Pain prevention & control, Peripheral Nervous System Diseases chemically induced, Peripheral Nervous System Diseases prevention & control, Pyrimidines administration & dosage

Abstract

Chemotherapy-induced peripheral neuropathy is one of the most common dose-limiting side effects of cancer treatment. Currently, there is no Food and Drug Administration-approved treatment available. Histone deacetylase 6 (HDAC6) is a microtubule-associated deacetylase whose function includes regulation of α-tubulin-dependent intracellular mitochondrial transport. Here, we examined the effect of HDAC6 inhibition on established cisplatin-induced peripheral neuropathy. We used a novel HDAC6 inhibitor ACY-1083, which shows 260-fold selectivity towards HDAC6 vs other HDACs. Our results show that HDAC6 inhibition prevented cisplatin-induced mechanical allodynia, and also completely reversed already existing cisplatin-induced mechanical allodynia, spontaneous pain, and numbness. These findings were confirmed using the established HDAC6 inhibitor ACY-1215 (Ricolinostat), which is currently in clinical trials for cancer treatment. Mechanistically, treatment with the HDAC6 inhibitor increased α-tubulin acetylation in the peripheral nerve. In addition, HDAC6 inhibition restored the cisplatin-induced reduction in mitochondrial bioenergetics and mitochondrial content in the tibial nerve, indicating increased mitochondrial transport. At a later time point, dorsal root ganglion mitochondrial bioenergetics also improved. HDAC6 inhibition restored the loss of intraepidermal nerve fiber density in cisplatin-treated mice. Our results demonstrate that pharmacological inhibition of HDAC6 completely reverses all the hallmarks of established cisplatin-induced peripheral neuropathy by normalization of mitochondrial function in dorsal root ganglia and nerve, and restoration of intraepidermal innervation. These results are especially promising because one of the HDAC6 inhibitors tested here is currently in clinical trials as an add-on cancer therapy, highlighting the potential for a fast clinical translation of our findings.

Published

2017

103. Mesenchymal stem cells attenuate MRI-identifiable injury, protect white matter, and improve long-term functional outcomes after neonatal focal stroke in rats.

Author

van Velthoven CT, Dzietko M, Wendland MF, Derugin N, Faustino J, Heijnen CJ, Ferriero DM, and Vexler ZS

Subjects

Age Factors, Analysis of Variance, Animals, Animals, Newborn, Bromodeoxyuridine metabolism, Disease Models, Animal, Gene Expression Regulation, Developmental physiology, Glial Fibrillary Acidic Protein metabolism, Image Processing, Computer-Assisted, Lectins metabolism, Myelin Basic Protein metabolism, Psychomotor Disorders etiology, Rats, Rats, Sprague-Dawley, White Matter metabolism, Cell- and Tissue-Based Therapy methods, Infarction, Middle Cerebral Artery diagnostic imaging, Infarction, Middle Cerebral Artery pathology, Infarction, Middle Cerebral Artery therapy, Magnetic Resonance Imaging, Mesenchymal Stem Cells physiology, White Matter pathology

Abstract

Cell therapy has emerged as a potential treatment for many neurodegenerative diseases including stroke and neonatal ischemic brain injury. Delayed intranasal administration of mesenchymal stem cells (MSCs) after experimental hypoxia-ischemia and after a transient middle cerebral artery occlusion (tMCAO) in neonatal rats has shown improvement in long-term functional outcomes, but the effects of MSCs on white matter injury (WMI) are insufficiently understood. In this study we used longitudinal T2-weighted (T2W) and diffusion tensor magnetic resonance imaging (MRI) to characterize chronic injury after tMCAO induced in postnatal day 10 (P10) rats and examined the effects of delayed MSC administration on WMI, axonal coverage, and long-term somatosensory function. We show unilateral injury- and region-dependent changes in diffusion fraction anisotropy 1 and 2 weeks after tMCAO that correspond to accumulation of degraded myelin basic protein, astrocytosis, and decreased axonal coverage. With the use of stringent T2W-based injury criteria at 72 hr after tMCAO to randomize neonatal rats to receive intranasal MSCs or vehicle, we show that a single MSC administration attenuates WMI and enhances somatosensory function 28 days after stroke. A positive correlation was found between MSC-enhanced white matter integrity and functional performance in injured neonatal rats. Collectively, these data indicate that the damage induced by tMCAO progresses over time and is halted by administration of MSCs. © 2016 Wiley Periodicals, Inc., (© 2016 Wiley Periodicals, Inc.)

Published

2017

104. Inhibition of Mitochondrial p53 Accumulation by PFT-μ Prevents Cisplatin-Induced Peripheral Neuropathy.

Author

Maj MA, Ma J, Krukowski KN, Kavelaars A, and Heijnen CJ

Abstract

Chemotherapy-induced peripheral neuropathy (CIPN), a debilitating major side effect of cancer treatment, is characterized by pain and sensory loss in hand and feet. Platinum-based chemotherapeutics like cisplatin frequently induce CIPN. The molecular mechanism underlying these neurotoxic symptoms is incompletely understood and there are no preventive or curative interventions. We hypothesized that cisplatin acts as a cellular stressor that triggers p53 accumulation at mitochondria, leading to mitochondrial dysfunction and CIPN. To test this hypothesis, we examined the effect of the small molecule pifithrin-μ (PFT-μ), an inhibitor of p53 mitochondrial association on CIPN and the associated mitochondrial dysfunction. We show here for the first time that in vivo cisplatin rapidly increases mitochondrial accumulation of p53 in dorsal root ganglia (DRG), spinal cord, and peripheral nerve without evidence for apoptosis. Cisplatin-treatment also reduced mitochondrial membrane potential and lead to abnormal mitochondrial morphology and impaired mitochondrial function in DRG neurons. Pre-treatment with PFT-μ prevented the early cisplatin-induced increase in mitochondrial p53 and the reduction in mitochondrial membrane potential. Inhibition of the early mitochondrial p53 accumulation by PFT-μ also prevented the abnormalities in mitochondrial morphology and mitochondrial bioenergetics (reduced oxygen consumption rate, maximum respiratory capacity, and adenosine triphosphate synthesis) that develop in DRG and peripheral nerve after cisplatin-treatment. Functionally, inhibition of mitochondrial p53 accumulation prevented the hallmarks of CIPN including mechanical allodynia, peripheral sensory loss (numbness) as quantified by an adhesive-removal task, and loss of intra-epidermal nerve fibers. In conclusion, PFT-μ is a potential neuroprotective agent that prevents cisplatin-induced mitochondrial dysfunction in DRG and peripheral nerves thereby protecting against CIPN through blockade of the early cisplatin-induced increase in mitochondrial p53. Notably, there is accumulating evidence that PFT-μ has anti-tumor activities and could therefore be an attractive candidate to prevent CIPN while promoting tumor cell death.

Published

2017

105. Pifithrin-μ Prevents Cisplatin-Induced Chemobrain by Preserving Neuronal Mitochondrial Function.

Author

Chiu GS, Maj MA, Rizvi S, Dantzer R, Vichaya EG, Laumet G, Kavelaars A, and Heijnen CJ

Subjects

Animals, Blotting, Western, Cognition Disorders chemically induced, Disease Models, Animal, Head and Neck Neoplasms pathology, Male, Maze Learning drug effects, Mice, Mice, Inbred C57BL, Microscopy, Electron, Transmission, Mitochondria drug effects, Real-Time Polymerase Chain Reaction, Tumor Suppressor Protein p53 drug effects, Antineoplastic Agents toxicity, Brain drug effects, Cisplatin toxicity, Neurons drug effects, Neuroprotective Agents pharmacology, Sulfonamides pharmacology

Abstract

Cognitive impairment, termed chemobrain, is a common neurotoxicity associated with chemotherapy treatment, affecting an estimated 78% of patients. Prompted by the hypothesis that neuronal mitochondrial dysfunction underlies chemotherapy-induced cognitive impairment (CICI), we explored the efficacy of administering the small-molecule pifithrin (PFT)-μ, an inhibitor of mitochondrial p53 accumulation, in preventing CICI. Male C57BL/6J mice injected with cisplatin ± PFT-μ for two 5-day cycles were assessed for cognitive function using novel object/place recognition and alternation in a Y-maze. Cisplatin impaired performance in the novel object/place recognition and Y-maze tests. PFT-μ treatment prevented CICI and associated cisplatin-induced changes in coherency of myelin basic protein fibers in the cingular cortex and loss of doublecortin + cells in the subventricular zone and hippocampal dentate gyrus. Mechanistically, cisplatin decreased spare respirator capacity of brain synaptosomes and caused abnormal mitochondrial morphology, which was counteracted by PFT-μ administration. Notably, increased mitochondrial p53 did not lead to cerebral caspase-3 activation or cytochrome-c release. Furthermore, PFT-μ administration did not impair the anticancer efficacy of cisplatin and radiotherapy in tumor-bearing mice. Our results supported the hypothesis that neuronal mitochondrial dysfunction induced by mitochondrial p53 accumulation is an underlying cause of CICI and that PFT-μ may offer a tractable therapeutic strategy to limit this common side-effect of many types of chemotherapy. Cancer Res; 77(3); 742-52. ©2016 AACR., Competing Interests: The authors report no conflicts of interest in this work., (©2016 American Association for Cancer Research.)

Published

2017

106. Mechanisms of Neurotoxic Symptoms as a Result of Breast Cancer and Its Treatment: Considerations on the Contribution of Stress, Inflammation, and Cellular Bioenergetics.

Author

Lacourt TE and Heijnen CJ

Abstract

Purpose of Review: Breast cancer and its treatment are associated with a range of neurotoxic symptoms, such as fatigue, cognitive impairment, and pain. Although these symptoms generally subside after treatment completion, they become chronic in a significant subset of patients. We here summarize recent findings on neuroinflammation, stress, and mitochondrial dysfunction as mechanistic pathways leading to neurotoxic symptom experience in breast cancer patients and survivors., Recent Findings: Neuroinflammation related to stress or cancer treatment and stress resulting from diagnosis, treatment, or (cancer-related) worrying are important predictors of a neurotoxic symptom experience, both during and after treatment for breast cancer. Both inflammation and stress hormones, as well as cancer treatment, can induce mitochondrial dysfunction resulting in reduced cellular energy., Summary: We propose reduced cellular energy (mitochondrial dysfunction) induced by inflammation, oxygen radical production, and stress as a result of cancer and/or cancer treatment as a final mechanism underlying neurotoxic symptoms.

Published

2017

107. Delayed administration of neural stem cells after hypoxia-ischemia reduces sensorimotor deficits, cerebral lesion size, and neuroinflammation in neonatal mice.

Author

Braccioli L, Heijnen CJ, Coffer PJ, and Nijboer CH

Subjects

Animals, Animals, Newborn, Behavior, Animal, Cell Movement, Disease Models, Animal, Female, Hippocampus pathology, Hypoxia-Ischemia, Brain pathology, Hypoxia-Ischemia, Brain physiopathology, Inflammation pathology, Inflammation therapy, Male, Mice, Mice, Inbred C57BL, Psychomotor Performance, Time Factors, Transplantation, Homologous, Hypoxia-Ischemia, Brain therapy, Neural Stem Cells transplantation

Abstract

Background: Hypoxic-ischemic (HI) encephalopathy causes mortality and severe morbidity in neonates. Treatments with a therapeutic window >6 h are currently not available. Here, we explored whether delayed transplantation of allogenic neural stem cells (NSCs) at 10 d after HI could be a tool to repair HI brain injury and improve behavioral impairments., Methods: HI was induced in 9-d-old mice. Animals received NSCs or vehicle intracranially in the hippocampus at 10 d post-HI. Sensorimotor performance was assessed by cylinder rearing test. Lesion size, synaptic integrity, and fate of injected NSCs were determined by immuno-stainings. Neuroinflammation was studied by immuno-stainings of brain sections, primary glial cultures, and TNFα ELISA., Results: NSC transplantation at 10 d post-insult induced long-term improvement of motor performance and synaptic integrity, and reduced lesion size compared to vehicle-treatment. HI-induced neuroinflammation was reduced after NSC treatment, at least partially by factors secreted by NSCs. Injected NSCs migrated toward and localized at the damaged hippocampus. Transplanted NSCs differentiated toward the neuronal lineage and formed a niche with endogenous precursors., Conclusion: Our study provides evidence of the efficacy of NSC transplantation late after HI as a tool to reduce neonatal HI brain injury through regeneration of the lesion.

Published

2017

108. Epac1 interacts with importin β1 and controls neurite outgrowth independently of cAMP and Rap1.

Author

Baameur F, Singhmar P, Zhou Y, Hancock JF, Cheng X, Heijnen CJ, and Kavelaars A

Subjects

Cell Line, Cyclic AMP metabolism, Guanine Nucleotide Exchange Factors genetics, HEK293 Cells, Humans, Proteomics, rap1 GTP-Binding Proteins metabolism, Cell Membrane metabolism, Guanine Nucleotide Exchange Factors metabolism, Neuronal Outgrowth, beta Karyopherins metabolism

Abstract

Exchange protein directly activated by cAMP-1 (Epac1) is a cAMP sensor that regulates multiple cellular functions including cellular migration, proliferation and differentiation. Classically, Epac1 is thought to exert its effects through binding of cAMP leading to a conformational change in Epac1 and its accumulation at the plasma membrane (PM) where it activates Rap1. In search for regulators of Epac1 activity, we show here that importin β1 (impβ1) is an Epac1 binding partner that prevents PM accumulation of Epac1. We demonstrate that in the absence of impβ1, endogenous as well as overexpressed Epac1 accumulate at the PM. Moreover, agonist-induced PM translocation of Epac1 leads to dissociation of Epac1 from impβ1. Localization of Epac1 at the PM in the absence of impβ1, requires residue R82 in its DEP domain. Notably, the PM accumulation of Epac1 in the absence of impβ1 does not require binding of cAMP to Epac1 and does not result in Rap1 activation. Functionally, PM accumulation of Epac1, an Epac1 mutant deficient in cAMP binding, or an Epac1 mutant tethered to the PM, is sufficient to inhibit neurite outgrowth. In conclusion, we uncover a cAMP-independent function of Epac1 at the PM and demonstrate that impβ1 controls subcellular localization of Epac1.

Published

2016

109. CD8+ T Cells and Endogenous IL-10 Are Required for Resolution of Chemotherapy-Induced Neuropathic Pain.

Author

Krukowski K, Eijkelkamp N, Laumet G, Hack CE, Li Y, Dougherty PM, Heijnen CJ, and Kavelaars A

Subjects

Animals, Antineoplastic Agents, CD8-Positive T-Lymphocytes pathology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Neuralgia pathology, Pain Perception drug effects, CD8-Positive T-Lymphocytes drug effects, Interleukin-10 metabolism, Neuralgia chemically induced, Neuralgia metabolism, Paclitaxel adverse effects, Pain Measurement drug effects

Abstract

Chemotherapy-induced peripheral neuropathy (CIPN), characterized by pain and numbness in hands and feet, is a common side effect of cancer treatment. In most patients, symptoms of CIPN subside after treatment completion. However, in a substantial subgroup, CIPN persists long into survivorship. Impairment in pain resolution pathways may explain persistent CIPN. We investigated the contribution of T cells and endogenous interleukin (IL)-10 to resolution of CIPN. Paclitaxel-induced mechanical allodynia was prolonged in T-cell-deficient (Rag1 -/- ) mice compared with wild-type (WT) mice. There were no differences between WT and Rag1 -/- mice in severity of paclitaxel-induced mechanical allodynia. Adoptive transfer of either CD3 + or CD8 + , but not CD4 + , T cells to Rag1 -/- mice normalized resolution of CIPN. Paclitaxel treatment increased the number of T cells in lumbar dorsal root ganglia (DRG), where CD8 + T cells were the major subset. Inhibition of endogenous IL-10 signaling by intrathecal injection of anti-IL-10 to WT mice or Rag1 -/- mice reconstituted with CD8 + T cells delayed recovery from paclitaxel-induced mechanical allodynia. Recovery was also delayed in IL-10 knock-out mice. Conversely, administration of exogenous IL-10 attenuated paclitaxel-induced allodynia. In vitro, IL-10 suppressed abnormal paclitaxel-induced spontaneous discharges in DRG neurons. Paclitaxel increased DRG IL-10 receptor expression and this effect requires CD8 + T cells. In conclusion, we identified a novel mechanism for resolution of CIPN that requires CD8 + T cells and endogenous IL-10. We propose that CD8 + T cells increase DRG IL-10 receptor expression and that IL-10 suppresses the abnormal paclitaxel-induced spontaneous discharges by DRG neurons to promote recovery from CIPN., Significance Statement: Chemotherapy-induced peripheral neuropathy persists after completion of cancer treatment in a significant subset of patients, whereas others recover. Persistent neuropathy after completion of cancer treatment severely affects quality of life. We propose that understanding how neuropathy resolves will identify novel avenues for treatment. We identified a novel and critical role for CD8 + T cells and for endogenous IL-10 in recovery from paclitaxel-induced neuropathy in mice. Enhancing the capacity of CD8 + T cells to promote resolution or increasing IL-10 signaling are promising targets for novel interventions. Clinically, peripheral blood CD8 + T-cell function and/or the capacity of individuals to produce IL-10 may represent biomarkers of risk for developing persistent peripheral neuropathy after completion of cancer treatment., (Copyright © 2016 the authors 0270-6474/16/3611074-10$15.00/0.)

Published

2016

110. Executive functioning and diabetes: The role of anxious arousal and inflammation.

Author

Murdock KW, LeRoy AS, Lacourt TE, Duke DC, Heijnen CJ, and Fagundes CP

Subjects

Adult, Aged, Anxiety immunology, Diabetes Complications psychology, Diabetes Mellitus, Type 2 metabolism, Female, Glycated Hemoglobin analysis, Humans, Inflammation metabolism, Inflammation physiopathology, Inflammation psychology, Inhibition, Psychological, Interleukin-6 analysis, Interleukin-6 blood, Male, Middle Aged, Self Report, Arousal physiology, Diabetes Complications physiopathology, Executive Function physiology

Abstract

Individuals who perform poorly on measures of the executive function of inhibition have higher anxious arousal in comparison to those with better performance. High anxious arousal is associated with a pro-inflammatory response. Chronically high anxious arousal and inflammation increase one's risk of developing type 2 diabetes. We sought to evaluate anxious arousal and inflammation as underlying mechanisms linking inhibition with diabetes incidence. Participants (N=835) completed measures of cognitive abilities, a self-report measure of anxious arousal, and donated blood to assess interleukin-6 (IL-6) and glycated hemoglobin (HbA1c). Individuals with low inhibition were more likely to have diabetes than those with high inhibition due to the serial pathway from high anxious arousal to IL-6. Findings remained when entering other indicators of cognitive abilities as covariates, suggesting that inhibition is a unique cognitive ability associated with diabetes incidence. On the basis of our results, we propose several avenues to explore for improved prevention and treatment efforts for type 2 diabetes., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

111. IL4-10 Fusion Protein Is a Novel Drug to Treat Persistent Inflammatory Pain.

Author

Eijkelkamp N, Steen-Louws C, Hartgring SA, Willemen HL, Prado J, Lafeber FP, Heijnen CJ, Hack CE, van Roon JA, and Kavelaars A

Subjects

Animals, Carrageenan toxicity, Cells, Cultured, Disease Models, Animal, Female, Freund's Adjuvant toxicity, Humans, Inflammation chemically induced, Interleukin-10 genetics, Interleukin-10 metabolism, Interleukin-4 genetics, Interleukin-4 metabolism, Lipopolysaccharides pharmacology, Male, Mice, Mice, Inbred C57BL, Neuroglia drug effects, Neuroglia metabolism, Pain Management, Pain Threshold drug effects, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Recombinant Fusion Proteins therapeutic use, Spinal Cord cytology, Treatment Outcome, Analgesics therapeutic use, Inflammation complications, Interleukin-10 therapeutic use, Interleukin-4 therapeutic use, Neuralgia drug therapy, Neuralgia etiology

Abstract

Unlabelled: Chronic pain is a major clinical problem that is difficult to treat and requires novel therapies. Although most pain therapies primarily target neurons, neuroinflammatory processes characterized by spinal cord and dorsal root ganglion production of proinflammatory cytokines play an important role in persistent pain states and represent potential therapeutic targets. Anti-inflammatory cytokines are attractive candidates to regulate aberrant neuroinflammatory processes, but the therapeutic potential of these cytokines as stand-alone drugs is limited. Their optimal function requires concerted actions with other regulatory cytokines, and their relatively small size causes rapid clearance. To overcome these limitations, we developed a fusion protein of the anti-inflammatory cytokines interleukin 4 (IL4) and IL10. The IL4-10 fusion protein is a 70 kDa glycosylated dimeric protein that retains the functional activity of both cytokine moieties. Intrathecal administration of IL4-10 dose-dependently inhibited persistent inflammatory pain in mice: three IL4-10 injections induced full resolution of inflammatory pain in two different mouse models of persistent inflammatory pain. Both cytokine moieties were required for optimal effects. The IL4-10 fusion protein was more effective than the individual cytokines or IL4 plus IL10 combination therapy and also inhibited allodynia in a mouse model of neuropathic pain. Mechanistically, IL4-10 inhibited the activity of glial cells and reduced spinal cord and dorsal root ganglion cytokine levels without affecting paw inflammation. In conclusion, we developed a novel fusion protein with improved efficacy to treat pain, compared with wild-type anti-inflammatory cytokines. The IL4-10 fusion protein has potential as a treatment for persistent inflammatory pain., Significance Statement: The treatment of chronic pain is a major clinical and societal challenge. Current therapies to treat persistent pain states are limited and often cause major side effects. Therefore, novel analgesic treatments are urgently needed. In search of a novel drug to treat chronic pain, we developed a fusion protein consisting of two prototypic regulatory cytokines, interleukin 4 (IL4) and IL10. The work presented in this manuscript shows that this IL4-10 fusion protein overcomes some major therapeutic limitations of pain treatment with individual cytokines. The IL4-10 fusion protein induces full resolution of persistent inflammatory pain in two different mouse models. These novel findings are significant, as they highlight the IL4-10 fusion protein as a long-needed potential new drug to stop persistent pain states., (Copyright © 2016 the authors 0270-6474/16/367353-11$15.00/0.)

Published

2016

112. Dorsal Root Ganglion Infiltration by Macrophages Contributes to Paclitaxel Chemotherapy-Induced Peripheral Neuropathy.

Author

Zhang H, Li Y, de Carvalho-Barbosa M, Kavelaars A, Heijnen CJ, Albrecht PJ, and Dougherty PM

Subjects

Anesthetics administration & dosage, Animals, Antibodies pharmacology, Antigens, CD metabolism, Antigens, Differentiation, Myelomonocytic metabolism, Bone Density Conservation Agents administration & dosage, Chemokine CCL2 immunology, Chemokine CCL2 metabolism, Clodronic Acid administration & dosage, Disease Models, Animal, Drug Administration Routes, GAP-43 Protein metabolism, Hyperalgesia etiology, Isoflurane administration & dosage, Lipopolysaccharides pharmacology, Macrophages physiology, Male, Pain Threshold drug effects, Peripheral Nervous System Diseases drug therapy, Peripheral Nervous System Diseases pathology, Rats, Rats, Sprague-Dawley, Spinal Cord pathology, Spleen drug effects, Spleen pathology, Time Factors, Tumor Necrosis Factor-alpha metabolism, Ubiquitin Thiolesterase metabolism, Antineoplastic Agents, Phytogenic toxicity, Cell Movement drug effects, Ganglia, Spinal pathology, Macrophages drug effects, Paclitaxel toxicity, Peripheral Nervous System Diseases chemically induced

Abstract

Unlabelled: Chemotherapy-induced peripheral neuropathy (CIPN) is a disruptive and persistent side effect of cancer treatment with paclitaxel. Recent reports showed that paclitaxel treatment results in the activation of Toll-like receptor 4 (TLR4) signaling and increased expression of monocyte chemoattractant protein 1 (MCP-1) in dorsal root ganglion cells. In this study, we sought to determine whether an important consequence of this signaling and also a key step in the CIPN phenotype was the recruitment and infiltration of macrophages into dorsal root ganglia (DRG). Here, we show that macrophage infiltration does occur in a time course that matches the onset of the behavioral CIPN phenotype in Sprague-Dawley rats. Moreover, depletion of macrophages by systemic administration of liposome-encapsulated clodronate (clophosome) partially reversed behavioral signs of paclitaxel-induced CIPN as well as reduced tumor necrosius factor α expression in DRG. Intrathecal injection of MCP-1 neutralizing antibodies reduced paclitaxel-induced macrophage recruitment into the DRG and also blocked the behavioral signs of CIPN. Intrathecal treatment with the TLR4 antagonist lipopolysaccharide-RS (LPS-RS) blocked mechanical hypersensitivity, reduced MCP-1 expression, and blocked the infiltration of macrophages into the DRG in paclitaxel-treated rats. The inhibition of macrophage infiltration into DRG after paclitaxel treatment with clodronate or LPS-RS prevented the loss of intraepidermal nerve fibers (IENFs) observed after paclitaxel treatment alone. These results are the first to indicate a mechanistic link such that activation of TLR4 by paclitaxel leads to increased expression of MCP-1 by DRG neurons resulting in macrophage infiltration to the DRG that express inflammatory cytokines and the combination of these events results in IENF loss and the development of behavioral signs of CIPN., Perspective: This paper shows that activation of innate immunity by paclitaxel results in a sequence of signaling events that results in the infiltration of the dorsal root ganglia by activated macrophages. Macrophages appear to drive the development of behavioral hypersensitivity and the loss of distal epidermal nerve fibers, and hence play an important role in the mechanism of paclitaxel-related neuropathy., (Copyright © 2016 American Pain Society. Published by Elsevier Inc. All rights reserved.)

Published

2016

113. Metformin Prevents Cisplatin-Induced Cognitive Impairment and Brain Damage in Mice.

Author

Zhou W, Kavelaars A, and Heijnen CJ

Subjects

Animals, Behavior, Animal drug effects, Brain drug effects, Brain pathology, Brain Injuries etiology, Brain Injuries pathology, Disease Models, Animal, Female, Hyperalgesia pathology, Hyperalgesia prevention & control, Hypoglycemic Agents pharmacology, Hypoglycemic Agents therapeutic use, Metformin pharmacology, Mice, Mice, Inbred C57BL, Myelin Basic Protein chemistry, Myelin Basic Protein metabolism, Pyramidal Cells metabolism, Pyramidal Cells pathology, Brain Injuries prevention & control, Cisplatin, Cognition Disorders chemically induced, Cognition Disorders prevention & control, Metformin therapeutic use

Abstract

Rationale: Chemotherapy-induced cognitive impairment, also known as 'chemobrain', is now widely recognized as a frequent adverse side effect of cancer treatment that often persists into survivorship. There are no drugs available to prevent or treat chemotherapy-induced cognitive deficits. The aim of this study was to establish a mouse model of cisplatin-induced cognitive deficits and to determine the potential preventive effects of the anti-diabetic drug metformin., Results: Treatment of C57/BL6J mice with cisplatin (cumulative dose 34.5 mg/kg) impaired performance in the novel object and place recognition task as well as in the social discrimination task indicating cognitive deficits. Co-administration of metformin prevented these cisplatin-induced cognitive impairments. At the structural level, we demonstrate that cisplatin reduces coherency of white matter fibers in the cingulate cortex. Moreover, the number of dendritic spines and neuronal arborizations as quantified on Golgi-stained brains was reduced after cisplatin treatment. Co-administration of metformin prevented all of these structural abnormalities in cisplatin-treated mice. In contrast to what has been reported in other models of chemobrain, we do not have evidence for persistent microglial or astrocyte activation in the brains of cisplatin-treated mice. Finally, we show that co-administration of metformin also protects against cisplatin-induced peripheral neuropathy., Conclusion: In summary, we show here for the first time that treatment of mice with cisplatin induces cognitive deficits that are associated with structural abnormalities in the brain. Moreover, we present the first evidence that the widely used and safe anti-diabetic drug metformin protects against these deleterious effects of cancer treatment. In view of the ongoing clinical trials to examine the potential efficacy of metformin as add-on therapy in patients treated for cancer, these findings should allow rapid clinical translation.

Published

2016

114. Critical role for Epac1 in inflammatory pain controlled by GRK2-mediated phosphorylation of Epac1.

Author

Singhmar P, Huo X, Eijkelkamp N, Berciano SR, Baameur F, Mei FC, Zhu Y, Cheng X, Hawke D, Mayor F Jr, Murga C, Heijnen CJ, and Kavelaars A

Subjects

Amino Acid Sequence, Animals, Chronic Disease, Freund's Adjuvant toxicity, Ganglia, Spinal physiopathology, Guanine Nucleotide Exchange Factors deficiency, Guanine Nucleotide Exchange Factors genetics, Hyperalgesia etiology, Inflammation chemically induced, Ion Channels physiology, Mechanoreceptors physiology, Mice, Mice, Knockout, Molecular Sequence Data, Nerve Tissue Proteins physiology, Pain etiology, Pain Threshold physiology, Phosphorylation, Phosphoserine metabolism, Protein Interaction Mapping, Protein Processing, Post-Translational, Protein Structure, Tertiary, Signal Transduction, rap1 GTP-Binding Proteins physiology, G-Protein-Coupled Receptor Kinase 2 physiology, Guanine Nucleotide Exchange Factors physiology, Hyperalgesia physiopathology, Inflammation complications, Nociception physiology, Pain physiopathology

Abstract

cAMP signaling plays a key role in regulating pain sensitivity. Here, we uncover a previously unidentified molecular mechanism in which direct phosphorylation of the exchange protein directly activated by cAMP 1 (EPAC1) by G protein kinase 2 (GRK2) suppresses Epac1-to-Rap1 signaling, thereby inhibiting persistent inflammatory pain. Epac1(-/-) mice are protected against inflammatory hyperalgesia in the complete Freund's adjuvant (CFA) model. Moreover, the Epac-specific inhibitor ESI-09 inhibits established CFA-induced mechanical hyperalgesia without affecting normal mechanical sensitivity. At the mechanistic level, CFA increased activity of the Epac target Rap1 in dorsal root ganglia of WT, but not of Epac1(-/-), mice. Using sensory neuron-specific overexpression of GRK2 or its kinase-dead mutant in vivo, we demonstrate that GRK2 inhibits CFA-induced hyperalgesia in a kinase activity-dependent manner. In vitro, GRK2 inhibits Epac1-to-Rap1 signaling by phosphorylation of Epac1 at Ser-108 in the Disheveled/Egl-10/pleckstrin domain. This phosphorylation event inhibits agonist-induced translocation of Epac1 to the plasma membrane, thereby reducing Rap1 activation. Finally, we show that GRK2 inhibits Epac1-mediated sensitization of the mechanosensor Piezo2 and that Piezo2 contributes to inflammatory mechanical hyperalgesia. Collectively, these findings identify a key role of Epac1 in chronic inflammatory pain and a molecular mechanism for controlling Epac1 activity and chronic pain through phosphorylation of Epac1 at Ser-108. Importantly, using the Epac inhibitor ESI-09, we validate Epac1 as a potential therapeutic target for chronic pain.

Published

2016

115. Sickness behavior induced by cisplatin chemotherapy and radiotherapy in a murine head and neck cancer model is associated with altered mitochondrial gene expression.

Author

Vichaya EG, Molkentine JM, Vermeer DW, Walker AK, Feng R, Holder G, Luu K, Mason RM, Saligan L, Heijnen CJ, Kavelaars A, Mason KA, Lee JH, and Dantzer R

Subjects

Animals, Brain drug effects, Brain immunology, Brain pathology, Brain radiation effects, Chemoradiotherapy, Cytokines metabolism, Gene Expression drug effects, Gene Expression radiation effects, Head and Neck Neoplasms genetics, Head and Neck Neoplasms pathology, Head and Neck Neoplasms physiopathology, Illness Behavior physiology, Liver drug effects, Liver immunology, Liver pathology, Liver radiation effects, Male, Mice, Inbred C57BL, Mitochondria drug effects, Mitochondria metabolism, Mitochondria radiation effects, Motivation drug effects, Motivation physiology, Motivation radiation effects, Motor Activity drug effects, Motor Activity physiology, Motor Activity radiation effects, Neoplasm Transplantation, Oropharyngeal Neoplasms genetics, Oropharyngeal Neoplasms pathology, Oropharyngeal Neoplasms physiopathology, Oropharyngeal Neoplasms therapy, Papillomaviridae, Radiation-Sensitizing Agents pharmacology, Antineoplastic Agents pharmacology, Cisplatin pharmacology, Genes, Mitochondrial drug effects, Genes, Mitochondrial radiation effects, Head and Neck Neoplasms therapy, Illness Behavior drug effects, Illness Behavior radiation effects

Abstract

The present study was undertaken to explore the possible mechanisms of the behavioral alterations that develop in response to cancer and to cancer therapy. For this purpose we used a syngeneic heterotopic mouse model of human papilloma virus (HPV)-related head and neck cancer in which cancer therapy is curative. Mice implanted or not with HPV+ tumor cells were exposed to sham treatment or a regimen of cisplatin and radiotherapy (chemoradiation). Sickness was measured by body weight loss and reduced food intake. Motivation was measured by burrowing, a highly prevalent species specific behavior. Tumor-bearing mice showed a gradual decrease in burrowing over time and increased brain and liver inflammatory cytokine mRNA expression by 28 days post tumor implantation. Chemoradiation administered to healthy mice resulted in a mild decrease in burrowing, body weight, and food intake. Chemoradiation in tumor-bearing mice decreased tumor growth and abrogated liver and brain inflammation, but failed to attenuate burrowing deficits. PCR array analysis of selected hypoxia and mitochondrial genes revealed that both the tumor and chemoradiation altered the expression of genes involved in mitochondrial energy metabolism within the liver and brain and increased expression of genes related to HIF-1α signaling within the brain. The most prominent changes in brain mitochondrial genes were noted in tumor-bearing mice treated with chemoradiation. These findings indicate that targeting mitochondrial dysfunction following cancer and cancer therapy may be a strategy for prevention of cancer-related symptoms., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2016

116. Impaired oligodendrocyte maturation in preterm infants: Potential therapeutic targets.

Author

van Tilborg E, Heijnen CJ, Benders MJ, van Bel F, Fleiss B, Gressens P, and Nijboer CH

Subjects

Animals, Brain drug effects, Brain pathology, Humans, Leukoencephalopathies pathology, Leukoencephalopathies physiopathology, Leukoencephalopathies therapy, Neurogenesis drug effects, Neurogenesis physiology, Oligodendroglia drug effects, Oligodendroglia pathology, Brain physiopathology, Infant, Premature physiology, Oligodendroglia physiology

Abstract

Preterm birth is an evolving challenge in neonatal health care. Despite declining mortality rates among extremely premature neonates, morbidity rates remain very high. Currently, perinatal diffuse white matter injury (WMI) is the most commonly observed type of brain injury in preterm infants and has become an important research area. Diffuse WMI is associated with impaired cognitive, sensory and psychological functioning and is increasingly being recognized as a risk factor for autism-spectrum disorders, ADHD, and other psychological disturbances. No treatment options are currently available for diffuse WMI and the underlying pathophysiological mechanisms are far from being completely understood. Preterm birth is associated with maternal inflammation, perinatal infections and disrupted oxygen supply which can affect the cerebral microenvironment by causing activation of microglia, astrogliosis, excitotoxicity, and oxidative stress. This intricate interplay of events negatively influences oligodendrocyte development, causing arrested oligodendrocyte maturation or oligodendrocyte cell death, which ultimately results in myelination failure in the developing white matter. This review discusses the current state in perinatal WMI research, ranging from a clinical perspective to basic molecular pathophysiology. The complex regulation of oligodendrocyte development in healthy and pathological conditions is described, with a specific focus on signaling cascades that may play a role in WMI. Furthermore, emerging concepts in the field of WMI and issues regarding currently available animal models are put forward. Novel insights into the molecular mechanisms underlying impeded oligodendrocyte maturation in diffuse WMI may aid the development of novel treatment options which are desperately needed to improve the quality-of-life of preterm neonates., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2016

117. Assessment of long-term safety and efficacy of intranasal mesenchymal stem cell treatment for neonatal brain injury in the mouse.

Author

Donega V, Nijboer CH, van Velthoven CT, Youssef SA, de Bruin A, van Bel F, Kavelaars A, and Heijnen CJ

Subjects

Animals, Animals, Newborn, Behavior, Animal, Biomarkers metabolism, Brain metabolism, Brain pathology, Brain physiopathology, Cells, Cultured, Cognition, Disease Models, Animal, Hypoxia-Ischemia, Brain metabolism, Hypoxia-Ischemia, Brain pathology, Hypoxia-Ischemia, Brain physiopathology, Hypoxia-Ischemia, Brain psychology, Mesenchymal Stem Cell Transplantation adverse effects, Mice, Inbred C57BL, Motor Activity, Myelin Basic Protein metabolism, Recognition, Psychology, Recovery of Function, Risk Assessment, Time Factors, Brain surgery, Hypoxia-Ischemia, Brain surgery, Mesenchymal Stem Cell Transplantation methods, Microtubule-Associated Proteins metabolism

Abstract

Background: For clinical translation, we assessed whether intranasal mesenchymal stem cell (MSC) treatment after hypoxia-ischemia (HI) induces neoplasia in the brain or periphery at 14 mo. Furthermore, the long-term effects of MSCs on behavior and lesion size were determined., Method: HI was induced in 9-d-old mice. Pups received an intranasal administration of 0.5 × 10(6) MSCs or vehicle at 10 d post-HI. Full macroscopical and microscopical pathological analysis of 39 organs per mouse was performed. Sensorimotor behavior was assessed in the cylinder-rearing test at 10 d, 28 d, 6 mo, and 9 mo. Cognition was measured with the novel object recognition test at 3 and 14 mo post-HI. Lesion size was determined by analyzing mouse-anti-microtubule-associated protein 2 (MAP2) and mouse-anti-myelin basic protein (MBP) staining at 5 wk and 14 mo., Results: At 14 mo post-HI, we did not observe any neoplasia in the nasal turbinates, brain, or other organs of HI mice treated with MSCs. Furthermore, our results show that MSC-induced improvement of sensorimotor and cognitive function is long lasting. In contrast, HI-vehicle mice showed severe behavioral impairment. Recovery of MAP2- and MBP-positive area lasted up to 14 mo following MSC treatment., Conclusion: Our results provide strong evidence of the long-term safety and positive effects of MSC treatment following neonatal HI in mice.

Published

2015

118. Prevention of chemotherapy-induced peripheral neuropathy by the small-molecule inhibitor pifithrin-μ.

Author

Krukowski K, Nijboer CH, Huo X, Kavelaars A, and Heijnen CJ

Subjects

Animals, Cisplatin toxicity, Disease Models, Animal, Female, Ganglia, Spinal pathology, Humans, Hyperalgesia drug therapy, Hyperalgesia etiology, Mice, Mice, Inbred C57BL, Microscopy, Electron, Transmission, Mitochondria pathology, Mitochondria ultrastructure, Pain Measurement, Pain Threshold drug effects, Peripheral Nervous System Diseases pathology, Ubiquitin Thiolesterase metabolism, Xenograft Model Antitumor Assays, Analgesics therapeutic use, Antineoplastic Agents, Phytogenic adverse effects, Paclitaxel adverse effects, Peripheral Nervous System Diseases chemically induced, Peripheral Nervous System Diseases prevention & control, Sulfonamides therapeutic use

Abstract

Chemotherapy-induced peripheral neuropathy (CIPN) is a common side effect of cancer treatment. It is the most frequent cause of dose reduction or treatment discontinuation in patients treated for cancer with commonly used drugs including taxanes and platinum-based compounds. No FDA-approved treatments for CIPN are available. In rodents, CIPN is represented by peripheral mechanical allodynia in association with retraction of intraepidermal nerve fibers. The mechanism of chemotherapy-induced neurotoxicity is unclear, but it has been established that mitochondrial dysfunction is an important component of the dysregulation in peripheral sensory neurons. We have shown earlier that inhibition of mitochondrial p53 accumulation with the small compound pifithrin-μ (PFT-μ) prevents cerebral neuronal death in a rodent model of hypoxic-ischemic brain damage. We now explore whether PFT-μ is capable of preventing neuronal mitochondrial damage and CIPN in mice. We demonstrate for the first time that PFT-μ prevents both paclitaxel- and cisplatin-induced mechanical allodynia. Electron microscopic analysis of peripheral sensory nerves revealed that PFT-μ secured mitochondrial integrity in paclitaxel-treated mice. In addition, PFT-μ administration protects against chemotherapy-induced loss of intraepidermal nerve fibers in the paw. To determine whether neuroprotective treatment with PFT-μ would interfere with the antitumor effects of chemotherapy, ovarian tumor cells were cultured in vitro with PFT-μ and paclitaxel. Pifithrin-μ does not inhibit tumor cell death but even enhances paclitaxel-induced tumor cell death. These data are the first to identify PFT-μ as a potential therapeutic strategy for prevention of CIPN to combat one of the most devastating side effects of chemotherapy.

Published

2015

119. Reversal of diet-induced obesity and insulin resistance by inducible genetic ablation of GRK2.

Author

Vila-Bedmar R, Cruces-Sande M, Lucas E, Willemen HL, Heijnen CJ, Kavelaars A, Mayor F Jr, and Murga C

Subjects

Animals, G-Protein-Coupled Receptor Kinase 2 genetics, Glucose genetics, Humans, Mice, Mice, Knockout, Obesity etiology, Obesity genetics, Obesity pathology, Adiposity, G-Protein-Coupled Receptor Kinase 2 metabolism, Glucose metabolism, Insulin Resistance, Obesity metabolism

Abstract

Insulin resistance is a common feature of obesity and predisposes individuals to various prevalent pathological conditions. G protein (heterotrimeric guanine nucleotide-binding protein)-coupled receptor kinase 2 (GRK2) integrates several signal transduction pathways and is emerging as a physiologically relevant inhibitor of insulin signaling. GRK2 abundance is increased in humans with metabolic syndrome and in different murine models of insulin resistance. To support GRK2 as a potential drug target in type 2 diabetes and obesity, we investigated whether lowering GRK2 abundance reversed an ongoing systemic insulin-resistant phenotype, using a mouse model of tamoxifen-induced GRK2 ablation after high-fat diet-dependent obesity and insulin resistance. Tamoxifen-triggered GRK2 deletion impeded further body weight gain, normalized fasting glycemia, improved glucose tolerance, and was associated with preserved insulin sensitivity in skeletal muscle and liver, thereby maintaining whole-body glucose homeostasis. Moreover, when continued to be fed a high-fat diet, these animals displayed reduced fat mass and smaller adipocytes, were resistant to the development of liver steatosis, and showed reduced expression of proinflammatory markers in the liver. Our results indicate that GRK2 acts as a hub to control metabolic functions in different tissues, which is key to controlling insulin resistance development in vivo. These data suggest that inhibiting GRK2 could reverse an established insulin-resistant and obese phenotype, thereby putting forward this enzyme as a potential therapeutic target linking glucose homeostasis and regulation of adiposity., (Copyright © 2015, American Association for the Advancement of Science.)

Published

2015

120. Peripheral indoleamine 2,3-dioxygenase 1 is required for comorbid depression-like behavior but does not contribute to neuropathic pain in mice.

Author

Zhou W, Dantzer R, Budac DP, Walker AK, Mao-Ying QL, Lee AW, Heijnen CJ, and Kavelaars A

Subjects

Animals, Brain metabolism, Depression complications, Depression genetics, Disease Models, Animal, Indoleamine-Pyrrole 2,3,-Dioxygenase genetics, Male, Mice, Motor Activity physiology, Neuralgia complications, Neuralgia genetics, Spinal Cord metabolism, Behavior, Animal physiology, Depression metabolism, Indoleamine-Pyrrole 2,3,-Dioxygenase metabolism, Liver metabolism, Neuralgia metabolism

Abstract

Chronic pain frequently co-occurs with major depressive disorder but the mechanisms are poorly understood. We investigated the contribution of indoleamine 2,3-dioxygenase-1 (IDO1), a rate-limiting enzyme in the conversion of tryptophan to neurotoxic metabolites, to this comorbidity using the spared nerve injury (SNI) model of neuropathic pain in mice. SNI resulted in unilateral mechanical allodynia, reduced social interaction, and increased immobility in the forced swim test without changes in locomotor activity. These findings indicate SNI-induced pain and comorbid depression-like behavior. These behavioral responses were accompanied by increases in plasma kynurenine/tryptophan ratios and increased expression of Ido1 and Il1b mRNA in the liver. Interestingly, SNI did not induce detectable changes in spinal cord or brain Ido1 mRNA levels. SNI was associated with spinal cord inflammatory activity as evidenced by increased Il1b mRNA expression. The SNI-induced increase of liver Ido1and Il1b mRNA was abrogated by intrathecal administration of the IL-1 inhibitor IL-1RA. Intrathecal IL-1RA also inhibited both mechanical allodynia and depression-like behavior. We also show that Ido1 is required for the development of depression-like behavior because Ido1(-/-) mice do not develop increased immobility in the forced swim test or decreased social exploration in response to SNI. Mechanical allodynia was similar in WT and Ido1(-/-) mice. In conclusion, our findings show for the first time that neuropathic pain is associated with an increase of Ido1 in liver, but not brain, downstream of spinal cord IL-1β signaling and that Ido1 mediates comorbid depression. Moreover, comorbidity of neuropathic pain and depression are only partially mediated by a common mechanism because mechanical hyperalgesia develops independently of Ido1., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2015

121. Mechanisms of chemotherapy-induced behavioral toxicities.

Author

Vichaya EG, Chiu GS, Krukowski K, Lacourt TE, Kavelaars A, Dantzer R, Heijnen CJ, and Walker AK

Abstract

While chemotherapeutic agents have yielded relative success in the treatment of cancer, patients are often plagued with unwanted and even debilitating side-effects from the treatment which can lead to dose reduction or even cessation of treatment. Common side effects (symptoms) of chemotherapy include (i) cognitive deficiencies such as problems with attention, memory and executive functioning; (ii) fatigue and motivational deficit; and (iii) neuropathy. These symptoms often develop during treatment but can remain even after cessation of chemotherapy, severely impacting long-term quality of life. Little is known about the underlying mechanisms responsible for the development of these behavioral toxicities, however, neuroinflammation is widely considered to be one of the major mechanisms responsible for chemotherapy-induced symptoms. Here, we critically assess what is known in regards to the role of neuroinflammation in chemotherapy-induced symptoms. We also argue that, based on the available evidence, neuroinflammation is unlikely the only mechanism involved in the pathogenesis of chemotherapy-induced behavioral toxicities. We evaluate two other putative candidate mechanisms. To this end we discuss the mediating role of damage-associated molecular patterns (DAMPs) activated in response to chemotherapy-induced cellular damage. We also review the literature with respect to possible alternative mechanisms such as a chemotherapy-induced change in the bioenergetic status of the tissue involving changes in mitochondrial function in relation to chemotherapy-induced behavioral toxicities. Understanding the mechanisms that underlie the emergence of fatigue, neuropathy, and cognitive difficulties is vital to better treatment and long-term survival of cancer patients.

Published

2015

122. Neonatal glucocorticoid treatment: long-term effects on the hypothalamus-pituitary-adrenal axis, immune system, and problem behavior in 14-17 year old adolescents.

Author

Ter Wolbeek M, Kavelaars A, de Vries WB, Tersteeg-Kamperman M, Veen S, Kornelisse RF, van Weissenbruch M, Baerts W, Liem KD, van Bel F, and Heijnen CJ

Subjects

Adolescent, Aggression psychology, Anxiety psychology, Case-Control Studies, Cohort Studies, Depression psychology, Dexamethasone therapeutic use, Female, Gestational Age, Humans, Hydrocortisone therapeutic use, Hypothalamo-Hypophyseal System physiopathology, Immune System metabolism, Immune System physiopathology, Infant, Newborn, Infant, Premature, Interferon-gamma immunology, Interleukin-10 immunology, Interleukin-4 immunology, Interleukin-6 immunology, Longitudinal Studies, Male, Pituitary-Adrenal System physiopathology, Saliva chemistry, Sex Factors, Stress, Psychological physiopathology, Tumor Necrosis Factor-alpha immunology, Adrenocorticotropic Hormone metabolism, Bronchopulmonary Dysplasia prevention & control, Cytokines immunology, Glucocorticoids therapeutic use, Hydrocortisone metabolism, Hypothalamo-Hypophyseal System metabolism, Pituitary-Adrenal System metabolism, Stress, Psychological metabolism

Abstract

Neonatal glucocorticoid (GC) treatment is used to prevent bronchopulmonary dysplasia (BPD) in prematurely born babies. In the 1990s, treatment regimens with relatively high doses of dexamethasone (DEX) were common. As an alternative, hydrocortisone (HC) was used. Earlier, we compared long-term effects of both GCs in children aged 7-10 and detected adverse effects of neonatal DEX treatment, but not of HC, on a range of outcomes. The aim of the current cohort study was to investigate whether long-term effects of neonatal DEX were maintained and whether effects of HC remained absent at adolescent age (14-17years). We compared 71 DEX-treated and 67 HC-treated adolescents. In addition, 71 adolescents who were not neonatally treated with GCs participated. All were born <32weeks of gestation. DEX-treated girls showed increased adrenocorticotropic hormone (ACTH) and cortisol responses in the Trier Social Stress Test. The cortisol awakening response was lower in HC-treated participants compared to untreated participants. Negative feedback function of the HPA-axis in the dexamethasone suppression test did not differ between groups. In contrast to our observations at the age of 7-10years, we did not observe group differences in mitogen-induced cytokine production at the age of 14-17years. DEX-treated girls showed more social problems and anxious/depressed behavior than HC-treated girls. Untreated girls showed more problem behavior as well. In conclusion, our results suggest that, especially in girls, neonatal DEX has a programming effect on the HPA-axis and on the ability to adjust to the environment. The loss of group differences on immune system measures indicate that potentially negative effects detected at a younger age subsided., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2015

123. Cytokine production as a putative biological mechanism underlying stress sensitization in high combat exposed soldiers.

Author

Smid GE, van Zuiden M, Geuze E, Kavelaars A, Heijnen CJ, and Vermetten E

Subjects

Adult, Afghan Campaign 2001-, Combat Disorders diagnosis, Humans, Life Change Events, Middle Aged, Models, Theoretical, Netherlands, Prospective Studies, Risk Factors, Stress Disorders, Post-Traumatic diagnosis, Stress, Psychological diagnosis, Young Adult, Combat Disorders metabolism, Cytokines metabolism, Military Personnel psychology, Stress Disorders, Post-Traumatic metabolism, Stress, Psychological metabolism

Abstract

Objective: Combat stress exposed soldiers may respond to post-deployment stressful life events (SLE) with increases in symptoms of posttraumatic stress disorder (PTSD), consistent with a model of stress sensitization. Several lines of research point to sensitization as a model to describe the relations between exposure to traumatic events, subsequent SLE, and symptoms of PTSD. Based on previous findings we hypothesized that immune activation, measured as a high in vitro capacity of leukocytes to produce cytokines upon stimulation, underlies stress sensitization., Methods: We assessed mitogen-induced cytokine production at 1 month, SLE at 1 year, and PTSD symptoms from 1 month up to 2 years post-deployment in soldiers returned from deployment to Afghanistan (N=693). Exploratory structural equation modeling as well as latent growth models were applied., Results: The data demonstrated significant three-way interaction effects of combat stress exposure, cytokine production, and post-deployment SLE on linear change in PTSD symptoms over the first 2 years following return from deployment. In soldiers reporting high combat stress exposure, both high mitogen-stimulated T-cell cytokine production and high innate cytokine production were associated with increases in PTSD symptoms in response to post-deployment SLE. In low combat stress exposed soldiers as well as those with low cytokine production, post-deployment SLE were not associated with increases in PTSD symptoms., Conclusion: High stimulated T-cell and innate cytokine production may contribute to stress sensitization in recently deployed, high combat stress exposed soldiers. These findings suggest that detecting and eventually normalizing immune activation may potentially complement future strategies to prevent progression of PTSD symptoms following return from deployment., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

124. The neonatal brain is not protected by osteopontin peptide treatment after hypoxia-ischemia.

Author

Bonestroo HJ, Nijboer CH, van Velthoven CT, van Bel F, and Heijnen CJ

Subjects

Administration, Intranasal, Animals, Animals, Newborn, Behavior, Animal drug effects, Disease Models, Animal, Female, Infusions, Intralesional, Injections, Intraperitoneal, Male, Mice, Mice, Inbred C57BL, Hypoxia-Ischemia, Brain drug therapy, Neuroprotective Agents, Osteopontin administration & dosage, Osteopontin pharmacology

Abstract

Neonatal encephalopathy due to perinatal hypoxia-ischemia (HI) is a severe condition, and current treatment options are limited. Expression of endogenous osteopontin (OPN), a multifunction glycoprotein, is strongly upregulated in the brain after neonatal HI. Intracerebrally administered OPN has been shown to be neuroprotective following experimental neonatal HI and adult stroke. In the present study, we determined whether intranasal, intraperitoneal or intracerebral treatment with a smaller TAT-OPN peptide is neuroprotective in neonatal mice with HI brain damage. The TAT-OPN peptide exerts bioactivity as it was as potent as full-length OPN in inducing cell adhesion in an in vitro adhesion assay. Intranasal administration of TAT-OPN peptide immediately after HI (T0) or in a repetitive treatment schedule of T0, 3 h, day (D) 1, 2 and 3 after HI did not protect cerebral gray or white matter after HI. Intraperitoneal TAT-OPN treatment at T0 or in two extended treatment schedules (D5, 7, 9, 11, 13, 15 after HI or T0, D1, 3, 5, 7, 9, 11, 13 and 15 after HI) did not result in neuroprotection either. Moreover, no functional improvement (cylinder rearing test and adhesive removal task) was observed following TAT-OPN treatment in any of the intraperitoneal treatment schedules. We validated that the TAT-OPN peptide reached the brain after intranasal or intraperitoneal administration by using an HIV-TAT staining. Finally, also intracerebral administration of the TAT-OPN peptide 1 h after HI did not reduce cerebral damage. Our data show that administration of the TAT-OPN peptide did not exert neuroprotective effects on neonatal HI-induced brain injury or sensorimotor behavioral deficits., (© 2015 S. Karger AG, Basel.)

Published

2015

125. Development of cerebral gray and white matter injury and cerebral inflammation over time after inflammatory perinatal asphyxia.

Author

Bonestroo HJ, Heijnen CJ, Groenendaal F, van Bel F, and Nijboer CH

Subjects

Animals, Animals, Newborn, Disease Models, Animal, Female, Gray Matter injuries, Hypoxia pathology, Hypoxia-Ischemia, Brain pathology, Inflammation drug therapy, Inflammation pathology, Mice, Inbred C57BL, Microglia drug effects, Microglia metabolism, Pregnancy, White Matter injuries, Asphyxia drug therapy, Gray Matter drug effects, Lipopolysaccharides pharmacology, White Matter drug effects

Abstract

Antenatal inflammation is associated with increased severity of hypoxic-ischemic (HI) encephalopathy and adverse outcome in human neonates and experimental rodents. We investigated the effect of lipopolysaccharide (LPS) on the timing of HI-induced cerebral tissue loss and gray matter injury, white matter injury and integrity, and the cerebral inflammatory response. On postnatal day 9, mice underwent HI by unilateral carotid artery occlusion followed by systemic hypoxia which resulted in early neuronal damage (MAP2 loss) at 3 h that did not increase up to day 15. LPS injection 14 h before HI (LPS+HI) significantly and gradually aggravated MAP2 loss from 3 h up to day 15, resulting in an acellular cystic lesion. LPS+HI increased white matter damage, reduced myelination in the corpus callosum and increased white matter fiber coherency in the cingulum. The number of oligodendrocytes throughout the lineage (Olig2-positive) was increased whereas more mature myelinating (CNPase-positive) oligodendrocytes were strongly decreased after LPS+HI. LPS+HI induced an increased and prolonged expression of cerebral cytokines/chemokines compared to HI. Additionally, LPS+HI increased macrophage/microglia activation and influx of neutrophils in the brain compared to HI. This study demonstrates the sensitizing effect of LPS on neonatal HI brain injury for an extended time-frame up to 15 days postinsult. LPS before HI induced a gradual increase in gray and white matter deficits, including reduced numbers of more mature myelinating oligodendrocytes and a decrease in white matter integrity. Moreover, LPS+HI prolonged and intensified the cerebral inflammatory response, including cellular infiltration. In conclusion, as the timing of damage and/or involved pathways are changed when HI is preceded by inflammation, experimental therapies might require modifications in the time window, dosage or combinations of therapies for efficacious neuroprotection., (© 2015 S. Karger AG, Basel.)

Published

2015

126. Intranasal administration of human MSC for ischemic brain injury in the mouse: in vitro and in vivo neuroregenerative functions.

Author

Donega V, Nijboer CH, Braccioli L, Slaper-Cortenbach I, Kavelaars A, van Bel F, and Heijnen CJ

Subjects

Administration, Intranasal, Animals, Cell Differentiation, Cell Movement, Glial Fibrillary Acidic Protein metabolism, Humans, Hypoxia-Ischemia, Brain pathology, Mice, Inbred C57BL, Motor Activity, Neural Stem Cells cytology, Neuroglia pathology, Organic Chemicals metabolism, Sensorimotor Cortex pathology, Hypoxia-Ischemia, Brain physiopathology, Hypoxia-Ischemia, Brain therapy, Mesenchymal Stem Cell Transplantation, Mesenchymal Stem Cells cytology, Nerve Regeneration

Abstract

Intranasal treatment with C57BL/6 MSCs reduces lesion volume and improves motor and cognitive behavior in the neonatal hypoxic-ischemic (HI) mouse model. In this study, we investigated the potential of human MSCs (hMSCs) to treat HI brain injury in the neonatal mouse. Assessing the regenerative capacity of hMSCs is crucial for translation of our knowledge to the clinic. We determined the neuroregenerative potential of hMSCs in vitro and in vivo by intranasal administration 10 d post-HI in neonatal mice. HI was induced in P9 mouse pups. 1×10(6) or 2×10(6) hMSCs were administered intranasally 10 d post-HI. Motor behavior and lesion volume were measured 28 d post-HI. The in vitro capacity of hMSCs to induce differentiation of mouse neural stem cell (mNSC) was determined using a transwell co-culture differentiation assay. To determine which chemotactic factors may play a role in mediating migration of MSCs to the lesion, we performed a PCR array on 84 chemotactic factors 10 days following sham-operation, and at 10 and 17 days post-HI. Our results show that 2×10(6) hMSCs decrease lesion volume, improve motor behavior, and reduce scar formation and microglia activity. Moreover, we demonstrate that the differentiation assay reflects the neuroregenerative potential of hMSCs in vivo, as hMSCs induce mNSCs to differentiate into neurons in vitro. We also provide evidence that the chemotactic factor CXCL10 may play an important role in hMSC migration to the lesion site. This is suggested by our finding that CXCL10 is significantly upregulated at 10 days following HI, but not at 17 days after HI, a time when MSCs no longer reach the lesion when given intranasally. The results described in this work also tempt us to contemplate hMSCs not only as a potential treatment option for neonatal encephalopathy, but also for a plethora of degenerative and traumatic injuries of the nervous system.

Published

2014

127. Intranasally administered mesenchymal stem cells promote a regenerative niche for repair of neonatal ischemic brain injury.

Author

Donega V, Nijboer CH, van Tilborg G, Dijkhuizen RM, Kavelaars A, and Heijnen CJ

Subjects

Administration, Intranasal, Animals, Animals, Newborn, Brain Injuries etiology, Brain-Derived Neurotrophic Factor genetics, Brain-Derived Neurotrophic Factor metabolism, Cell Differentiation, Cell Proliferation, Coculture Techniques, Doublecortin Protein, Fluorescent Dyes, Functional Laterality, Ischemia complications, Mice, Mice, Inbred C57BL, Nerve Growth Factor genetics, Nerve Growth Factor metabolism, Nerve Tissue Proteins metabolism, Neuroglia physiology, Organic Chemicals, Time Factors, Brain Injuries surgery, Mesenchymal Stem Cells physiology, Nerve Regeneration physiology

Abstract

Previous work from our group has shown that intranasal MSC-treatment decreases lesion volume and improves motor and cognitive behavior after hypoxic-ischemic (HI) brain damage in neonatal mice. Our aim was to determine the kinetics of MSC migration after intranasal administration, and the early effects of MSCs on neurogenic processes and gliosis at the lesion site. HI brain injury was induced in 9-day-old mice and MSCs were administered intranasally at 10days post-HI. The kinetics of MSC migration were investigated by immunofluorescence and MRI analysis. BDNF and NGF gene expression was determined by qPCR analysis following MSC co-culture with HI brain extract. Nestin, Doublecortin, NeuN, GFAP, Iba-1 and M1/M2 phenotypic expression was assessed over time. MRI and immunohistochemistry analyses showed that MSCs reach the lesion site already within 2h after intranasal administration. At 12h after administration the number of MSCs at the lesion site peaks and decreases significantly at 72h. The number of DCX(+) cells increased 1 to 3days after MSC administration in the SVZ. At the lesion, GFAP(+)/nestin(+) and DCX(+) expression increased 3 to 5days after MSC-treatment. The number of NeuN(+) cells increased within 5days, leading to a dramatic regeneration of the somatosensory cortex and hippocampus at 18days after intranasal MSC administration. Interestingly, MSCs expressed significantly more BDNF gene when exposed to HI brain extract in vitro. Furthermore, MSC-treatment resulted in the resolution of the glial scar surrounding the lesion, represented by a decrease in reactive astrocytes and microglia and polarization of microglia towards the M2 phenotype. In view of the current lack of therapeutic strategies, we propose that intranasal MSC administration is a powerful therapeutic option through its functional repair of the lesion represented by regeneration of the cortical and hippocampal structure and decrease of gliosis., (Copyright © 2014. Published by Elsevier Inc.)

Published

2014

128. Association between brain natriuretic peptide, markers of inflammation and the objective and subjective response to cardiac resynchronization therapy.

Author

Brouwers C, Versteeg H, Meine M, Heijnen CJ, Kavelaars AM, Pedersen SS, and Mommersteeg PM

Subjects

Aged, Biomarkers blood, Female, Follow-Up Studies, Humans, Male, Middle Aged, Surveys and Questionnaires, Treatment Outcome, Cardiac Resynchronization Therapy psychology, Cytokines blood, Inflammation blood, Natriuretic Peptide, Brain blood

Abstract

Introduction: Studies suggest that cardiac resynchronization therapy (CRT) can induce a decrease in brain natriuretic peptide (BNP) and systemic inflammation, which may be associated with CRT-response. However, the evidence is inconclusive. We examined levels of BNP and inflammatory markers from pre-CRT implantation to 14months follow-up in CRT-responders and nonresponders, defined by two response criteria., Methods: We studied 105 heart failure patients implanted with a CRT-defibrillator (68% men; age=65.4±10.1years). The objective CRT-response was defined as a reduction of ⩾15% in left ventricular end systolic volume; subjective CRT-response was defined as an improvement of ⩾10 points in patient-reported health status assessed with the Kansas City Cardiomyopathy Questionnaire. Plasma BNP and markers of inflammation (CRP, IL-6, TNFα, sTNFr1 and sTNFr2) were measured at three time points., Results: Pre-implantation concentrations of TNFα were significantly lower for subjective responders compared to nonresponders (p=.05), but there was no difference in BNP and the other inflammatory markers at baseline. Objective CRT-response was significantly associated with lower BNP levels over time (F=27.31, p<.001), and subjective CRT-response with lower TNFα levels (F=5.67, p=.019)., Conclusion: Objective and subjective response to CRT was associated with lower levels of BNP and TNFα, respectively, but not with other markers of inflammation. This indicates that response to CRT is not automatically related to a stronger overall decrease in inflammation. Large-scale studies are warranted that further examine the relation between the clinical effects of CRT on inflammatory markers, as the latter have been associated with poor prognosis in heart failure., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

129. The anti-diabetic drug metformin protects against chemotherapy-induced peripheral neuropathy in a mouse model.

Author

Mao-Ying QL, Kavelaars A, Krukowski K, Huo XJ, Zhou W, Price TJ, Cleeland C, and Heijnen CJ

Subjects

Animals, Cisplatin adverse effects, Disease Models, Animal, Hyperalgesia chemically induced, Hyperalgesia complications, Hyperalgesia drug therapy, Hypoglycemic Agents pharmacology, Metformin pharmacology, Mice, Inbred C57BL, Nerve Fibers drug effects, Nerve Fibers pathology, Neuralgia chemically induced, Neuralgia complications, Neuralgia drug therapy, Paclitaxel adverse effects, Peripheral Nervous System Diseases complications, Protective Agents pharmacology, Hypoglycemic Agents therapeutic use, Metformin therapeutic use, Peripheral Nervous System Diseases chemically induced, Peripheral Nervous System Diseases drug therapy, Protective Agents therapeutic use

Abstract

Chemotherapy-induced peripheral neuropathy (CIPN) characterized by loss of sensory sensitivity and pain in hands and feet is the major dose-limiting toxicity of many chemotherapeutics. At present, there are no FDA-approved treatments for CIPN. The anti-diabetic drug metformin is the most widely used prescription drug in the world and improves glycemic control in diabetes patients. There is some evidence that metformin enhances the efficacy of cancer treatment. The aim of this study was to test the hypothesis that metformin protects against chemotherapy-induced neuropathic pain and sensory deficits. Mice were treated with cisplatin together with metformin or saline. Cisplatin induced increased sensitivity to mechanical stimulation (mechanical allodynia) as measured using the von Frey test. Co-administration of metformin almost completely prevented the cisplatin-induced mechanical allodynia. Co-administration of metformin also prevented paclitaxel-induced mechanical allodynia. The capacity of the mice to detect an adhesive patch on their hind paw was used as a novel indicator of chemotherapy-induced sensory deficits. Co-administration of metformin prevented the cisplatin-induced increase in latency to detect the adhesive patch indicating that metformin prevents sensory deficits as well. Moreover, metformin prevented the reduction in density of intra-epidermal nerve fibers (IENFs) in the paw that develops as a result of cisplatin treatment. We conclude that metformin protects against pain and loss of tactile function in a mouse model of CIPN. The finding that metformin reduces loss of peripheral nerve endings indicates that mechanism underlying the beneficial effects of metformin includes a neuroprotective activity. Because metformin is widely used for treatment of type II diabetes, has a broad safety profile, and is currently being tested as an adjuvant drug in cancer treatment, clinical translation of these findings could be rapidly achieved.

Published

2014

130. Monocytes/Macrophages control resolution of transient inflammatory pain.

Author

Willemen HL, Eijkelkamp N, Garza Carbajal A, Wang H, Mack M, Zijlstra J, Heijnen CJ, and Kavelaars A

Subjects

Animals, Carrageenan, Cells, Cultured, Female, G-Protein-Coupled Receptor Kinase 2 genetics, G-Protein-Coupled Receptor Kinase 2 metabolism, Gene Knockout Techniques, Hot Temperature, Interleukin-10 genetics, Interleukin-10 metabolism, Interleukin-1beta, Mice, Inbred C57BL, Mice, Transgenic, Touch, Hyperalgesia physiopathology, Inflammation physiopathology, Macrophages physiology, Monocytes physiology, Pain physiopathology

Abstract

Unlabelled: Insights into mechanisms governing resolution of inflammatory pain are of great importance for many chronic pain-associated diseases. Here we investigate the role of macrophages/monocytes and the anti-inflammatory cytokine interleukin-10 (IL-10) in the resolution of transient inflammatory pain. Depletion of mice from peripheral monocytes/macrophages delayed resolution of intraplantar IL-1β- and carrageenan-induced inflammatory hyperalgesia from 1 to 3 days to >1 week. Intrathecal administration of a neutralizing IL-10 antibody also markedly delayed resolution of IL-1β- and carrageenan-induced inflammatory hyperalgesia. Recently, we showed that IL-1β- and carrageenan-induced hyperalgesia is significantly prolonged in LysM-GRK2(+/-) mice, which have reduced levels of G-protein-coupled receptor kinase 2 (GRK2) in LysM(+) myeloid cells. Here we show that adoptive transfer of wild-type, but not of GRK2(+/-), bone marrow-derived monocytes normalizes the resolution of IL-1β-induced hyperalgesia in LysM-GRK2(+/-) mice. Adoptive transfer of IL-10(-/-) bone marrow-derived monocytes failed to normalize the duration of IL-1β-induced hyperalgesia in LysM-GRK2(+/-) mice. Mechanistically, we show that GRK2(+/-) macrophages produce less IL-10 in vitro. In addition, intrathecal IL-10 administration attenuated IL-1β-induced hyperalgesia in LysM-GRK2(+/-) mice, whereas it had no effect in wild-type mice. Our data uncover a key role for monocytes/macrophages in promoting resolution of inflammatory hyperalgesia via a mechanism dependent on IL-10 signaling in dorsal root ganglia., Perspective: We show that IL-10-producing monocytes/macrophages promote resolution of transient inflammatory hyperalgesia. Additionally, we show that reduced monocyte/macrophage GRK2 impairs resolution of hyperalgesia and reduces IL-10 production. We propose that low GRK2 expression and/or impaired IL-10 production by monocytes/macrophages represent peripheral biomarkers for the risk of developing chronic pain after inflammation., (Published by Elsevier Inc.)

Published

2014

131. Long-term functional consequences and ongoing cerebral inflammation after subarachnoid hemorrhage in the rat.

Author

Kooijman E, Nijboer CH, van Velthoven CT, Mol W, Dijkhuizen RM, Kesecioglu J, and Heijnen CJ

Subjects

Animals, Brain Damage, Chronic immunology, Cerebral Cortex immunology, Encephalitis immunology, Macrophages immunology, Male, Neutrophils immunology, Psychomotor Disorders immunology, Rats, Wistar, Recovery of Function, Subarachnoid Hemorrhage immunology, Cerebral Cortex pathology, Encephalitis physiopathology, Subarachnoid Hemorrhage physiopathology

Abstract

Subarachnoid hemorrhage (SAH) represents a considerable health problem with an incidence of 6-7 per 100.000 individuals per year in Western society. We investigated the long-term consequences of SAH on behavior, neuroinflammation and gray- and white-matter damage using an endovascular puncture model in Wistar rats. Rats were divided into a mild or severe SAH group based on their acute neurological score at 24 h post-SAH. The degree of hemorrhage determined in post-mortem brains at 48 h strongly correlated with the acute neurological score. Severe SAH induced increased TNF-α, IL-1β, IL-10, MCP-1, MIP2, CINC-1 mRNA expression and cortical neutrophil influx at 48 h post-insult. Neuroinflammation after SAH was very long-lasting and still present at day 21 as determined by Iba-1 staining (microglia/macrophages) and GFAP (astrocytes). Long-term neuroinflammation was strongly associated with the degree of severity of SAH. Cerebral damage to gray- and white-matter was visualized by immunohistochemistry for MAP2 and MBP at 21 days after SAH. Severe SAH induced significant gray- and white-matter damage. MAP2 loss at day 21 correlated significantly with the acute neurological score determined at 24 h post-SAH. Sensorimotor behavior, determined by the adhesive removal task and von Frey test, was affected after severe SAH at day 21. In conclusion, we are the first to show that SAH induces ongoing cortical inflammation. Moreover, SAH induces mainly cortical long-term brain damage, which is associated with long-term sensorimotor damage.

Published

2014

132. Therapeutic potential of genetically modified mesenchymal stem cells after neonatal hypoxic-ischemic brain damage.

Author

van Velthoven CT, Braccioli L, Willemen HL, Kavelaars A, and Heijnen CJ

Subjects

Administration, Intranasal, Animals, Animals, Newborn, Brain-Derived Neurotrophic Factor genetics, Brain-Derived Neurotrophic Factor metabolism, Calcium-Binding Proteins, Cell Differentiation, Cell Proliferation, EGF Family of Proteins, Genetic Vectors therapeutic use, Hedgehog Proteins genetics, Hedgehog Proteins metabolism, Hypoxia-Ischemia, Brain pathology, Mice, Mice, Inbred C57BL, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Oligodendroglia metabolism, Proteins genetics, Proteins metabolism, Transduction, Genetic, Treatment Outcome, Adenoviridae genetics, Genetic Vectors administration & dosage, Hypoxia-Ischemia, Brain therapy, Mesenchymal Stem Cells metabolism, Neural Stem Cells metabolism

Abstract

Mesenchymal stem cells (MSCs) have been shown to improve outcomes after neonatal hypoxic-ischemic (HI) brain injury possibly by secretion of growth factors stimulating repair processes. We investigated whether MSCs, modified to secrete specific growth factors, can further enhance recovery. Using an in vitro assay, we show that MSC-secreting brain derived neurotrophic factor (BDNF), epidermal growth factor-like 7 (EGFL7), persephin (PSP), or sonic hedgehog (SHH) regulate proliferation and differentiation of neural stem cells. Moreover, mice that received an intranasal application of 100,000 MSC-BDNF showed significantly improved outcomes as demonstrated by improved motor function and decreased lesion volume compared with mice treated with empty vector (EV) MSCs. Treatment with MSC-EGFL7 improved motor function but had no effect on lesion size. Treatment with MSC-PSP or MSC-SHH neither improved outcome nor reduced lesion size in comparison with MSC-EV-treated mice. Moreover, mice treated with MSC-SHH showed even decreased functional outcomes when compared with those treated with MSC-EV. Treatment with MSC-BDNF induced cell proliferation in the ischemic hemisphere lasting at least 18 days after MSC administration, whereas treatment with MSC-EV did not. These data suggest that gene-modified cell therapy might be a useful approach to consider for treatment of neonatal HI brain damage. However, care must be taken when selecting the agent to overexpress.

Published

2014

133. Inflammatory markers and development of symptom burden in patients with multiple myeloma during autologous stem cell transplantation.

Author

Wang XS, Shi Q, Shah ND, Heijnen CJ, Cohen EN, Reuben JM, Orlowski RZ, Qazilbash MH, Johnson VE, Williams LA, Mendoza TR, and Cleeland CS

Subjects

Adult, Aged, Biomarkers blood, Cytokines blood, Female, Hematopoietic Stem Cell Transplantation, Humans, Induction Chemotherapy, Leukocyte Count, Longitudinal Studies, Male, Middle Aged, Multiple Myeloma therapy, Neoplasm Staging, Severity of Illness Index, Time Factors, Transplantation, Autologous, Inflammation Mediators blood, Multiple Myeloma diagnosis, Multiple Myeloma metabolism

Abstract

Purpose: Increasing research suggests that inflammation mediates symptom development. In this longitudinal study, we examined inflammatory factors related to the development of high symptom burden during autologous hematopoietic stem cell transplant (AuSCT) for multiple myeloma., Experimental Design: Patients (n = 63) repeatedly reported symptom severity on the MD Anderson Symptom Inventory multiple myeloma module (MDASI-MM) and contributed blood samples periodically for up to 100 days after AuSCT for inflammatory marker assays. The temporal associations between serum inflammatory marker concentrations and symptom severity outcomes were examined by nonlinear mixed-effect modeling., Results: Fatigue, pain, disturbed sleep, lack of appetite, and drowsiness were consistently the most severe MDASI-MM symptoms during the study. Peak symptom severity occurred on day 8 after AuSCT, during white blood cell count nadir. Patterns of serum interleukin (IL)-6 (peak on day 9) and soluble IL-6 receptor (sIL-6R; nadir on day 8) expression paralleled symptom development over time (both P < 0.0001). By univariate analysis, serum IL-6, sIL-6R, IL-10, C-reactive protein, macrophage inflammatory protein (MIP)-1α, sIL-1R2, sIL-1RA, and soluble tumor necrosis factor receptor 1 were significantly related to the most severe symptoms during the first 30 days after AuSCT (all P < 0.05). By multivariate analysis, IL-6 (estimate = 0.170; P = 0.004) and MIP-1α (estimate = -0.172; P = 0.006) were temporally associated with the severity of the component symptom score., Conclusions: Systemic inflammatory response was associated with high symptom burden during the acute phase of AuSCT. Additional research is needed to understand how the inflammatory response is mechanistically associated with symptom expression and whether suppression of this response can reduce symptoms without compromising tumor control., (©2014 AACR)

Published

2014

134. Uterine selection of human embryos at implantation.

Author

Brosens JJ, Salker MS, Teklenburg G, Nautiyal J, Salter S, Lucas ES, Steel JH, Christian M, Chan YW, Boomsma CM, Moore JD, Hartshorne GM, Sućurović S, Mulac-Jericevic B, Heijnen CJ, Quenby S, Koerkamp MJ, Holstege FC, Shmygol A, and Macklon NS

Subjects

Animals, Calcium Signaling physiology, Cells, Cultured, Chromosome Aberrations embryology, Culture Media, Conditioned pharmacology, Endoplasmic Reticulum Stress genetics, Epithelial Cells metabolism, Female, Gene Expression Profiling, HSC70 Heat-Shock Proteins biosynthesis, HSC70 Heat-Shock Proteins genetics, Humans, Insulin-Like Growth Factor Binding Protein 1 metabolism, Mice, Mice, Inbred C57BL, Prolactin metabolism, RNA Interference, RNA, Small Interfering, Signal Transduction, Trypsin metabolism, Blastocyst physiology, Decidua cytology, Embryo Implantation physiology, Embryo, Mammalian physiology, Uterus physiology

Abstract

Human embryos frequently harbor large-scale complex chromosomal errors that impede normal development. Affected embryos may fail to implant although many first breach the endometrial epithelium and embed in the decidualizing stroma before being rejected via mechanisms that are poorly understood. Here we show that developmentally impaired human embryos elicit an endoplasmic stress response in human decidual cells. A stress response was also evident upon in vivo exposure of mouse uteri to culture medium conditioned by low-quality human embryos. By contrast, signals emanating from developmentally competent embryos activated a focused gene network enriched in metabolic enzymes and implantation factors. We further show that trypsin, a serine protease released by pre-implantation embryos, elicits Ca(2+) signaling in endometrial epithelial cells. Competent human embryos triggered short-lived oscillatory Ca(2+) fluxes whereas low-quality embryos caused a heightened and prolonged Ca(2+) response. Thus, distinct positive and negative mechanisms contribute to active selection of human embryos at implantation.

Published

2014

135. Exosomes: a new weapon to treat the central nervous system.

Author

Braccioli L, van Velthoven C, and Heijnen CJ

Subjects

Animals, Brain Diseases pathology, Cell- and Tissue-Based Therapy methods, Cell- and Tissue-Based Therapy trends, Central Nervous System pathology, Drug Delivery Systems methods, Exosomes physiology, Humans, Treatment Outcome, Brain Diseases drug therapy, Brain Diseases surgery, Central Nervous System surgery, Drug Delivery Systems trends, Exosomes transplantation

Abstract

The potential of exosomes to treat central nervous system (CNS) pathologies has been recently demonstrated. These studies make way for a complete new field that aims to exploit the natural characteristics of these vesicles, considered for a long time as side products of physiological cellular pathways. Recently, however, the biological significance of exosomes has been evaluated and exosomes can now be viewed upon as new relevant functional entities for development of novel therapeutic strategies. In this review, we aim to summarize the state-of-the-art role of exosomes in the CNS and to speculate about possible future therapeutic applications of exosomes. In particular, we will speculate about the use of these vesicles as a substitute of cell-based therapies for the treatment of brain damage and review the potential of exosomes as drug delivery vehicles for the CNS.

Published

2014

136. The rodent endovascular puncture model of subarachnoid hemorrhage: mechanisms of brain damage and therapeutic strategies.

Author

Kooijman E, Nijboer CH, van Velthoven CT, Kavelaars A, Kesecioglu J, and Heijnen CJ

Subjects

Animals, Apoptosis, Brain Injuries therapy, Cytokines metabolism, Disease Models, Animal, Humans, Signal Transduction, Subarachnoid Hemorrhage complications, Subarachnoid Hemorrhage therapy, Brain Injuries etiology, Punctures adverse effects, Subarachnoid Hemorrhage etiology

Abstract

Subarachnoid hemorrhage (SAH) represents a considerable health problem. To date, limited therapeutic options are available. In order to develop effective therapeutic strategies for SAH, the mechanisms involved in SAH brain damage should be fully explored. Here we review the mechanisms of SAH brain damage induced by the experimental endovascular puncture model. We have included a description of similarities and distinctions between experimental SAH in animals and human SAH pathology. Moreover, several novel treatment options to diminish SAH brain damage are discussed.SAH is accompanied by cerebral inflammation as demonstrated by an influx of inflammatory cells into the cerebral parenchyma, upregulation of inflammatory transcriptional pathways and increased expression of cytokines and chemokines. Additionally, various cell death pathways including cerebral apoptosis, necrosis, necroptosis and autophagy are involved in neuronal damage caused by SAH.Treatment strategies aiming at inhibition of inflammatory or cell death pathways demonstrate the importance of these mechanisms for survival after experimental SAH. Moreover, neuroregenerative therapies using stem cells are discussed as a possible strategy to repair the brain after SAH since this therapy may extend the window of treatment considerably. We propose the endovascular puncture model as a suitable animal model which resembles the human pathology of SAH and which could be applied to investigate novel therapeutic therapies to combat this debilitating insult.

Published

2014

137. The neuroimmune basis of fatigue.

Author

Dantzer R, Heijnen CJ, Kavelaars A, Laye S, and Capuron L

Subjects

Animals, Humans, Fatigue etiology, Fatigue immunology, Fatigue physiopathology, Neuroimmunomodulation physiology

Abstract

The exact nature and pathophysiology of fatigue remain largely elusive despite its high prevalence in physically ill patients. Studies on the relationship between the immune system and the central nervous system provide a new perspective on the mechanisms of fatigue. Inflammatory mediators that are released by activated innate immune cells at the periphery and in the central nervous system alter the metabolism and activity of neurotransmitters, generate neurotoxic compounds, decrease neurotrophic factors, and profoundly disturb the neuronal environment. The resulting alterations in fronto-striatal networks together with the activation of insula by inflammatory interoceptive stimuli underlie the many dimensions of fatigue including reduced incentive motivation, decreased behavioral flexibility, uncertainty about usefulness of actions, and awareness of fatigue., (Published by Elsevier Ltd.)

Published

2014

138. Neuroinflammation and comorbidity of pain and depression.

Author

Walker AK, Kavelaars A, Heijnen CJ, and Dantzer R

Subjects

Animals, Brain, Comorbidity, Depression immunology, Humans, Inflammation epidemiology, Inflammation immunology, Pain immunology, Depression epidemiology, Pain epidemiology

Abstract

Comorbid depression and chronic pain are highly prevalent in individuals suffering from physical illness. Here, we critically examine the possibility that inflammation is the common mediator of this comorbidity, and we explore the implications of this hypothesis. Inflammation signals the brain to induce sickness responses that include increased pain and negative affect. This is a typical and adaptive response to acute inflammation. However, chronic inflammation induces a transition from these typical sickness behaviors into depression and chronic pain. Several mechanisms can account for the high comorbidity of pain and depression that stem from the precipitating inflammation in physically ill patients. These mechanisms include direct effects of cytokines on the neuronal environment or indirect effects via downregulation of G protein-coupled receptor kinase 2, activation of the tryptophan-degrading enzyme indoleamine 2,3-dioxygenase that generates neurotropic kynurenine metabolites, increased brain extracellular glutamate, and the switch of GABAergic neurotransmission from inhibition to excitation. Despite the existence of many neuroimmune candidate mechanisms for the co-occurrence of depression and chronic pain, little work has been devoted so far to critically assess their mediating role in these comorbid symptoms. Understanding neuroimmune mechanisms that underlie depression and pain comorbidity may yield effective pharmaceutical targets that can treat both conditions simultaneously beyond traditional antidepressants and analgesics.

Published

2013

139. Adequate endocrine and cardiovascular response to social stress in survivors of childhood acute lymphoblastic leukemia.

Author

Gordijn MS, Gemke RJ, Bierings MB, Hoogerbrugge PM, Tersteeg-Kamperman MD, Heijnen CJ, Rotteveel J, and Kaspers GJ

Subjects

Adolescent, Analysis of Variance, Child, Female, Follow-Up Studies, Hemodynamics physiology, Humans, Hydrocortisone metabolism, Male, Saliva chemistry, Cardiovascular Physiological Phenomena, Endocrine System physiology, Precursor Cell Lymphoblastic Leukemia-Lymphoma physiopathology, Precursor Cell Lymphoblastic Leukemia-Lymphoma psychology, Social Environment, Stress, Psychological physiopathology, Survivors psychology

Abstract

Survivors of childhood ALL have been demonstrated to have increased morning cortisol levels compared to healthy controls. Information regarding the response of the HPA axis and the sympathetic nervous system to stress in childhood ALL survivors is not available. The present study aimed at assessing the endocrine and cardiovascular stress response in childhood ALL survivors and healthy controls by evaluating perceived stress on visual analog scales, by determining saliva cortisol, blood pressure and heart rate in response to the Trier Social Stress Test for Children (TSST-C). Fifty survivors who had completed their treatment for childhood ALL 57 (IQR 47.0-72.3) months before and 50 healthy age and sex matched controls were included. Exposure to the TSST-C induced a significant response of perceived stress, saliva cortisol and cardiovascular outcome variables in the total study group. These responses did not significantly differ between survivors of childhood ALL and healthy controls. We conclude that the endocrine and cardiovascular response to social stress are intact in survivors of childhood ALL., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

140. Reprint of: In-vitro model systems for the study of human embryo-endometrium interactions.

Author

Weimar CH, Post Uiterweer ED, Teklenburg G, Heijnen CJ, and Macklon NS

Abstract

Implantation requires highly orchestrated interactions between the developing embryo and maternal endometrium. The association between abnormal implantation and reproductive failure is evident, both in normal pregnancy and in assisted reproduction patients. Failure of implantation is the pregnancy rate-limiting step in assisted reproduction, but, as yet, empirical interventions have largely failed to address this problem. Better understanding of the mechanisms underlying human embryo-endometrium signalling is a prerequisite for the further improvement of assisted reproduction outcomes and the development of effective interventions to prevent early pregnancy loss. Studying human embryo implantation is challenging since in-vivo experiments are impractical and unethical, and studies in animal models do not always translate well to humans. However, in recent years in-vitro models have been shown to provide a promising way forward. This review discusses the principal models used to study early human embryo development and initial stages of implantation in vitro. While each model has limitations, exploiting these models will improve understanding of the molecular mechanisms and embryo-endometrium cross-talk at the early implantation site. They provide valuable tools to study early embryo development and pathophysiology of reproductive disorders and have revealed novel disease mechanisms such as the role of epigenetic modifications in recurrent miscarriage., (Copyright © 2013. Published by Elsevier Ltd.)

Published

2013

141. Detection of cervical cancer recurrence during follow-up: a multivariable comparison of 9 frequently investigated serum biomarkers.

Author

Hoogendam JP, Zaal A, Rutten EG, Heijnen CJ, Kenter GG, Veldhuis WB, Verheijen RH, and Zweemer RP

Subjects

Adult, Aged, Aged, 80 and over, Cohort Studies, Female, Follow-Up Studies, Humans, Longitudinal Studies, Middle Aged, Neoplasm Recurrence, Local pathology, Neoplasm Staging, Retrospective Studies, Uterine Cervical Neoplasms pathology, Biomarkers, Tumor blood, Neoplasm Recurrence, Local blood, Uterine Cervical Neoplasms blood

Abstract

Objective: To assess the diagnostic accuracy and model the optimal combination of commonly studied serum biomarkers aimed at identifying recurrence in cervical cancer patients., Methods: From a systematic literature search, nine biomarkers (CA-15.3, CA-125, CEA, CYFRA 21-1, hsCRP, IL-6, SCC-Ag, TNF-α and VEGF) were selected for a serum analysis. Samples were derived from a historical cervical cancer cohort. Subjects with serum samples stored in a biobank were included when quality criteria were met, and one sample preceding and at least one following primary treatment were available. In case of recurrence, two additional post-recurrence samples were analyzed. Biomarker serum levels were quantified by enzyme linked or chemiluminescence microparticle immunoassays. Logistic regression and receiver operating curve analysis were employed for selection, modeling and comparison on the diagnostic accuracy of the tested biomarkers., Results: 205 samples were analyzed from 75 subjects, of whom 19 (25.3%) had a recurrence. The area under the curve (AUC) of CA-15.3, CA-125, CEA, CYFRA 21-1, IL-6, TNF-α and VEGF were all <0.750. Only SCC-Ag and hsCRP were included in the final model with an AUC of 0.822 (95% CI: 0.744-0.900) and 0.831 (95% CI: 0.758-0.905) respectively. Combined AUC was 0.870 (95% CI: 0.805-0.935). Rises in SCC-Ag and hsCRP significantly increased the odds for recurrence. Each ng/ml of SCC-Ag increase, related to an odds ratio (OR) of 1.117 (95% CI: 1.039-1.200). Comparably, the OR for hsCRP (in mg/ml) was 1.025 (95% CI: 1.012-1.038)., Conclusion: Combined testing of SCC-Ag and hsCRP yields the highest detection rate of disease recurrence during cervical cancer follow-up., (© 2013.)

Published

2013

142. Balancing GRK2 and EPAC1 levels prevents and relieves chronic pain.

Author

Wang H, Heijnen CJ, van Velthoven CT, Willemen HL, Ishikawa Y, Zhang X, Sood AK, Vroon A, Eijkelkamp N, and Kavelaars A

Subjects

Animals, Carrageenan toxicity, Cattle, Chronic Pain etiology, Chronic Pain genetics, Chronic Pain physiopathology, Cyclic AMP physiology, Dinoprostone physiology, Female, G-Protein-Coupled Receptor Kinase 2 biosynthesis, G-Protein-Coupled Receptor Kinase 2 genetics, Ganglia, Spinal pathology, Gene Expression Regulation, Gene Silencing, Genetic Therapy, Guanine Nucleotide Exchange Factors biosynthesis, Guanine Nucleotide Exchange Factors genetics, Hindlimb innervation, Hyperalgesia chemically induced, Hyperalgesia genetics, Hyperalgesia therapy, Injections, Spinal, Mice, Mice, Inbred C57BL, Models, Animal, Nociceptors enzymology, Nociceptors physiology, Oligonucleotides, Antisense administration & dosage, Oligonucleotides, Antisense pharmacology, Oligopeptides toxicity, Recombinant Fusion Proteins genetics, Sciatic Nerve pathology, Second Messenger Systems, Sensory Receptor Cells enzymology, Sensory Receptor Cells physiology, Chronic Pain prevention & control, G-Protein-Coupled Receptor Kinase 2 physiology, Guanine Nucleotide Exchange Factors physiology, Hyperalgesia physiopathology

Abstract

Chronic pain is a major clinical problem, yet the mechanisms underlying the transition from acute to chronic pain remain poorly understood. In mice, reduced expression of GPCR kinase 2 (GRK2) in nociceptors promotes cAMP signaling to the guanine nucleotide exchange factor EPAC1 and prolongs the PGE2-induced increase in pain sensitivity (hyperalgesia). Here we hypothesized that reduction of GRK2 or increased EPAC1 in dorsal root ganglion (DRG) neurons would promote the transition to chronic pain. We used 2 mouse models of hyperalgesic priming in which the transition from acute to chronic PGE2-induced hyperalgesia occurs. Hyperalgesic priming with carrageenan induced a sustained decrease in nociceptor GRK2, whereas priming with the PKCε agonist ΨεRACK increased DRG EPAC1. When either GRK2 was increased in vivo by viral-based gene transfer or EPAC1 was decreased in vivo, as was the case for mice heterozygous for Epac1 or mice treated with Epac1 antisense oligodeoxynucleotides, chronic PGE2-induced hyperalgesia development was prevented in the 2 priming models. Using the CFA model of chronic inflammatory pain, we found that increasing GRK2 or decreasing EPAC1 inhibited chronic hyperalgesia. Our data suggest that therapies targeted at balancing nociceptor GRK2 and EPAC1 levels have promise for the prevention and treatment of chronic pain.

Published

2013

143. In-vitro model systems for the study of human embryo-endometrium interactions.

Author

Weimar CH, Post Uiterweer ED, Teklenburg G, Heijnen CJ, and Macklon NS

Subjects

Cell Culture Techniques, Embryonic Development, Female, Humans, Infertility, Female, Spheroids, Cellular, Trophoblasts, Cell Communication, Embryo Implantation physiology, Endometrium physiology, Models, Biological

Abstract

Implantation requires highly orchestrated interactions between the developing embryo and maternal endometrium. The association between abnormal implantation and reproductive failure is evident, both in normal pregnancy and in assisted reproduction patients. Failure of implantation is the pregnancy rate-limiting step in assisted reproduction, but, as yet, empirical interventions have largely failed to address this problem. Better understanding of the mechanisms underlying human embryo-endometrium signalling is a prerequisite for the further improvement of assisted reproduction outcomes and the development of effective interventions to prevent early pregnancy loss. Studying human embryo implantation is challenging since in-vivo experiments are impractical and unethical, and studies in animal models do not always translate well to humans. However, in recent years in-vitro models have been shown to provide a promising way forward. This review discusses the principal models used to study early human embryo development and initial stages of implantation in vitro. While each model has limitations, exploiting these models will improve understanding of the molecular mechanisms and embryo-endometrium cross-talk at the early implantation site. They provide valuable tools to study early embryo development and pathophysiology of reproductive disorders and have revealed novel disease mechanisms such as the role of epigenetic modifications in recurrent miscarriage., (Copyright © 2013. Published by Elsevier Ltd.)

Published

2013

144. Effects of murine and human bone marrow-derived mesenchymal stem cells on cuprizone induced demyelination.

Author

Nessler J, Bénardais K, Gudi V, Hoffmann A, Salinas Tejedor L, Janßen S, Prajeeth CK, Baumgärtner W, Kavelaars A, Heijnen CJ, van Velthoven C, Hansmann F, Skripuletz T, and Stangel M

Subjects

Animals, Cell Count, Cell Tracking, Chemokines genetics, Chemokines metabolism, Corpus Callosum metabolism, Corpus Callosum pathology, Cuprizone, Cytoprotection, Demyelinating Diseases chemically induced, Demyelinating Diseases pathology, Feeding Behavior, Hepatocyte Growth Factor genetics, Hepatocyte Growth Factor metabolism, Humans, Immunohistochemistry, Integrin alpha4 metabolism, Male, Mice, Mice, Inbred C57BL, Oligodendroglia metabolism, Oligodendroglia pathology, Organic Chemicals metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Bone Marrow Cells cytology, Demyelinating Diseases therapy, Mesenchymal Stem Cell Transplantation, Mesenchymal Stem Cells cytology

Abstract

For the treatment of patients with multiple sclerosis there are no regenerative approaches to enhance remyelination. Mesenchymal stem cells (MSC) have been proposed to exert such regenerative functions. Intravenous administration of human MSC reduced the clinical severity of experimental autoimmune encephalomyelitis (EAE), an animal model mimicking some aspects of multiple sclerosis. However, it is not clear if this effect was achieved by systemic immunomodulation or if there is an active neuroregeneration in the central nervous system (CNS). In order to investigate remyelination and regeneration in the CNS we analysed the effects of intravenously and intranasally applied murine and human bone marrow-derived MSC on cuprizone induced demyelination, a toxic animal model which allows analysis of remyelination without the influence of the peripheral immune system. In contrast to EAE no effects of MSC on de- and remyelination and glial cell reactions were found. In addition, neither murine nor human MSC entered the lesions in the CNS in this toxic model. In conclusion, MSC are not directed into CNS lesions in the cuprizone model where the blood-brain-barrier is intact and thus cannot provide support for regenerative processes.

Published

2013

145. Early life intervention with glucocorticoids has negative effects on motor development and neuropsychological function in 14-17 year-old adolescents.

Author

ter Wolbeek M, de Sonneville LM, de Vries WB, Kavelaars A, Veen S, Kornelisse RF, van Weissenbruch M, Baerts W, Liem KD, van Bel F, and Heijnen CJ

Subjects

Adolescent, Attention drug effects, Dexamethasone therapeutic use, Educational Status, Executive Function drug effects, Female, Glucocorticoids therapeutic use, Humans, Infant, Newborn, Infant, Premature, Male, Neuropsychological Tests, Bronchopulmonary Dysplasia drug therapy, Dexamethasone pharmacology, Glucocorticoids pharmacology, Motor Skills drug effects

Abstract

Objective: To reduce the risk of bronchopulmonary dysplasia, preterm infants receive neonatal treatment with glucocorticoids, mostly dexamethasone (DEX). Compared to current protocols, treatment regimens of the late 1980s - early 1990s prescribed high doses of DEX for an extensive period up to 6 weeks. Worldwide at least one million children have been treated with this dose regimen. Previous studies have shown adverse effects of neonatal treatment with the glucocorticoid dexamethasone (DEX) on outcome in children aged 7-10 years. On the other hand, treatment with another glucocorticoid, hydrocortisone (HC), was not related to adverse effects in childhood. In the current study we determined the consequences of early life intervention with DEX or HC in adolescents (age 14-17 years). Besides motor function and intellectual capacities, we also examined fundamental neuropsychological functions which have so far received little attention., Methods: In an observational cohort study we compared 14-17 year-old adolescents who received DEX (.5 mg/kg/day tapering off to .1 mg/kg/day over 21 days, n=63), or HC (5 mg/kg/day tapering off to 1 mg/kg/day over 22 days, n=67), or did not receive neonatal glucocorticoids (untreated, n=71) after premature birth (gestational age<32 weeks). Because gestational age was shorter and duration of ventilation was longer in the DEX-treated group, all analyses were corrected for these potential confounders. Motor function, IQ, and neuropsychological functions were assessed., Results: DEX-treated group participants scored lower on gross motor skill tasks than their HC-treated and untreated counterparts. A higher proportion of DEX-treated girls needed special education compared to the other groups. DEX-treated adolescents performed poorer on neuropsychological tasks measuring alertness, visuomotor coordination, and emotion recognition. The HC-treated group did not differ from the untreated group., Conclusions: Even after 14-17 years, neonatal treatment with .5 mg/kg/day DEX was associated with adverse effects on motor function, school level, and neuropsychological functions, whereas treatment with the clinically equally effective dose of 5 mg/kg/day HC was not. Potential physiological mechanisms underlying the differences in dexamethasone and hydrocortisone effects are discussed. Based on the current findings, we recommend early identification of neuropsychological deficits after DEX treatment in order to specify extra educational needs., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2013

146. Mitochondrial JNK phosphorylation as a novel therapeutic target to inhibit neuroinflammation and apoptosis after neonatal ischemic brain damage.

Author

Nijboer CH, Bonestroo HJ, Zijlstra J, Kavelaars A, and Heijnen CJ

Subjects

Animals, Animals, Newborn, Apoptosis drug effects, Blotting, Western, Brain Ischemia complications, Disease Models, Animal, Electrophoretic Mobility Shift Assay, Enzyme Inhibitors pharmacology, Inflammation etiology, Inflammation metabolism, Mitochondria drug effects, Oxidative Stress drug effects, Phosphorylation, Rats, Rats, Wistar, Real-Time Polymerase Chain Reaction, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction drug effects, Brain Ischemia metabolism, Brain Ischemia physiopathology, MAP Kinase Kinase 4 antagonists & inhibitors, Mitochondria metabolism, Neuroprotective Agents pharmacology, Peptides pharmacology

Abstract

Neonatal encephalopathy is associated with high mortality and life-long developmental consequences. Therapeutic options are very limited. We assessed the effects of D-JNKi, a small peptide c-Jun N-terminal kinase (JNK) MAP kinase inhibitor, on neuroinflammation, mitochondrial integrity and neuronal damage in a neonatal rat model of ischemic brain damage. Hypoxic-ischemic (HI) brain injury was induced in postnatal-day 7 rats by unilateral carotid artery occlusion and hypoxia, and was followed by intraperitoneal D-JNKi treatment. We demonstrate here for the first time that a single intraperitoneal injection with D-JNKi directly after HI strongly reduces neonatal brain damage by >85% with a therapeutic window of at least 6h. D-JNKi treatment also restored cognitive and motor function as analyzed at 9weeks post-insult. Neuroprotective D-JNKi treatment inhibited phosphorylation of nuclear c-Jun (P-c-Jun), and consequently reduced activity of the AP-1 transcription factor and production of cerebral cytokines/chemokines as determined at 3 and 24h post-HI. Inhibition of P-c-Jun by D-JNKi is thought to be mediated via inhibition of the upstream phosphorylation of cytosolic and nuclear JNK and/or by preventing the direct interaction of phosphorylated (P-)JNK with c-Jun. Surprisingly, however, HI did not induce a detectable increase in P-JNK in cytosol or nucleus. Notably, we show here for the first time that HI induces P-JNK only in the mitochondrial fraction, which was completely prevented by D-JNKi treatment. The hypothesis that mitochondrial JNK activation is key to HI brain injury was supported by data showing that treatment of rat pups with SabKIM1 peptide, a specific mitochondrial JNK inhibitor, is also neuroprotective. Inhibition of HI-induced mitochondrial JNK activation was associated with preservation of mitochondrial integrity as evidenced by prevention of ATP loss and inhibition of lipid peroxidation. The HI-induced increase in apoptotic markers (cytochrome c release and caspase 3 activation) as analyzed at 24h post-HI were also strongly reduced by D-JNKi and the mitochondrial anti-apoptotic proteins Bcl-2 and Bcl-xL were upregulated. Neuroprotection was lost after repeated 0+3h D-JNKi treatment which was associated with complete inhibition of the second peak of AP-1 activity and disability to upregulate mitochondrial Bcl-2 and Bcl-xL. We show here for the first time that D-JNKi treatment efficiently protects the neonatal brain against ischemic brain damage and subsequent cognitive and motor impairment. We propose that inhibition of phosphorylation of mitochondrial JNK is a pivotal step in preventing early loss of mitochondrial integrity leading to reduced neuroinflammation and inhibition of apoptotic neuronal loss. Moreover we show the crucial role of upregulation of mitochondrial anti-apoptotic proteins to maintain neuroprotection., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

147. Astrocyte GRK2 as a novel regulator of glutamate transport and brain damage.

Author

Nijboer CH, Heijnen CJ, Degos V, Willemen HL, Gressens P, and Kavelaars A

Subjects

Animals, Animals, Newborn, Blotting, Western, Cytoskeletal Proteins metabolism, Disease Models, Animal, Female, Fluorescent Antibody Technique, Immunoprecipitation, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, RNA, Small Interfering, Amino Acid Transport System X-AG metabolism, Astrocytes metabolism, G-Protein-Coupled Receptor Kinase 2 metabolism, Glutamic Acid metabolism, Hypoxia-Ischemia, Brain metabolism

Abstract

G protein-coupled receptor (GPCR) kinase 2 (GRK2) regulates cellular signaling via desensitization of GPCRs and by direct interaction with intracellular signaling molecules. We recently described that ischemic brain injury decreases cerebral GRK2 levels. Here we studied the effect of astrocyte GRK2-deficiency on neonatal brain damage in vivo. As astrocytes protect neurons by taking up glutamate via plasma-membrane transporters, we also studied the effect of GRK2 on the localization of the GLutamate ASpartate Transporter (GLAST). Brain damage induced by hypoxia-ischemia was significantly reduced in GFAP-GRK2(+/-) mice, which have a 60% reduction in astrocyte GRK2 compared to GFAP-WT littermates. In addition, GRK2-deficient astrocytes have higher plasma-membrane levels of GLAST and an increased capacity to take up glutamate in vitro. In search for the mechanism by which GRK2 regulates GLAST expression, we observed increased GFAP levels in GRK2-deficient astrocytes. GFAP and the cytoskeletal protein ezrin are known regulators of GLAST localization. In line with this evidence, GRK2-deficiency reduced phosphorylation of the GRK2 substrate ezrin and enforced plasma-membrane GLAST association after stimulation with the group I mGluR-agonist DHPG. When ezrin was silenced, the enhanced plasma-membrane GLAST association in DHPG-exposed GRK2-deficient astrocytes was prevented. In conclusion, we identified a novel role of astrocyte GRK2 in regulating plasma-membrane GLAST localization via an ezrin-dependent route. We demonstrate that the 60% reduction in astrocyte GRK2 protein level that is observed in GFAP-GRK2(+/-) mice is sufficient to significantly reduce neonatal ischemic brain damage. These findings underline the critical role of GRK2 regulation in astrocytes for dampening the extent of brain damage after ischemia., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

148. Mesenchymal stem cell transplantation attenuates brain injury after neonatal stroke.

Author

van Velthoven CT, Sheldon RA, Kavelaars A, Derugin N, Vexler ZS, Willemen HL, Maas M, Heijnen CJ, and Ferriero DM

Subjects

Animals, Cell Proliferation, Disease Models, Animal, Infarction, Middle Cerebral Artery drug therapy, Infarction, Middle Cerebral Artery pathology, Nerve Fibers, Myelinated pathology, Neurons metabolism, Rats, Rats, Sprague-Dawley, Stroke pathology, Brain pathology, Brain-Derived Neurotrophic Factor therapeutic use, Infarction, Middle Cerebral Artery therapy, Mesenchymal Stem Cell Transplantation methods, Stroke therapy

Abstract

Background and Purpose: Brain injury caused by stroke is a frequent cause of perinatal morbidity and mortality with limited therapeutic options. Mesenchymal stem cells (MSC) have been shown to improve outcome after neonatal hypoxic-ischemic brain injury mainly by secretion of growth factors stimulating repair processes. We investigated whether MSC treatment improves recovery after neonatal stroke and whether MSC overexpressing brain-derived neurotrophic factor (MSC-BDNF) further enhances recovery., Methods: We performed 1.5-hour transient middle cerebral artery occlusion in 10-day-old rats. Three days after reperfusion, pups with evidence of injury by diffusion-weighted MRI were treated intranasally with MSC, MSC-BDNF, or vehicle. To determine the effect of MSC treatment, brain damage, sensorimotor function, and cerebral cell proliferation were analyzed., Results: Intranasal delivery of MSC- and MSC-BDNF significantly reduced infarct size and gray matter loss in comparison with vehicle-treated rats without any significant difference between MSC- and MSC-BDNF-treatment. Treatment with MSC-BDNF significantly reduced white matter loss with no significant difference between MSC- and MSC-BDNF-treatment. Motor deficits were also improved by MSC treatment when compared with vehicle-treated rats. MSC-BDNF-treatment resulted in an additional significant improvement of motor deficits 14 days after middle cerebral artery occlusion, but there was no significant difference between MSC or MSC-BDNF 28 days after middle cerebral artery occlusion. Furthermore, treatment with either MSC or MSC-BDNF induced long-lasting cell proliferation in the ischemic hemisphere., Conclusions: Intranasal administration of MSC after neonatal stroke is a promising therapy for treatment of neonatal stroke. In this experimental paradigm, MSC- and BNDF-hypersecreting MSC are equally effective in reducing ischemic brain damage.

Published

2013

149. Predicting PTSD: pre-existing vulnerabilities in glucocorticoid-signaling and implications for preventive interventions.

Author

van Zuiden M, Kavelaars A, Geuze E, Olff M, and Heijnen CJ

Subjects

Humans, Polymorphism, Single Nucleotide, Receptors, Glucocorticoid genetics, Risk Factors, Stress Disorders, Post-Traumatic metabolism, Stress Disorders, Post-Traumatic physiopathology, Tacrolimus Binding Proteins genetics, Tacrolimus Binding Proteins metabolism, Glucocorticoids metabolism, Receptors, Glucocorticoid metabolism, Signal Transduction physiology, Stress Disorders, Post-Traumatic diagnosis

Abstract

Posttraumatic stress disorder (PTSD) is an anxiety disorder that may develop in response to a traumatic event. Approximately 10% of trauma-exposed individuals subsequently develop PTSD. It is hypothesized that the development of PTSD is associated with biological vulnerability factors, which are already present prior to the onset of symptoms. In this review we present an overview of currently identified vulnerability factors in the glucocorticoid (GC) signaling pathway for the development of PTSD. In addition, the implications of the identified vulnerability factors for potential preventive intervention strategies, including glucocorticoid receptor (GR) agonists and oxytocin, are discussed. Summarized, the findings of these studies indicate that individuals vulnerable for development of PTSD have dysregulations on various levels of the GC-signaling cascade: i.e. low levels of circulating levels of cortisol shortly after trauma, high GR number in peripheral blood mononuclear cells (PBMCs), high GILZ mRNA expression and low FKBP5 expression in PBMCs prior to trauma, and high sensitivity of T-cells for regulation by GCs prior to trauma. Furthermore, single nucleotide polymorphisms in the GR and FKBP5 genes have been found to be associated with increased risk for PTSD. Collectively, the identified vulnerability factors tentatively suggest that the development of PTSD may be preceded by a high sensitivity of various cells for regulation by GCs. The identification of these vulnerability factors may ultimately aid selective targeting of preventive interventions towards individuals at risk for PTSD. In addition, the identification of these vulnerability factors may eventually result in new preventive pharmacological strategies for PTSD., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2013

150. The endogenous regenerative capacity of the damaged newborn brain: boosting neurogenesis with mesenchymal stem cell treatment.

Author

Donega V, van Velthoven CT, Nijboer CH, Kavelaars A, and Heijnen CJ

Subjects

Animals, Brain growth & development, Brain physiopathology, Brain Ischemia physiopathology, Humans, Infant, Newborn, Brain physiology, Brain surgery, Brain Ischemia surgery, Mesenchymal Stem Cell Transplantation methods, Neurogenesis, Regeneration

Abstract

Neurogenesis continues throughout adulthood. The neurogenic capacity of the brain increases after injury by, e.g., hypoxia-ischemia. However, it is well known that in many cases brain damage does not resolve spontaneously, indicating that the endogenous regenerative capacity of the brain is insufficient. Neonatal encephalopathy leads to high mortality rates and long-term neurologic deficits in babies worldwide. Therefore, there is an urgent need to develop more efficient therapeutic strategies. The latest findings indicate that stem cells represent a novel therapeutic possibility to improve outcome in models of neonatal encephalopathy. Transplanted stem cells secrete factors that stimulate and maintain neurogenesis, thereby increasing cell proliferation, neuronal differentiation, and functional integration. Understanding the molecular and cellular mechanisms underlying neurogenesis after an insult is crucial for developing tools to enhance the neurogenic capacity of the brain. The aim of this review is to discuss the endogenous capacity of the neonatal brain to regenerate after a cerebral ischemic insult. We present an overview of the molecular and cellular mechanisms underlying endogenous regenerative processes during development as well as after a cerebral ischemic insult. Furthermore, we will consider the potential to use stem cell transplantation as a means to boost endogenous neurogenesis and restore brain function.

Published

2013