Your search keyword '"Robert H. Garman"' showing total 104 results

1. Nervous System Sampling for General Toxicity and Neurotoxicity Studies in the Laboratory Minipig With Emphasis on the Göttingen Minipig

Author

Rosa Anna Manno, James P. Morrison, Aaron M. Sargeant, Ingrid D. Pardo, Brad Bolon, Robert H. Garman, and Raffaella Capobianco

Subjects

Nervous system, Swine, business.industry, Histological Techniques, Neurotoxicity, Cell Biology, Göttingen minipig, Toxicology, Bioinformatics, medicine.disease, Pathology and Forensic Medicine, medicine.anatomical_structure, Spinal Cord, Toxicity, medicine, Animals, Swine, Miniature, Neurotoxicity Syndromes, Sampling (medicine), Laboratories, business, Molecular Biology

Abstract

The use of minipigs as an alternative nonclinical species has increased in the last 20 years. The Society of Toxicologic Pathology (STP) has produced generic “best practice” recommendations for nervous system sampling in nonrodents during general toxicity studies ( Toxicol Pathol 41[7]: 1028–1048, 2013), but their adaptation to the minipig has not been attempted. Here, we describe 2 trimming schemes suitable for evaluating the unique neuroanatomic features of the minipig brain in nonclinical toxicity studies. The first scheme is intended for general toxicity studies (Tier 1) to screen agents with unknown or no anticipated neurotoxic potential; this approach using 7 coronal hemisections accords with the published STP “best practice” recommendations. The second trimming scheme for neurotoxicity studies (Tier 2) uses 14 coronal hemisections and 2 full coronal sections to investigate toxicants where the nervous system is a suspected or known target organ. Collection of spinal cord, ganglia (somatic and autonomic), and nerves from minipigs during nonclinical studies should follow published STP “best practice” recommendations for sampling the central (CNS, Toxicol Pathol 41[7]: 1028–1048, 2013) and peripheral (PNS, Toxicol Pathol 46[4]: 372–402, 2018) nervous systems.

Published

2021

2. A Technical Guide to Sampling the Beagle Dog Nervous System for General Toxicity and Neurotoxicity Studies

Author

Xavier Palazzi, Ingrid D. Pardo, Hayley Ritenour, Deepa B. Rao, Brad Bolon, and Robert H. Garman

Subjects

Dogs, Spinal Cord, Peripheral Nervous System, Toxicity Tests, Animals, Neurotoxicity Syndromes, Cell Biology, Toxicology, Molecular Biology, Pathology and Forensic Medicine, Specimen Handling

Abstract

Beagle dogs are a key nonrodent species in nonclinical safety evaluation of new biomedical products. The Society of Toxicologic Pathology (STP) has published “best practices” recommendations for nervous system sampling in nonrodents during general toxicity studies ( Toxicol Pathol 41[7]: 1028-1048, 2013), but their adaptation to the Beagle dog has not been defined specifically. Here we provide 2 trimming schemes suitable for evaluating the unique neuroanatomic features of the dog brain in nonclinical toxicity studies. The first scheme is intended for general toxicity studies (Tier 1) to screen test articles with unknown or no anticipated neurotoxic potential; this plan using at least 7 coronal hemisections matches the STP “best practices” recommendations. The second trimming scheme for neurotoxicity studies (Tier 2) uses up to 14 coronal levels to investigate test articles where the brain is a suspected or known target organ. Collection of spinal cord, ganglia (somatic and autonomic), and nerves for dogs during nonclinical studies should follow published STP “best practices” recommendations for sampling the central ( Toxicol Pathol 41[7]: 1028-1048, 2013) and peripheral ( Toxicol Pathol 46[4]: 372-402, 2018) nervous systems. This technical guide also demonstrates the locations and approaches to collecting uncommonly sampled peripheral nervous system sites.

Published

2022

3. Proliferative and Nonproliferative Lesions of the Rat and Mouse Central and Peripheral Nervous Systems: New and Revised INHAND Terms

Author

Alys Bradley, Ramesh C. Kovi, Wolfgang Kaufmann, Deepa B. Rao, Mark T. Butt, Alok K. Sharma, Sibylle Gröters, Robert C. Sills, Robert H. Garman, Brad Bolon, Peter B Little, Sarah D Cramer, Makoto Shibutani, Catherine George, Stephanie Czasch, Georg Krinke, and Isao Narama

Subjects

Pathology, medicine.medical_specialty, 040301 veterinary sciences, Central nervous system, Neural tissues, Toxicology, 030226 pharmacology & pharmacy, Pathology and Forensic Medicine, 0403 veterinary science, Mice, 03 medical and health sciences, 0302 clinical medicine, Peripheral Nervous System, Animals, Medicine, International harmonization, Molecular Biology, business.industry, 04 agricultural and veterinary sciences, Cell Biology, Rats, Peripheral, Tissue sections, medicine.anatomical_structure, Peripheral nervous system, business

Abstract

Harmonization of diagnostic terminology used during the histopathologic analysis of rodent tissue sections from nonclinical toxicity studies will improve the consistency of data sets produced by laboratories located around the world. The INHAND Project ( International Harmonization of Nomenclature and Diagnostic Criteria for Lesions in Rats and Mice) is a cooperative enterprise of 4 major societies of toxicologic pathology to develop a globally accepted standard vocabulary for proliferative and nonproliferative lesions in rodents. A prior manuscript ( Toxicol Pathol 2012;40[4 Suppl]:87S-157S) defined multiple diagnostic terms for toxicant-induced lesions, common spontaneous and age-related changes, and principal confounding artifacts in the rat and mouse central nervous system (CNS) and peripheral nervous system (PNS). The current article defines 9 new diagnostic terms and updates 2 previous terms for findings in the rodent CNS and PNS, the need for which has become evident in the years since the publication of the initial INHAND nomenclature for findings in rodent neural tissues. The nomenclature presented in this document is also available electronically on the Internet at the goRENI website ( http://www.goreni.org/ ).

Published

2020

4. Hypoxia–ischemia-mediated effects on neurodevelopmentally regulated cold-shock proteins in neonatal mice under strict temperature control

Author

Travis C. Jackson, Jeremy R. Herrmann, Robert H. Garman, Richard D. Kang, Vincent A. Vagni, Kiersten Gorse, Keri Janesko-Feldman, Jason Stezoski, and Patrick M. Kochanek

Subjects

Pediatrics, Perinatology and Child Health

Published

2022

5. Hypoxia-ischemia-mediated effects on neurodevelopmentally regulated cold-shock proteins in neonatal mice under strict temperature control

Author

Travis C, Jackson, Jeremy R, Herrmann, Robert H, Garman, Richard D, Kang, Vincent A, Vagni, Kiersten, Gorse, Keri, Janesko-Feldman, Jason, Stezoski, and Patrick M, Kochanek

Abstract

Neonates have high levels of cold-shock proteins (CSPs) in the normothermic brain for a limited period following birth. Hypoxic-ischemic (HI) insults in term infants produce neonatal encephalopathy (NE), and it remains unclear whether HI-induced pathology alters baseline CSP expression in the normothermic brain.Here we established a version of the Rice-Vannucci model in PND 10 mice that incorporates rigorous temperature control.Common carotid artery (CCA)-ligation plus 25 min hypoxia (8% OThe findings suggest the need to determine whether optimized therapeutic hypothermia (depth and duration) can prevent the age-related decline in neuroprotective CSPs like RBM3 in the brain, and improve outcomes during critical phases of secondary injury and recovery after NE.The rapid decrease in endogenous neuroprotective cold-shock proteins (CSPs) in the normothermic cortex, thalamus, and hippocampus from postnatal day (PND) 11-18, coincides with the timing of thermogenesis maturation in neonatal mice. Hypoxia-ischemia (HI) has a minor impact on the normal age-dependent decline in brain CSP levels in neonates maintained normothermic post-injury. HI robustly disrupts the expected correlation in RNA-binding motif 3 (RBM3) and reticulon-3 (RTN3). The potent neuroprotectant RBM3 is not increased 1-4 days after HI in a mouse model of neonatal encephalopathy (NE) in the term newborn and in which rigorous temperature control prevents the manifestation of endogenous post-insult hypothermia.

Published

2021

6. Neuropathology Evaluation in Juvenile Toxicity Studies in Rodents: Comparison of Developmental Neurotoxicity Studies for Chemicals With Juvenile Animal Studies for Pediatric Pharmaceuticals

Author

Brad Bolon, Lori A. Dostal, and Robert H. Garman

Subjects

Nervous system, Pathology, medicine.medical_specialty, Paraffin Embedding, business.industry, H&E stain, Rodentia, Cell Biology, Neuropathology, Toxicology, Spinal cord, Pathology and Forensic Medicine, medicine.anatomical_structure, Pharmaceutical Preparations, Spinal Cord, Animals, Laboratory, Toxicity, medicine, Juvenile, Animals, Humans, Juvenile animal, Sciatic nerve, business, Molecular Biology

Abstract

The developmental neuropathology examination in juvenile toxicity studies depends on the nature of the product candidate, its intended use, and the exposure scenario (eg, dose, duration, and route). Expectations for sampling, processing, and evaluating neural tissues differ for developmental neurotoxicity studies (DNTS) for chemicals and juvenile animal studies (JAS) for pediatric pharmaceuticals. Juvenile toxicity studies typically include macroscopic observations, brain weights, and light microscopic evaluation of routine hematoxylin and eosin (H&E)-stained sections from major neural tissues (brain, spinal cord, and sciatic nerve) as neuropathology endpoints. The DNTS is a focused evaluation of the nervous system, so the study design incorporates perfusion fixation, plastic embedding of at least one nerve, quantitative analysis of selected brain regions, and sometimes special neurohistological stains. In contrast, the JAS examines multiple systems, so neural tissues undergo conventional tissue processing (eg, immersion fixation, paraffin embedding, H&E staining only). An “expanded neurohistopathology” (or “expanded neuropathology”) approach may be performed for JAS if warranted, typically by light microscopic evaluation of more neural tissues (usually additional sections of brain, ganglia, and/or more nerves) or/and special neurohistological stains, to investigate specific questions (eg, a more detailed exploration of a potential neuroactive effect) or to fulfill regulatory requests.

Published

2021

7. Nervous System Sampling for General Toxicity and Neurotoxicity Studies in Rabbits

Author

Colleen Huddleston, Deepa B. Rao, Brad Bolon, Alys Bradley, Robert H. Garman, Ingrid D. Pardo, and James P. Morrison

Subjects

Nervous system, 040301 veterinary sciences, Intact brain, Toxicology, Bioinformatics, 030226 pharmacology & pharmacy, Nervous System, Pathology and Forensic Medicine, Specimen Handling, 0403 veterinary science, 03 medical and health sciences, 0302 clinical medicine, Peripheral Nervous System, medicine, Animals, Sampling (medicine), Molecular Biology, business.industry, Histological Techniques, Neurotoxicity, 04 agricultural and veterinary sciences, Cell Biology, Multiple species, medicine.disease, Spinal cord, medicine.anatomical_structure, Spinal Cord, Peripheral nervous system, Toxicity, Neurotoxicity Syndromes, Rabbits, business

Abstract

Although manuscripts for multiple species recommending nervous system sampling for histopathology evaluation in safety assessment have been published in the past 15 years, none have addressed the laboratory rabbit. Here, we describe 2 trimming schemes for evaluating the rabbit brain in nonclinical toxicity studies. In both schemes, the intact brain is cut in the coronal plane to permit bilateral assessment. The first scheme is recommended for general toxicity studies (tier 1) in screening agents where there is no anticipated neurotoxic potential; this 6-section approach is consistent with the Society of Toxicologic Pathology (STP) “best practice” recommendations for brain sampling in nonrodents ( Toxicol Pathol 41: 1028-1048, 20131). The second trimming scheme is intended for dedicated neurotoxicity studies (tier 2) to characterize known or suspected neurotoxicants where the nervous system is a key target organ. This tier 2 strategy relies on coronal trimming of the whole brain into 3-mm-thick slices and then evaluating 12 sections. Collection of spinal cord, ganglia, and nerve specimens for rabbits during nonclinical studies should follow published STP “best practice” recommendations for sampling the central nervous system1 and peripheral nervous system ( Toxicol Pathol 46: 372-402, 20182).

Published

2020

8. Scientific and Regulatory Policy Committee Points to Consider: Histopathologic Evaluation in Safety Assessment Studies for PEGylated Pharmaceutical Products

Author

Bevin Zimmerman, Brad Bolon, Robert H. Garman, Annamaria Braendli-Baiocco, David L. Hutto, Renaud Fleurance, Joan Lane, Sundeep Chandra, Annette Romeike, Aaron M. Sargeant, Bindu Bennet, and Armando R. Irizarry Rovira

Subjects

Drug-Related Side Effects and Adverse Reactions, 040301 veterinary sciences, Drug target, Drug Evaluation, Preclinical, Toxicology, Bioinformatics, 030226 pharmacology & pharmacy, Polyethylene Glycols, Pathology and Forensic Medicine, 0403 veterinary science, Toxicology studies, 03 medical and health sciences, 0302 clinical medicine, Tissue damage, Animals, Medicine, Tissue Distribution, Policy Making, Animal species, Molecular Biology, business.industry, 04 agricultural and veterinary sciences, Cell Biology, Regulatory policy, Pharmaceutical Preparations, Consumer Product Safety, Organ Specificity, Vacuoles, business, Cytoplasmic Vacuolation

Abstract

Colorless, intracytoplasmic vacuoles occur in multiple tissues in animals following repeated administration of polyethylene glycol (PEG)-conjugated molecules. The extent of vacuolation depends on physical characteristics and molecular backbone of the PEG and the dose, product, drug target/pharmacology, and duration of exposure. The collective experience gathered from multiple nonclinical toxicology studies of PEGylated biopharmaceuticals indicates that in general, PEG-related vacuolation is not associated with demonstrable cell and tissue damage or dysfunction and is reversible with sufficient duration of drug-free periods. Existing data are insufficient to predict whether nonclinical animal species differ in their sensitivity to develop PEG-associated vacuoles; however, recent data suggest that there may be species differences. Recent comprehensive reviews have addressed the basic challenges in developing PEGylated pharmaceutical products, including general reference to and description of PEG-associated tissue findings. These manuscripts have identified gaps in our current understanding of PEG-associated vacuolation, including the lack of a widely accepted standardized histological terminology and criteria to record and grade the severity of vacuolation as well as insufficient knowledge regarding the nature of the contents of these vacuoles. The goal of this article is to help address some of the gaps identified above by providing points to consider, including a pictorial review of PEG-associated microscopic findings, when evaluating and reporting the extent, severity, and significance (adversity or lack of adversity) of PEG-associated cytoplasmic vacuolation in safety assessment studies. [Box: see text]

Published

2018

9. STP Position Paper: Recommended Best Practices for Sampling, Processing, and Analysis of the Peripheral Nervous System (Nerves and Somatic and Autonomic Ganglia) during Nonclinical Toxicity Studies

Author

Georg Krinke, Brad Bolon, Bernard S Jortner, Deepa B. Rao, Karl F. Jensen, Robert H. Garman, Mark T. Butt, Lydia L. Andrews-Jones, Michael S. Thibodeau, Ingrid D. Pardo, James P. Morrison, and Alok K. Sharma

Subjects

040301 veterinary sciences, Autonomic ganglion, H&E stain, Neuropathology, Toxicology, Specimen Handling, Pathology and Forensic Medicine, 0403 veterinary science, 03 medical and health sciences, Trigeminal ganglion, 0302 clinical medicine, Peripheral Nervous System, medicine, Animals, Humans, Sampling (medicine), Molecular Biology, business.industry, Histological Techniques, Neurotoxicity, 04 agricultural and veterinary sciences, Cell Biology, medicine.disease, medicine.anatomical_structure, Peripheral nervous system, Spinal nerve, business, Neuroscience, 030217 neurology & neurosurgery

Abstract

Peripheral nervous system (PNS) toxicity is surveyed inconsistently in nonclinical general toxicity studies. These Society of Toxicologic Pathology “best practice” recommendations are designed to ensure consistent, efficient, and effective sampling, processing, and evaluation of PNS tissues for four different situations encountered during nonclinical general toxicity (screening) and dedicated neurotoxicity studies. For toxicity studies where neurotoxicity is unknown or not anticipated (situation 1), PNS evaluation may be limited to one sensorimotor spinal nerve. If somatic PNS neurotoxicity is suspected (situation 2), analysis minimally should include three spinal nerves, multiple dorsal root ganglia, and a trigeminal ganglion. If autonomic PNS neuropathy is suspected (situation 3), parasympathetic and sympathetic ganglia should be assessed. For dedicated neurotoxicity studies where a neurotoxic effect is expected (situation 4), PNS sampling follows the strategy for situations 2 and/or 3, as dictated by functional or other compound/target-specific data. For all situations, bilateral sampling with unilateral processing is acceptable. For situations 1–3, PNS is processed conventionally (immersion in buffered formalin, paraffin embedding, and hematoxylin and eosin staining). For situation 4 (and situations 2 and 3 if resources and timing permit), perfusion fixation with methanol-free fixative is recommended. Where PNS neurotoxicity is suspected or likely, at least one (situations 2 and 3) or two (situation 4) nerve cross sections should be postfixed with glutaraldehyde and osmium before hard plastic resin embedding; soft plastic embedding is not a suitable substitute for hard plastic. Special methods may be used if warranted to further characterize PNS findings. Initial PNS analysis should be informed, not masked (“blinded”). Institutions may adapt these recommendations to fit their specific programmatic requirements but may need to explain in project documentation the rationale for their chosen PNS sampling, processing, and evaluation strategy.

Published

2018

10. Recommendations for harmonization of data collection and analysis of developmental neurotoxicity endpoints in regulatory guideline studies: Proceedings of workshops presented at Society of Toxicology and joint Teratology Society and Neurobehavioral Teratology Society meetings

Author

Brad Bolon, Angela Hofstra, Virginia C. Moser, Abby A. Li, Wolfgang Kaufmann, Thomas J. Vidmar, Wayne J. Bowers, Kathleen Raffaele, Susan L. Makris, Edmund Lau, Alan M. Hoberman, Robert H. Garman, Larry Sheets, and Roland N. Auer

Subjects

Societies, Scientific, 0301 basic medicine, Guidelines as Topic, Harmonization, Context (language use), Toxicology, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Developmental Neuroscience, Toxicity Tests, Animals, Humans, Medicine, United States Environmental Protection Agency, Data reporting, Risk management, Teratology, Government, Health risk assessment, business.industry, Guideline, Congresses as Topic, United States, 030104 developmental biology, Research Design, Neurotoxicity Syndromes, Risk assessment, business, 030217 neurology & neurosurgery

Abstract

The potential for developmental neurotoxicity (DNT) of environmental chemicals may be evaluated using specific test guidelines from the US Environmental Protection Agency or the Organisation for Economic Cooperation and Development (OECD). These guidelines generate neurobehavioral, neuropathological, and morphometric data that are evaluated by regulatory agencies globally. Data from these DNT guideline studies, or the more recent OECD extended one-generation reproductive toxicity guideline, play a pivotal role in children's health risk assessment in different world areas. Data from the same study may be interpreted differently by regulatory authorities in different countries resulting in inconsistent evaluations that may lead to inconsistencies in risk assessment decisions internationally, resulting in regional differences in public health protection or in commercial trade barriers. These issues of data interpretation and reporting are also relevant to juvenile and pre-postnatal studies conducted more routinely for pharmaceuticals and veterinary medicines. There is a need for development of recommendations geared toward the operational needs of the regulatory scientific reviewers who apply these studies in risk assessments, as well as the scientists who generate DNT data sets. The workshops summarized here draw upon the experience of the authors representing government, industry, contract research organizations, and academia to discuss the scientific issues that have emerged from diverse regulatory evaluations. Although various regulatory bodies have different risk management decisions and labeling requirements that are difficult to harmonize, the workshops provided an opportunity to work toward more harmonized scientific approaches for evaluating DNT data within the context of different regulatory frameworks. Five speakers and their coauthors with neurotoxicology, neuropathology, and regulatory toxicology expertise discussed issues of variability, data reporting and analysis, and expectations in DNT data that are encountered by regulatory authorities. In addition, principles for harmonized evaluation of data were suggested using guideline DNT data as case studies.

Published

2017

11. Nitrite pharmacokinetics, safety and efficacy after experimental ventricular fibrillation cardiac arrest

Author

Jason Stezoski, Cameron Dezfulian, Philip E. Empey, Keri Janesko-Feldman, Francis Kim, Thomas Uray, Travis C. Jackson, Robert H. Garman, Patrick M. Kochanek, and Tomas Drabek

Subjects

0301 basic medicine, Male, Cancer Research, Resuscitation, Physiology, medicine.medical_treatment, Clinical Biochemistry, 030204 cardiovascular system & hematology, Return of spontaneous circulation, Targeted temperature management, Biochemistry, Article, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Pharmacokinetics, medicine, Animals, Humans, Tissue Distribution, Cardiopulmonary resuscitation, Nitrite, Nitrites, Brain Diseases, business.industry, Hypothermia, medicine.disease, Heart Arrest, 030104 developmental biology, chemistry, Blood-Brain Barrier, Anesthesia, Ventricular fibrillation, Ventricular Fibrillation, Administration, Intravenous, medicine.symptom, business

Abstract

INTRODUCTION: Besides therapeutic hypothermia or targeted temperature management no novel therapies have been developed to improve outcomes of patients after cardiac arrest (CA). Recent studies suggest that nitrite reduces neurological damage after asphyxial CA. Nitrite is also implicated as a new mediator of remote post conditioning produced by tourniquet inflation-deflation, which is under active investigation in CA. However, little is known about brain penetration or pharmacokinetics (PK). Therefore, to define the optimal use of this agent, studies on the PK of nitrite in experimental ventricular fibrillation (VF) are needed. We tested the hypothesis that nitrite administered after resuscitation from VF is detectable in cerebrospinal fluid (CSF), brain and other organ tissues, produces no adverse hemodynamic effects, and improves neurologic outcome in rats. METHODS: After return of spontaneous circulation (ROSC) of 5 min untreated VF, adult male Sprague-Dawley rats were given intravenous nitrite (8 μM, 0.13 mg/kg) or placebo as a 5 min infusion beginning at 5 min after CA. Additionally, sham groups with and without nitrite treatment were also studied. Whole blood nitrite levels were serially measured. After 15 minutes, CSF, brain, heart and liver tissue were collected. In a second series, using a randomized and blinded treatment protocol, rats were treated with nitrite or placebo after arrest. Neurological deficit scoring (NDS) was performed daily and eight days after resuscitation, fear conditioning testing (FCT) and brain histology were assessed. RESULTS: In an initial series of experiments, rats (n=21) were randomized to 4 groups: VF-CPR and nitrite therapy (n=6), VF-CPR and placebo therapy (n=5), sham (n=5), or sham plus nitrite therapy (n=5). Whole blood nitrite levels increased during drug infusion to 57.14 ± 10.82 μM at 11 min post-resuscitation time (1 min after dose completion) in the VF nitrite group vs. 0.94±0.58 μM in the VF placebo group (p

Published

2019

12. Phenotyping cardiac arrest: bench and bedside characterization of brain and heart injury based on etiology

Author

Ankur A. Doshi, Patrick M. Kochanek, Clifton W. Callaway, Andrew M. Lamade, Jonathan Elmer, Thomas Uray, Cameron Dezfulian, Keri Janesko-Feldman, Robert H. Garman, Jason Stezoski, Adam Frisch, Niel Chen, Francis X. Guyette, Tomas Drabek, Josh C Reynolds, Amalea Misse, and Jon C. Rittenberger

Subjects

Male, Cardiac output, medicine.medical_specialty, Heart Injury, Hemodynamics, 030204 cardiovascular system & hematology, Return of spontaneous circulation, Critical Care and Intensive Care Medicine, Article, Rats, Sprague-Dawley, 03 medical and health sciences, Asphyxia, 0302 clinical medicine, Internal medicine, medicine, Animals, Humans, Prospective Studies, Ejection fraction, biology, business.industry, Myocardium, Brain, 030208 emergency & critical care medicine, medicine.disease, Troponin, Heart Arrest, Rats, Disease Models, Animal, Phenotype, Ventricular fibrillation, Ventricular Fibrillation, cardiovascular system, Cardiology, biology.protein, Cardiovascular Injury, business

Abstract

OBJECTIVES Cardiac arrest etiology may be an important source of between-patient heterogeneity, but the impact of etiology on organ injury is unknown. We tested the hypothesis that asphyxial cardiac arrest results in greater neurologic injury than cardiac etiology cardiac arrest (ventricular fibrillation cardiac arrest), whereas ventricular fibrillation cardiac arrest results in greater cardiovascular dysfunction after return of spontaneous circulation. DESIGN Prospective observational human and randomized animal study. SETTING University laboratory and ICUs. PATIENTS Five-hundred forty-three cardiac arrest patients admitted to ICU. SUBJECTS Seventy-five male Sprague-Dawley rats. INTERVENTIONS We examined neurologic and cardiovascular injury in Isoflurane-anesthetized rat cardiac arrest models matched by ischemic time. Hemodynamic and neurologic outcomes were assessed after 5 minutes no flow asphyxial cardiac arrest or ventricular fibrillation cardiac arrest. Comparison was made to injury patterns observed after human asphyxial cardiac arrest or ventricular fibrillation cardiac arrest. MEASUREMENTS AND MAIN RESULTS In rats, cardiac output (20 ± 10 vs 45 ± 9 mL/min) and pH were lower and lactate higher (9.5 ± 1.0 vs 6.4 ± 1.3 mmol/L) after return of spontaneous circulation from ventricular fibrillation cardiac arrest versus asphyxial cardiac arrest (all p < 0.01). Asphyxial cardiac arrest resulted in greater early neurologic deficits, 7-day neuronal loss, and reduced freezing time (memory) after conditioned fear (all p < 0.05). Brain antioxidant reserves were more depleted following asphyxial cardiac arrest. In adjusted analyses, human ventricular fibrillation cardiac arrest was associated with greater cardiovascular injury based on peak troponin (7.8 ng/mL [0.8-57 ng/mL] vs 0.3 ng/mL [0.0-1.5 ng/mL]) and ejection fraction by echocardiography (20% vs 55%; all p < 0.0001), whereas asphyxial cardiac arrest was associated with worse early neurologic injury and poor functional outcome at hospital discharge (n = 46 [18%] vs 102 [44%]; p < 0.0001). Most ventricular fibrillation cardiac arrest deaths (54%) were the result of cardiovascular instability, whereas most asphyxial cardiac arrest deaths (75%) resulted from neurologic injury (p < 0.0001). CONCLUSIONS In transcending rat and human studies, we find a consistent phenotype of heart and brain injury after cardiac arrest based on etiology: ventricular fibrillation cardiac arrest produces worse cardiovascular dysfunction, whereas asphyxial cardiac arrest produces worsened neurologic injury associated with greater oxidative stress.

Published

2018

13. Spontaneous Ectopic Choroid Plexus with Sclerosis in Adult Beagle Dogs

Author

Michael Mirsky, Ingrid D. Pardo, Christopher Houle, Ahmed M. Shoieb, Rosemary Santos, and Robert H. Garman

Subjects

Male, Pathology, medicine.medical_specialty, Ependymal Cell, 040301 veterinary sciences, Connective tissue, Choristoma, Toxicology, Corpus callosum, Beagle, Pathology and Forensic Medicine, 0403 veterinary science, 03 medical and health sciences, 0302 clinical medicine, Dogs, Medicine, Hamartoma, Animals, Dog Diseases, Molecular Biology, Sclerosis, business.industry, Leptomeninges, 04 agricultural and veterinary sciences, Cell Biology, medicine.disease, medicine.anatomical_structure, Choroid Plexus, Choroid plexus, Female, business, Neural development, 030217 neurology & neurosurgery

Abstract

Microscopic examination of the brain of adult Beagle dogs from four different general toxicity studies revealed the presence of ectopic choroid plexus tissue in six individual dogs (4 females and 2 males) with ages ranging from 12 to 18 months. In each dog, this finding was characterized by a well-circumscribed mass localized to a region above and along the corpus callosum without any apparent compression of adjacent brain tissue. Each mass was composed of columnar ependymal cells forming tubular structures surrounded by variable amounts of fibrovascular connective tissue and had the appearance of small rests of ependymal cells that had been penetrated by the leptomeninges during neural development. There were no associated clinical signs or macroscopic correlates. Based on morphologic appearance, a diagnosis of spontaneous ectopic choroid plexus with secondary sclerosis was made. To the authors’ knowledge, ectopic choroid plexus has not been reported in Beagle dogs and is rare in humans and horses.

Published

2018

14. Nervous System

Author

Mark T. Butt, David C. Dorman, Robert H. Garman, and Brad Bolon

Subjects

Nervous system, business.industry, Neurological function, Vulnerability, Neurotoxicity, Comparative biology, Neuropathology, Premature senescence, medicine.disease, Biomarker, Harm, medicine.anatomical_structure, Toxicity, medicine, Limited capacity, business, Neuroscience, Neuroanatomy

Abstract

Clinical diseases characterized by significant neurological deficits are among the most devastating outcomes produced by exposure to toxicants. The exquisite sensitivity of the nervous system results from its limited capacity, especially centrally, to reverse or compensate for destruction as well as its neural cell–specific mechanisms and manifestations of toxicity. Present regulatory approaches for detecting and managing neurotoxic risk generally regard any substantial toxicant-induced change in neural chemistry, function, or structure as harmful (i.e., adverse). Neurotoxicant-induced injury may appear as an acute illness or death, typically pointing to severe disruption in CNS function, or structure-associated with a high-dose exposure. Alternatively, early declines in neurological function (i.e., premature senescence) and/or the quality of life often follow chronic and low-level neurotoxicant exposure. The practice of toxicologic neuropathology requires an integrated understanding of comparative neurobiology (the major likenesses and dissimilarities among species, strains, ages, and genders) and correlative neurobiology (the relationship among neural structure, function, and chemistry) as well as a solid grasp of neurotoxicant classes, targets, and mechanisms.

Published

2018

15. Regulatory Testing for Developmental Neurotoxicology

Author

W.J. Bowers, Brad Bolon, Wolfgang Kaufmann, M. KGaA, Abby A. Li, Roland N. Auer, Robert H. Garman, and L.P. Sheets

Subjects

0301 basic medicine, Developmental neurotoxicity, Guideline, Key issues, Risk regulation, Developmental psychology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Risk analysis (engineering), Auditory startle, Motor activity, Workgroup, Risk assessment, Psychology, 030217 neurology & neurosurgery

Abstract

International and U.S. guidance for developmental neurotoxicity (DNT) testing of chemicals are provided by OECD DNT test guideline 426, OECD extended one-generation reproductive toxicity study (EOGRTS) test guideline 443, and U.S. EPA DNT test guideline 870.6300. These guidelines with their multiple behavioral and neuropathology endpoints are among the most logistically complex, labor-intensive bioassays conducted for regulatory purposes. This article identifies key issues in the practical implementation and analysis of neurobehavioral and neuropathology endpoints, with emphasis on quantitative brain morphometry testing requirements. This article also reviews the development of DNT guidelines, strengths and limitations of validation efforts, regulatory triggers for DNT testing, and recent guidance from government and workgroup efforts to enhance conduct and interpretation of studies for regulatory risk assessment purposes.

Published

2018

16. Brain Vacuolation Resulting From Administration of the Type II Ampakine CX717 Is An Artifact Related to Molecular Structure and Chemical Reaction With Tissue Fixative Agents

Author

Bernard S Jortner, James M. Cook, Brad Bolon, Gary Lynch, Michael Rajesh Stephen, Richard Purcell, Christine M. Gall, Arnold S. Lippa, Steven A. Johnson, Zhong Sheng, Daniel P. Radin, and Robert H. Garman

Subjects

0301 basic medicine, Ampakine, Male, Photomicrography, Pathology, medicine.medical_specialty, Patch-Clamp Techniques, medicine.drug_class, Vacuole, AMPA receptor, In Vitro Techniques, Toxicology, Rats, Sprague-Dawley, 03 medical and health sciences, Fixatives, 0302 clinical medicine, Parenchyma, medicine, Animals, Fixative, Brain Chemistry, Glial fibrillary acidic protein, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Neurotoxicity, Brain, Isoxazoles, Synaptic Potentials, medicine.disease, Macaca fascicularis, 030104 developmental biology, medicine.anatomical_structure, Astrocytes, Vacuoles, biology.protein, Female, Artifacts, 030217 neurology & neurosurgery, Astrocyte

Abstract

Ampakines are small molecule positive allosteric modulators of the alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA). One class II ("low impact") ampakine, CX717, has been implicated to have a neurotoxic effect based on findings in nonclinical, long-term toxicity studies. The neurotoxicity concerns, which halted the clinical development of the molecule, arose due to a finding of extensive white matter vacuolation in multiple brain regions of animals that were administered high doses of CX717 in several test species (unpublished data). This work characterized the features and a potential mechanism by which ampakines induce vacuoles in brain tissue. Brain sections from adult rats given CX717 (750 mg/kg BID by oral gavage) exhibited no vacuoles with acute or short-term dosing. However, after 14 or more days of treatment, vacuoles were prominent in cerebellum, globus pallidus, and hippocampus. Vacuole margins were lined by glial fibrillary acidic protein (GFAP), and by transmission electron microscopy were shown to be astrocyte processes. CX717-associated vacuoles occurred in formaldehyde-fixed specimens but not flash-frozen samples. Time-course experiments showed that brain tissue slices from CX717-treated animals exhibit no vacuoles until immersed in formaldehyde fixative, whereupon vacuoles form and expand in a time-dependent manner. Chemical interactions in test tube experiments have demonstrated that the combination of CX717 and formalin in an aqueous solution produces an exothermic reaction. Taken together, the data indicate that CX717 does not induce vacuoles in vivo, but rather is associated with astrocyte vacuolation post mortem, likely as the ampakine reacts with formalin to produce gas pockets in brain parenchyma.

Published

2017

17. Screening of Biochemical and Molecular Mechanisms of Secondary Injury and Repair in the Brain after Experimental Blast-Induced Traumatic Brain Injury in Rats

Author

C. Edward Dixon, Valerian E. Kagan, David V. Ritzel, Robert H. Garman, Patrick M. Kochanek, Hong Q. Yan, Geoffrey S.F. Ling, David Shellington, Richard A. Bauman, Larry W. Jenkins, Samuel S. Shin, Edwin K. Jackson, Robert S. B. Clark, Faris A. Bandak, Hülya Bayır, Peter V. Swauger, and Steven Parks

Subjects

Male, Adenosine monophosphate, Pathology, medicine.medical_specialty, Rats, Sprague-Dawley, chemistry.chemical_compound, Blast Injuries, Internal medicine, medicine, Animals, Macrophage inflammatory protein, Neuroinflammation, Oligonucleotide Array Sequence Analysis, Glial fibrillary acidic protein, biology, business.industry, Gene Expression Profiling, Original Articles, medicine.disease, Adenosine, Nerve Regeneration, Rats, Disease Models, Animal, Chronic traumatic encephalopathy, Adenosine diphosphate, medicine.anatomical_structure, Endocrinology, chemistry, Brain Injuries, Nerve Degeneration, biology.protein, Neurology (clinical), Transcriptome, business, Astrocyte, medicine.drug

Abstract

Explosive blast-induced traumatic brain injury (TBI) is the signature insult in modern combat casualty care and has been linked to post-traumatic stress disorder, memory loss, and chronic traumatic encephalopathy. In this article we report on blast-induced mild TBI (mTBI) characterized by fiber-tract degeneration and axonal injury revealed by cupric silver staining in adult male rats after head-only exposure to 35 psi in a helium-driven shock tube with head restraint. We now explore pathways of secondary injury and repair using biochemical/molecular strategies. Injury produced ∼25% mortality from apnea. Shams received identical anesthesia exposure. Rats were sacrificed at 2 or 24 h, and brain was sampled in the hippocampus and prefrontal cortex. Hippocampal samples were used to assess gene array (RatRef-12 Expression BeadChip; Illumina, Inc., San Diego, CA) and oxidative stress (OS; ascorbate, glutathione, low-molecular-weight thiols [LMWT], protein thiols, and 4-hydroxynonenal [HNE]). Cortical samples were used to assess neuroinflammation (cytokines, chemokines, and growth factors; Luminex Corporation, Austin, TX) and purines (adenosine triphosphate [ATP], adenosine diphosphate, adenosine, inosine, 2'-AMP [adenosine monophosphate], and 5'-AMP). Gene array revealed marked increases in astrocyte and neuroinflammatory markers at 24 h (glial fibrillary acidic protein, vimentin, and complement component 1) with expression patterns bioinformatically consistent with those noted in Alzheimer's disease and long-term potentiation. Ascorbate, LMWT, and protein thiols were reduced at 2 and 24 h; by 24 h, HNE was increased. At 2 h, multiple cytokines and chemokines (interleukin [IL]-1α, IL-6, IL-10, and macrophage inflammatory protein 1 alpha [MIP-1α]) were increased; by 24 h, only MIP-1α remained elevated. ATP was not depleted, and adenosine correlated with 2'-cyclic AMP (cAMP), and not 5'-cAMP. Our data reveal (1) gene-array alterations similar to disorders of memory processing and a marked astrocyte response, (2) OS, (3) neuroinflammation with a sustained chemokine response, and (4) adenosine production despite lack of energy failure-possibly resulting from metabolism of 2'-3'-cAMP. A robust biochemical/molecular response occurs after blast-induced mTBI, with the body protected from blast and the head constrained to limit motion.

Published

2013

18. STP Position Paper

Author

Laura A. Gumprecht, Alys Bradley, Lydia Andrews-Jones, Robert H. Garman, Mark T. Butt, Karl F. Jensen, Robert C. Sills, Brad Bolon, Ingrid D. Pardo, Ann Radovsky, and Aude Roulois

Subjects

Nervous system, Pathology, medicine.medical_specialty, Central nervous system, Eye, Toxicology, Nervous System, Pathology and Forensic Medicine, Midbrain, Toxicity Tests, Animals, Medicine, Molecular Biology, business.industry, Histological Techniques, Organ Size, Cell Biology, Anatomy, Spinal cord, Pons, medicine.anatomical_structure, Peripheral nervous system, Medulla oblongata, Optic nerve, business

Abstract

The Society of Toxicologic Pathology charged a Nervous System Sampling Working Group with devising recommended practices to routinely screen the central nervous system (CNS) and peripheral nervous system (PNS) in Good Laboratory Practice–type nonclinical general toxicity studies. Brains should be weighed and trimmed similarly for all animals in a study. Certain structures should be sampled regularly: caudate/putamen, cerebellum, cerebral cortex, choroid plexus, eye (with optic nerve), hippocampus, hypothalamus, medulla oblongata, midbrain, nerve, olfactory bulb (rodents only), pons, spinal cord, and thalamus. Brain regions may be sampled bilaterally in rodents using 6 to 7 coronal sections, and unilaterally in nonrodents with 6 to 7 coronal hemisections. Spinal cord and nerves should be examined in transverse and longitudinal (or oblique) orientations. Most Working Group members considered immersion fixation in formalin (for CNS or PNS) or a solution containing acetic acid (for eye), paraffin embedding, and initial evaluation limited to hematoxylin and eosin (H&E)-stained sections to be acceptable for routine microscopic evaluation during general toxicity studies; other neurohistological methods may be undertaken if needed to better characterize H&E findings. Initial microscopic analyses should be qualitative and done with foreknowledge of treatments and doses (i.e., “unblinded”). The pathology report should clearly communicate structures that were assessed and methodological details. Since neuropathologic assessment is only one aspect of general toxicity studies, institutions should retain flexibility in customizing their sampling, processing, analytical, and reporting procedures as long as major neural targets are evaluated systematically.

Published

2013

19. Toxicologic Pathology Analysis for Translational Neuroscience: Improving Human Risk Assessment Using Optimized Animal Data

Author

Brad Bolon, Ingrid D. Pardo, James P. Morrison, Alok K. Sharma, Deepa B. Rao, and Robert H. Garman

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Neurotoxicity Syndrome, Neuropathology, Toxicology, Risk Assessment, Translational Research, Biomedical, 03 medical and health sciences, Animal data, Structure-Activity Relationship, 0302 clinical medicine, medicine, Animals, Humans, Developmental neurotoxicity, business.industry, Translational medicine, Neurosciences, 030104 developmental biology, medicine.anatomical_structure, Neurotoxicity Syndromes, business, Risk assessment, 030217 neurology & neurosurgery, Translational neuroscience, Neuroanatomy

Abstract

A half-day American College of Toxicology continuing education course presented key issues often confronted by translational neuroscientists when predicting human risk from animal-derived toxicologic pathology data. Two talks correlated discrete structures with major functions in brains of rodents and nonrodents. The third lecture provided practical advice to obtain highly homologous rodent brain sections for quantitative morphometry in developmental neurotoxicity testing. The last presentation discussed demographic influences (eg, species, strain, sex, age), physiological attributes (eg, body composition, brain vascularity, pharmacokinetic/pharmacodynamic patterns, etc), and husbandry parameters (eg, group housing) recognized to impact the actions of neuroactive chemicals. Speakers described common cases of real-world challenges to animal data interpretation encountered when designing studies or extrapolating biological responses across species. The efficiency of translational neuroscience efforts will likely be enhanced as new methods (eg, high-resolution non-invasive imaging) improve our capability to cross-connect subtle anatomic and/or biochemical lesions with functional changes over time.

Published

2016

20. Severe Brief Pressure-Controlled Hemorrhagic Shock after Traumatic Brain Injury Exacerbates Functional Deficits and Long-Term Neuropathological Damage in Mice

Author

Patrick M. Kochanek, Samuel A. Tisherman, Joseph N. Hemerka, Vincent Vagni, Xianren Wu, Larry W. Jenkins, Brian Blasiole, David Shellington, Robert H. Garman, Jennifer L. Exo, Hülya Bayır, Mu Xu, C. Edward Dixon, Keri Janesko-Feldman, Robert S. B. Clark, and Stephen R. Wisniewski

Subjects

Silver Staining, Mean arterial pressure, animal structures, Cell Survival, Traumatic brain injury, Contusions, Morris water navigation task, Cell Count, Nerve Tissue Proteins, Neuropathology, Shock, Hemorrhagic, Hippocampus, Mice, Blast Injuries, Heart Rate, Glial Fibrillary Acidic Protein, medicine, Animals, Arterial Pressure, Maze Learning, Neurons, business.industry, Head injury, Nuclear Proteins, Original Articles, medicine.disease, Polytrauma, Blood Cell Count, nervous system diseases, DNA-Binding Proteins, Mice, Inbred C57BL, Blood pressure, Brain Injuries, Shock (circulatory), Anesthesia, Neurology (clinical), Nervous System Diseases, medicine.symptom, business, psychological phenomena and processes, Blood Chemical Analysis

Abstract

Hypotension after traumatic brain injury (TBI) worsens outcome. We published the first report of TBI plus hemorrhagic shock (HS) in mice using a volume-controlled approach and noted increased neuronal death. To rigorously control blood pressure during HS, a pressure-controlled HS model is required. Our hypothesis was that a brief, severe period of pressure-controlled HS after TBI in mice will exacerbate functional deficits and neuropathology versus TBI or HS alone. C57BL6 male mice were randomized into four groups (n=10/group): sham, HS, controlled cortical impact (CCI), and CCI+HS. We used a pressure-controlled shock phase (mean arterial pressure [MAP]=25–27 mm Hg for 35 min) and its treatment after mild to moderate CCI including, a 90 min pre-hospital phase, during which lactated Ringer's solution was given to maintain MAP >70 mm Hg, and a hospital phase, when the shed blood was re-infused. On days 14–20, the mice were evaluated in the Morris water maze (MWM, hidden platform paradigm). On day 21, the lesion and hemispheric volumes were quantified. Neuropathology and hippocampal neuron counts (hematoxylin and eosin [H&E], Fluoro-Jade B, and NeuN) were evaluated in the mice (n=60) at 24 h, 7 days, or 21 days (n=5/group/time point). HS reduced MAP during the shock phase in the HS and CCI+HS groups (p

Published

2012

21. Technical Guide for Nervous System Sampling of the Cynomolgus Monkey for General Toxicity Studies

Author

Daniel Morton, Walter F. Bobrowski, Ingrid D. Pardo, Klaus Weber, Jerry F. Hardisty, and Robert H. Garman

Subjects

Male, Nervous system, Nerve root, Dissection, Histological Techniques, Central nervous system, Brain, Anterior commissure, Cell Biology, Anatomy, Biology, Toxicology, Spinal cord, Pons, Pathology and Forensic Medicine, Macaca fascicularis, medicine.anatomical_structure, Spinal Cord, Dorsal root ganglion, Peripheral nervous system, Toxicity Tests, medicine, Animals, Female, Molecular Biology

Abstract

For general toxicity studies, a technique was designed to consistently sample the most important neuroanatomic regions of the brain, spinal cord, and peripheral nerve of cynomolgus monkeys using a limited number of blocks and slides. Using the most rostral portion of the pons as a landmark, the entire fixed brain was cut dorsoventrally into cross-sectional slabs 4 mm in thickness. For microscopic evaluation, six blocks of the brain at the levels of the frontal pole, anterior commissure, rostral thalamus, caudal thalamus, middle cerebellum with brainstem, and occipital lobe were trimmed to fit in standard tissue cassettes. Cross- and oblique sections of the spinal cord including the dorsal root ganglion and dorsal and ventral nerve roots were obtained at the levels of C1–C4, T10–T12, and L1–L4. Cross- and longitudinal sections of the sciatic nerve were also obtained. This technique offers a consistent and reliable method to routinely sample most of the important regions of the central and peripheral nervous system of monkeys using ten blocks. This method is readily adaptable to other species of nonhuman primates, dogs, and minipigs and can be quickly learned by the technicians performing the trimming procedures.

Published

2012

22. Clinicopathologic Features of Intracranial Central Neurocytomas in 2 Dogs

Author

D.P. Sponenberg, Pablo Piñeyro, Robert H. Garman, John H. Rossmeisl, and Bernard S. Jortner

Subjects

Male, Ependymoma, Pathology, medicine.medical_specialty, Neurology, Blotting, Western, Brain tumor, Neuropathology, Lateral ventricles, Dogs, Fatal Outcome, Microscopy, Electron, Transmission, Central neurocytoma, Animals, Medicine, Neurocytoma, Dog Diseases, General Veterinary, biology, Brain Neoplasms, business.industry, medicine.disease, Immunohistochemistry, Synaptophysin, biology.protein, Differential diagnosis, business

Abstract

Background In humans, central neurocytomas are rare and typically benign intracranial tumors found within the lateral ventricles, although extraventricular variants have been reported. Intracranial central neurocytomas have not been previously recognized in domestic animals. Objectives To describe the clinicopathologic features of canine intracranial central neurocytomas. Animals Two dogs with spontaneous intracranial and intraventricular neoplasms. Results Both dogs experienced seizures, rapid neurological deterioration, and death from tumor-associated complications within 5 days of the onset of clinical signs, and had neoplastic masses within the lateral ventricles. A brain MRI was performed in 1 dog, which revealed a T1-isointense, heterogeneously T2 and FLAIR hyperintense, and markedly and heterogeneously contrast-enhancing mass lesions within both lateral ventricles. Histologically, the neoplasms resembled oligodendrogliomas. The diagnosis of central neurocytoma was supported by documenting expression of multiple neuronal markers, including neuron-specific enolase, synaptophysin, neural-cell adhesion molecule, and neuronal nuclear antigen within the tumors, and ultrastructural evidence of neuronal differentiation of neoplastic cells. Conclusions and Clinical Importance Central neurocytoma should be a differential diagnosis for dogs with intraventricular brain masses. Morphologic differentiation of central neurocytoma from other intraventricular neoplasms, such as ependymoma or oligdendroglioma, can be difficult, and definitive diagnosis often requires immunohistochemical or ultrastructural confirmation of the neural origin of the neoplasm.

Published

2012

23. Oral toxicity of vigabatrin in immature rats: Characterization of intramyelinic edema

Author

Ihor Bekersky, Stephen D. Collins, Dwain Tolbert, Reid Patterson, Bernard S Jortner, Stephen Wanaski, Stephen M. Sagar, Mark Walzer, and Robert H. Garman

Subjects

Male, Time Factors, Dose, GABA Agents, Administration, Oral, Physiology, Motor Activity, Pharmacology, Toxicology, Risk Assessment, Vigabatrin, Rats, Sprague-Dawley, Eating, Myelin, Toxicity Tests, Animals, Edema, Sexual maturity, Medicine, Myelin Sheath, Behavior, Animal, Dose-Response Relationship, Drug, business.industry, General Neuroscience, Body Weight, Age Factors, Brain, Intramyelinic edema, Rats, medicine.anatomical_structure, Toxicity, Ultrastructure, Female, Animal studies, business, medicine.drug

Abstract

Two toxicologic studies of vigabatrin were conducted with immature Sprague Dawley rats to characterize intramyelinic edema (IME) formation and assess potential impact on behavioral measures. Study 1 was a dosage-ranging characterization of overall toxicity of vigabatrin in young, developing rats. Study 2 evaluated vacuolar brain lesions found in Study 1.During Study 1, immature Sprague Dawley rats were orally administered deionized water (vehicle control), or vigabatrin at 5, 15, or 50mg/kg/day for ≤ 9 weeks, beginning at postnatal day 4 (PND 4) and followed by a recovery period. Toxicologic observations were collected, including adverse clinical signs, body weight gains, food consumption, ophthalmoloscopy, electroretinograms, sexual maturation, motor activity, memory, and learning behaviors. At sacrifice, CNS tissues were examined by light microscopy for evidence of IME. In Study 2, immature Sprague Dawley rats were again orally administered vigabatrin (50mg/kg/day for ≤ 9 weeks, beginning at PND 4). At sacrifice, CNS tissues were examined by both light and transmission electron microscopy for evidence of IME.At 5-50mg/kg/day, dosage-related reduced food consumption, decreased body weight, and delayed sexual maturation were found. Persisting through recovery, effects were more pronounced in males. Increased degrees of vacuolation were observed on PND 67 only after a dosage of 50mg/kg/day, and were attenuated during recovery. Vacuolar-change morphology was characteristic of IME, with no evidence of cellular or neuritic degeneration. Ultrastructural analyses revealed brain vacuoles initiated as splits of myelin sheaths along intra-period lines. These splits expanded, evolving into large membrane-rich vacuoles, and were more prominent at later stages of myelin development. Hypomyelination and gliopathy were noted from PNDs 4-15, and were likely related to vigabatrin exposure during active myelination. A lesser degree of hypomyelination was observed from PNDs 4-46 and 4-65. Vacuolation was markedly attenuated in post-recovery-period rats.The present studies indicated toxicities in young rats at vigabatrin dosages lower than those reported for toxicities in older rats. Dosages50mg/kg/day did not affect CNS, behavior, and reproductive development. However, at the greatest dosage, some retardation of physical growth, delay in sexual maturation, reduction in physical strength, and induction of CNS stimulation (handling-induced spasms) occurred. The key pathologic finding was vacuolar brain lesions in the white and gray matter, which generally reversed upon drug discontinuation. Vacuoles were confined to myelin sheaths, consistent with observations in adult rats. Vigabatrin delayed but did not eliminate myelination despite continued dosing, an effect greatest during active myelination.

Published

2011

24. Blast Exposure in Rats with Body Shielding Is Characterized Primarily by Diffuse Axonal Injury

Author

Edwin K. Jackson, Patrick M. Kochanek, Richard A. Bauman, David V. Ritzel, Hülya Bayır, Steven Parks, Robert S. B. Clark, Peter V. Swauger, Valerian E. Kagan, Lawrence C. Tong, Larry W. Jenkins, Robert C. Switzer, Robert H. Garman, and C. Edward Dixon

Subjects

Male, Pathology, medicine.medical_specialty, Traumatic brain injury, H&E stain, Poison control, Diffuse Axonal Injury, Rats, Sprague-Dawley, Protective Clothing, Blast Injuries, medicine, Animals, Pounds per square inch, Blast wave, business.industry, Diffuse axonal injury, Brain, Apnea, Hypothermia, medicine.disease, Axons, Rats, Disease Models, Animal, Neurology (clinical), medicine.symptom, business

Abstract

Blast-induced traumatic brain injury (TBI) is the signature insult in combat casualty care. Survival with neurological damage from otherwise lethal blast exposures has become possible with body armor use. We characterized the neuropathologic alterations produced by a single blast exposure in rats using a helium-driven shock tube to generate a nominal exposure of 35 pounds per square inch (PSI) (positive phase duration ∼ 4 msec). Using an IACUC-approved protocol, isoflurane-anesthetized rats were placed in a steel wedge (to shield the body) 7 feet inside the end of the tube. The left side faced the blast wave (with head-only exposure); the wedge apex focused a Mach stem onto the rat's head. The insult produced ∼ 25% mortality (due to impact apnea). Surviving and sham rats were perfusion-fixed at 24 h, 72 h, or 2 weeks post-blast. Neuropathologic evaluations were performed utilizing hematoxylin and eosin, amino cupric silver, and a variety of immunohistochemical stains for amyloid precursor protein (APP), glial fibrillary acidic protein (GFAP), ionized calcium-binding adapter molecule 1 (Iba1), ED1, and rat IgG. Multifocal axonal degeneration, as evidenced by staining with amino cupric silver, was present in all blast-exposed rats at all time points. Deep cerebellar and brainstem white matter tracts were most heavily stained with amino cupric silver, with the morphologic staining patterns suggesting a process of diffuse axonal injury. Silver-stained sections revealed mild multifocal neuronal death at 24 h and 72 h. GFAP, ED1, and Iba1 staining were not prominently increased, although small numbers of reactive microglia were seen within areas of neuronal death. Increased blood-brain barrier permeability (as measured by IgG staining) was seen at 24 h and primarily affected the contralateral cortex. Axonal injury was the most prominent feature during the initial 2 weeks following blast exposure, although degeneration of other neuronal processes was also present. Strikingly, silver staining revealed otherwise undetected abnormalities, and therefore represents a recommended outcome measure in future studies of blast TBI.

Published

2011

25. Modern Pathology Methods for Neural Investigations

Author

Sarah L. Hale, Rogely W. Boyce, Lydia Andrews-Jones, Robert C. Switzer, Bernard S. Jortner, Georg Krinke, Robert H. Garman, Peter B. Little, Mark T. Butt, John T. Boyce, William H. Jordan, and Karl F. Jensen

Subjects

Societies, Scientific, Pathology, medicine.medical_specialty, business.industry, Stereology, Cell Biology, Neuropathology, Congresses as Topic, Neural tissues, Toxicology, Nervous System, Xenobiotics, Pathology and Forensic Medicine, Evaluation Studies as Topic, Toxicity Tests, Animals, Humans, Medicine, Neurotoxicity Syndromes, Sampling (medicine), Nervous System Diseases, business, Molecular Biology

Abstract

This session at the 2010 joint symposium of the Society of Toxicologic Pathology (STP) and the International Federation of Societies of Toxicologic Pathologists (IFSTP) explored modern neuropathology methods for assessing the neurotoxicologic potential of xenobiotics. Conventional techniques to optimally prepare and evaluate the central and peripheral neural tissues while minimizing artifact were reviewed, and optimal schemes were set forth for evaluation of the nervous system during both routine (i.e., general toxicity) studies and enhanced (i.e., specialized neurotoxicity) studies. Stereology was introduced as the most appropriate means of examining the possible impact of toxicants on neural cell numbers. A focused discussion on brain sampling took place among a panel of expert neuroscientists (anatomists and pathologists) and the audience regarding the proper balance between sufficient sampling and cost- and time-effectiveness of the analysis. No consensus was reached on section orientation (coronal sections of both sides vs. a parasagittal longitudinal section with several unilateral hemisections from the contralateral side), but most panelists favored sampling at least 8 sections (or approximately double to triple the current complement) in routine toxicity studies.

Published

2011

26. Useful Toxicologic Neuropathology References for Pathologists and Toxicologists

Author

Brad Bolon, Robert H. Garman, Alys Bradley, and Georg Krinke

Subjects

Cognitive science, Gerontology, Internet, business.industry, Neurosciences, Cell Biology, Neuropathology, Neural tissues, Toxicology, Pathology and Forensic Medicine, Toxicology studies, Temporal diversity, Basic knowledge, Neurobiology, Physicians, Medicine, Neurotoxicity Syndromes, Bibliographies as Topic, Nervous System Diseases, business, Molecular Biology

Abstract

Investigations in toxicologic neuropathology are complex undertakings because of the intricate spatial and temporal diversity in the anatomic, functional, and molecular organization of the central and peripheral nervous systems. This compilation of toxicologic neuropathology resources has been designed to consolidate a broad range of useful neurobiology, neuropathology, and neurotoxicology resources in a single reference. This collection will increase familiarity with the basic knowledge, skills, and tools required for the proficient practice of toxicologic neuropathology and should help to improve the analysis and interpretation of pathology data sets from neural tissues in toxicology studies.

Published

2010

27. Oral gavage subchronic neurotoxicity and inhalation subchronic immunotoxicity studies of ethylbenzene in the rat

Author

Donald G. Stump, Jacques P.J. Maurissen, John F. Barnett, Vanessa L. Peachee, James S. Bus, Sandra Hong, Abby A. Li, Robert H. Garman, Les Freshwater, and John A. Foss

Subjects

Male, Neurotoxicity Syndrome, No-observed-adverse-effect level, Dose, Neurotoxins, Administration, Oral, Motor Activity, Pharmacology, Toxicology, Rats, Sprague-Dawley, Eating, Sex Factors, Oral administration, Administration, Inhalation, Benzene Derivatives, Animals, Medicine, Neurologic Examination, Analysis of Variance, No-Observed-Adverse-Effect Level, Dose-Response Relationship, Drug, Inhalation, business.industry, Liver Diseases, General Neuroscience, Body Weight, Neurotoxicity, medicine.disease, Rats, Disease Models, Animal, Ophthalmology, Dose–response relationship, Toxicity, Female, Kidney Diseases, Neurotoxicity Syndromes, business

Abstract

The potential for neurotoxicological and immunotoxicological effects of ethylbenzene was studied in young adult Crl:CD(SD) rats following 90-day oral (neurotoxicity) or 28-day inhalation (immunotoxicity) exposures. In the neurotoxicity study, ethylbenzene was administered orally via gavage twice daily at 0, 25, 125, or 250 mg/kg per dose (total daily dosages of 0, 50, 250, or 500 mg/kg bwt/day [mg/kg bwt/day]) for 13 weeks and the functional observational battery (FOB), automated tests for motor activity and neuropathological examination were conducted. In the immunotoxicity study, animals were exposed by inhalation to 0, 25, 100, or 500 ppm ethylbenzene (approximately 26, 90, or 342 mg/kg bwt/day as calculated from physiologically based pharmacokinetic modeling). Immunotoxicity was evaluated in female rats using the splenic antibody-forming cell plaque-forming assay in sheep red blood cell sensitized animals. The no-observed-effect level for the oral gavage study was 50mg/kg bwt/day based on increased relative weights of the liver and kidneys in the male rats. The no-observed-adverse-effect level (NOAEL) for adult neurotoxicity was the highest dose tested 500 mg/kg bwt/day. The NOAEL for the immunotoxicity evaluation was the highest tested exposure concentration, 500 ppm (342 mg/kg bwt/day).

Published

2010

28. Exsanguination cardiac arrest in rats treated by 60min, but not 75min, emergency preservation and delayed resuscitation is associated with intact outcome

Author

Samuel A. Tisherman, S. William Stezoski, Tomas Drabek, Jeremy Henchir, Patrick M. Kochanek, Jason Stezoski, Fei Han, and Robert H. Garman

Subjects

Male, inorganic chemicals, Resuscitation, Time Factors, Emergency Nursing, Drug Administration Schedule, law.invention, Brain ischemia, Electrolytes, Hypothermia, Induced, law, Intensive care, medicine, Cardiopulmonary bypass, Animals, Cardiopulmonary Bypass, business.industry, Hypothermia, medicine.disease, Esmolol, Cardiopulmonary Resuscitation, Heart Arrest, Rats, Anesthesia, Emergency Medicine, Nervous System Diseases, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Reperfusion injury, Perfusion, medicine.drug

Abstract

Emergency preservation and resuscitation (EPR) is a new approach for resuscitation of exsanguination cardiac arrest (CA) victims to buy time for surgical hemostasis. EPR uses a cold aortic flush to induce deep hypothermic preservation, followed by resuscitation with cardiopulmonary bypass (CPB). We previously reported that 20 min of EPR was feasible with intact outcome. In this report, we tested the limits for EPR in rats. Adult male isoflurane-anesthetized rats were subjected to rapid hemorrhage (12.5 ml over 5 min), followed by esmolol/KCl-induced CA and 1 min of no-flow. EPR was then induced by perfusion with 270 ml of ice-cold Plasma-Lyte to decrease body temperature to 15 degrees C. After 60 min (n=7) or 75 min (n=7) of EPR, resuscitation was attempted with CPB over 60 min, blood transfusion, correction of acid-base balance and electrolyte disturbances, and mechanical ventilation for 2h. Survival, overall performance category (OPC: 1=normal, 5=death), neurological deficit score (NDS), and histological damage score (HDS) were assessed in survivors on day 3. While all rats after 60 min EPR survived, only two out of seven rats after 75 min EPR survived (p

Published

2007

29. Emergency Preservation and Resuscitation with Profound Hypothermia, Oxygen, and Glucose Allows Reliable Neurological Recovery after 3 h of Cardiac Arrest from Rapid Exsanguination in Dogs

Author

Jeremy Henchir, Edwin K. Jackson, Tomas Drabek, Jason Stezoski, Patrick M. Kochanek, Robert H. Garman, Samuel A. Tisherman, Sherman Culver, Xianren Wu, and S. William Stezoski

Subjects

Male, Emergency Medical Services, Resuscitation, Consciousness, Critical Care, medicine.medical_treatment, Body Temperature, law.invention, Dogs, Hypothermia, Induced, law, Intensive care, medicine, Cardiopulmonary bypass, Animals, Neuropreservation, Cardiopulmonary resuscitation, Saline, Cardiopulmonary Bypass, biology, business.industry, Fissipedia, Brain, Hypothermia, biology.organism_classification, Cardiopulmonary Resuscitation, Heart Arrest, Oxygen, Glucose, Treatment Outcome, Neurology, Anesthesia, Neurology (clinical), Nervous System Diseases, medicine.symptom, Cardiology and Cardiovascular Medicine, business

Abstract

We have used a rapid induction of profound hypothermia (> 10°C) with delayed resuscitation using cardiopulmonary bypass (CPB) as a novel approach for resuscitation from exsanguination cardiac arrest (ExCA). We have defined this approach as emergency preservation and resuscitation (EPR). We observed that 2 h but not 3 h of preservation could be achieved with favorable outcome using ice-cold normal saline flush to induce profound hypothermia. We tested the hypothesis that adding energy substrates to saline during induction of EPR would allow intact recovery after 3 h CA. Dogs underwent rapid ExCA. Two minutes after CA, EPR was induced with arterial ice-cold flush. Four treatments ( n = 6/group) were defined by a flush solution with or without 2.5% glucose (G + or G–) and with either oxygen or nitrogen (O + or O–) rapidly targeting tympanic temperature of 8°C. At 3 h after CA onset, delayed resuscitation was initiated with CPB, followed by intensive care to 72 h. At 72 h, all dogs in the O + G + group regained consciousness, and the group had better neurological deficit scores and overall performance categories than the O—groups (both P < 0.05). In the O + G—group, four of the six dogs regained consciousness. All but one dog in the O—groups remained comatose. Brain histopathology in the O—G + was worse than the other three groups ( P < 0.05). We conclude that EPR induced with a flush solution containing oxygen and glucose allowed satisfactory recovery of neurological function after a 3 h of CA, suggesting benefit from substrate delivery during induction or maintenance of a profound hypothermic CA.

Published

2007

30. Prolonged deep hypothermic circulatory arrest in rats can be achieved without cognitive deficits

Author

Patrick M. Kochanek, Robert H. Garman, Xianren Wu, Samuel A. Tisherman, Tomas Drabek, Stephen R. Wisnewski, Jason Stezoski, Jesse A. Fisk, and C. Edward Dixon

Subjects

Male, medicine.medical_specialty, Critical Care, Morris water navigation task, Hematocrit, General Biochemistry, Genetics and Molecular Biology, law.invention, Rats, Sprague-Dawley, law, Cardiopulmonary bypass, medicine, Animals, Effects of sleep deprivation on cognitive performance, General Pharmacology, Toxicology and Pharmaceutics, Maze Learning, Neurons, Cardiopulmonary Bypass, medicine.diagnostic_test, business.industry, Brain, Cognition, Reflex, Vestibulo-Ocular, General Medicine, Rats, Cardiac surgery, Circulatory Arrest, Deep Hypothermia Induced, surgical procedures, operative, Anesthesia, Deep hypothermic circulatory arrest, Reflex, Blood Gas Analysis, Cognition Disorders, business, Psychomotor Performance, circulatory and respiratory physiology

Abstract

Cardiopulmonary bypass (CPB) and deep hypothermic circulatory arrest (DHCA) enable surgical repair of cardiovascular defects. However, neurological complications can result after both CPB and DHCA. We sought to investigate if 75 min of CPB or DHCA caused motor, cognitive or histological deficits in rats. Three groups were studied: DHCA, CPB, and sham. Rats in the DHCA group were subjected to 75 min DHCA at 15 degrees C, with a total CPB duration of 75 min. Rats in the CPB group were subjected to 75 min of normothermic CPB. Shams received the same anesthesia, cannulations and infusions. Motor function was assessed using beam testing on days 3-13. Cognitive performance was evaluated using Morris water maze tasks on days 7-13. Overall Performance Category (OPC) and Neurologic Deficit Score (NDS) were assessed daily. Histological Damage Score (HDS) was assessed in survivors on day 14. Sustained deficits on beam testing were seen only in the CPB group. Rats in the CPB and DHCA groups exhibited similar cognitive performance vs. sham. There were no differences in OPC or NDS between groups. Neuronal degeneration was present only in small foci in rats after DHCA (n=4/7). However, HDS was not different in individual brain regions or viscera between DHCA or CPB vs. sham. Surprisingly, CPB, but not DHCA was associated with motor deficits vs. sham, and no cognitive deficits were seen in either group vs. sham. Future studies with longer DHCA duration will be necessary to provide targets to assess novel preservation strategies.

Published

2007

31. Emergency preservation and delayed resuscitation allows normal recovery after exsanguination cardiac arrest in rats: A feasibility trial*

Author

Xianren Wu, Larry W. Jenkins, S. William Stezoski, Samuel A. Tisherman, Patrick M. Kochanek, Tomas Drabek, Robert H. Garman, Jason Stezoski, and Jesse A. Fisk

Subjects

Male, inorganic chemicals, Resuscitation, Time Factors, Critical Care and Intensive Care Medicine, law.invention, Rats, Sprague-Dawley, Brain ischemia, law, Intensive care, Cardiopulmonary bypass, Animals, Medicine, Cardiopulmonary Bypass, business.industry, Hypothermia, medicine.disease, Rats, Sprague dawley, Circulatory Arrest, Deep Hypothermia Induced, Circulacion extracorporea, Shock (circulatory), Anesthesia, Feasibility Studies, medicine.symptom, business

Abstract

Emergency preservation and resuscitation (EPR) comprise a novel approach for resuscitation of exsanguination cardiac arrest victims. EPR uses a cold aortic flush to induce deep hypothermic preservation, followed by resuscitation with cardiopulmonary bypass. Development of a rat EPR model would enable study of the molecular mechanisms of neuronal injury and the screening of novel agents for emergency preservation.A prospective, randomized study.University research facility.Adult male Sprague-Dawley rats.Isoflurane-anesthetized rats were subjected to lethal hemorrhage (12.5 mL for 5 mins), followed by KCl-induced cardiac arrest and 1 min of no flow. Three groups (n=6) were studied: hypothermic EPR (H-EPR; 0 degrees C flush; target temperature, 15 degrees C); normothermic EPR (N-EPR; 38 degrees C flush); and controls. After 20 mins of H-EPR or N-EPR, resuscitation was initiated with cardiopulmonary bypass for 60 mins and mechanical ventilation. Controls were subjected to complete experimental preparation and anesthesia without cardiac arrest, followed by 60 mins of cardiopulmonary bypass and mechanical ventilation. Surviving rats were extubated 2 hrs later. Survival, Overall Performance Category (1, normal; 5, death), Neurologic Deficit Score, Histologic Damage Score, and biochemistry were assessed in survivors on day 7.All rats in H-EPR and control groups survived, whereas none of the rats in the N-EPR group had restoration of spontaneous circulation. All rats in the H-EPR and control groups achieved Overall Performance Category 1, normal Neurologic Damage Score, and normal or near normal Histologic Damage Score and biochemical markers of organ injury.We have established an EPR model in rats showing no neurologic injury, despite an exsanguination cardiac arrest, followed by 20 mins of EPR using miniaturized cardiopulmonary bypass. Establishment of this model should facilitate application of molecular tools to study the effects of hypothermic preservation and reperfusion and to screen novel pharmacologic adjuncts.

Published

2007

32. Recommended Methods for Brain Processing and Quantitative Analysis in Rodent Developmental Neurotoxicity Studies

Author

Roland N. Auer, Wolfgang Kaufmann, Brad Bolon, Robert H. Garman, and Abby A. Li

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Rodent, Synaptogenesis, Neuropathology, Biology, Toxicology, Pathology and Forensic Medicine, 03 medical and health sciences, Mice, 0302 clinical medicine, biology.animal, medicine, Animals, Paraffin embedding, Molecular Biology, Developmental neurotoxicity, Brain Chemistry, Histological Techniques, Brain, Cell Biology, medicine.disease, Rats, Neuroanatomy, 030104 developmental biology, medicine.anatomical_structure, Heterotopia (medicine), Neurotoxicity Syndromes, 030217 neurology & neurosurgery, Maternal toxicity

Abstract

Neuropathology methods in rodent developmental neurotoxicity (DNT) studies have evolved with experience and changing regulatory guidance. This article emphasizes principles and methods to promote more standardized DNT neuropathology evaluation, particularly procurement of highly homologous brain sections and collection of the most reproducible morphometric measurements. To minimize bias, brains from all animals at all dose levels should be processed from brain weighing through paraffin embedding at one time using a counterbalanced design. Morphometric measurements should be anchored by distinct neuroanatomic landmarks that can be identified reliably on the faced block or in unstained sections and which address the region-specific circuitry of the measured area. Common test article–related qualitative changes in the developing brain include abnormal cell numbers (yielding altered regional size), displaced cells (ectopia and heterotopia), and/or aberrant differentiation (indicated by defective myelination or synaptogenesis), but rarely glial or inflammatory reactions. Inclusion of digital images in the DNT pathology raw data provides confidence that the quantitative analysis was done on anatomically matched (i.e., highly homologous) sections. Interpreting DNT neuropathology data and their presumptive correlation with neurobehavioral data requires an integrative weight-of-evidence approach including consideration of maternal toxicity, body weight, brain weight, and the pattern of findings across brain regions, doses, sexes, and ages.

Published

2015

33. Repetitive Mild Traumatic Brain Injury in the Developing Brain: Effects on Long-Term Functional Outcome and Neuropathology

Author

Cameron Dezfulian, Robert S. B. Clark, Robert H. Garman, Patrick M. Kochanek, Jesse Lewis, Emin Fidan, Valerian E. Kagan, Corina O. Bondi, Hülya Bayır, Henry Alexander, Jeffrey P. Cheng, and Anthony E. Kline

Subjects

0301 basic medicine, Male, Pathology, medicine.medical_specialty, External capsule, Traumatic brain injury, Morris water navigation task, Fluorescent Antibody Technique, Neuropathology, Corpus callosum, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Maze Learning, Brain Concussion, Microglia, Experimental model, Head injury, Recovery of Function, Original Articles, medicine.disease, Immunohistochemistry, Axons, Rats, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Neurology (clinical), Psychology, Cognition Disorders, 030217 neurology & neurosurgery

Abstract

Although accumulating evidence suggests that repetitive mild TBI (rmTBI) may cause long-term cognitive dysfunction in adults, whether rmTBI causes similar deficits in the immature brain is unknown. Here we used an experimental model of rmTBI in the immature brain to answer this question. Post-natal day (PND) 18 rats were subjected to either one, two, or three mild TBIs (mTBI) or an equivalent number of sham insults 24 h apart. After one or two mTBIs or sham insults, histology was evaluated at 7 days. After three mTBIs or sham insults, motor (d1–5), cognitive (d11–92), and histological (d21–92) outcome was evaluated. At 7 days, silver degeneration staining revealed axonal argyrophilia in the external capsule and corpus callosum after a single mTBI, with a second impact increasing axonal injury. Iba-1 immunohistochemistry showed amoeboid shaped microglia within the amygdalae bilaterally after mTBI. After three mTBI, there were no differences in beam balance, Morris water maze, and elevated plus maze performance versus sham. The rmTBI rats, however, showed impairment in novel object recognition and fear conditioning. Axonal silver staining was observed only in the external capsule on d21. Iba-1 staining did not reveal activated microglia on d21 or d92. In conclusion, mTBI results in traumatic axonal injury and microglial activation in the immature brain with repeated impact exacerbating axonal injury. The rmTBI in the immature brain leads to long-term associative learning deficit in adulthood. Defining the mechanisms damage from rmTBI in the developing brain could be vital for identification of therapies for children.

Published

2015

34. Induction of Profound Hypothermia for Emergency Preservation and Resuscitation Allows Intact Survival After Cardiac Arrest Resulting From Prolonged Lethal Hemorrhage and Trauma in Dogs

Author

Samuel A. Tisherman, S. William Stezoski, Patrick M. Kochanek, Jeremy Henchir, Xianren Wu, Tomas Drabek, Kristin Cochran, Jason Stezoski, and Robert H. Garman

Subjects

Male, Resuscitation, medicine.medical_treatment, Splenectomy, Hemorrhage, law.invention, Dogs, Hypothermia, Induced, law, Physiology (medical), Cardiopulmonary bypass, Animals, Medicine, Cardiopulmonary resuscitation, Saline, biology, business.industry, Fissipedia, Brain, Hypothermia, biology.organism_classification, Cardiopulmonary Resuscitation, Heart Arrest, Anesthesia, Wounds and Injuries, Emergencies, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Clinical death

Abstract

Background— Induction of profound hypothermia for emergency preservation and resuscitation (EPR) of trauma victims who experience exsanguination cardiac arrest may allow survival from otherwise-lethal injuries. Previously, we achieved intact survival of dogs from 2 hours of EPR after rapid hemorrhage. We tested the hypothesis that EPR would achieve good outcome if prolonged hemorrhage preceded cardiac arrest. Methods and Results— Two minutes after cardiac arrest from prolonged hemorrhage and splenic transection, dogs were randomized into 3 groups (n=7 each): (1) the cardiopulmonary resuscitation (CPR) group, resuscitated with conventional CPR, and the (2) EPR-I and (3) EPR-II groups, both of which received 20 L of a 2°C saline aortic flush to achieve a brain temperature of 10°C to 15°C. CPR or EPR lasted 60 minutes and was followed in all groups by a 2-hour resuscitation by cardiopulmonary bypass. Splenectomy was then performed. The CPR dogs were maintained at 38.0°C. In the EPR groups, mild hypothermia (34°C) was maintained for either 12 (EPR-I) or 36 (EPR-II) hours. Function and brain histology were evaluated 60 hours after rewarming in all dogs. Cardiac arrest occurred after 124±16 minutes of hemorrhage. In the CPR group, spontaneous circulation could not be restored without cardiopulmonary bypass; none survived. Twelve of 14 EPR dogs survived. Compared with the EPR-I group, the EPR-II group had better overall performance, final neurological deficit scores, and histological damage scores. Conclusions— EPR is superior to conventional CPR in facilitating normal recovery after cardiac arrest from trauma and prolonged hemorrhage. Prolonged mild hypothermia after EPR was critical for achieving intact neurological outcomes.

Published

2006

35. A ‘Best Practices’ Approach to Neuropathologic Assessment in Developmental Neurotoxicity Testing—for Today

Author

Karl F. Jensen, Barry Stuart, Georg Krinke, Robert H. Garman, and Brad Bolon

Subjects

Research design, Gerontology, 040301 veterinary sciences, Best practice, Neuropathology, Toxicology, Nervous System, 030226 pharmacology & pharmacy, Pathology and Forensic Medicine, 0403 veterinary science, 03 medical and health sciences, 0302 clinical medicine, Documentation, Pregnancy, Pathology, Animals, Humans, Medicine, Statistical analysis, Molecular Biology, Developmental neurotoxicity, business.industry, Histological Techniques, 04 agricultural and veterinary sciences, Cell Biology, Benchmarking, Neurology, Research Design, Prenatal Exposure Delayed Effects, Female, Neurotoxicity Syndromes, Engineering ethics, Nervous System Diseases, business, Risk assessment

Abstract

A key trait of developmental neurotoxicants is their ability to cause structural lesions in the immature nervous system. Thus, neuropathologic assessment is an essential element of developmental neurotoxicity (DNT) studies that are designed to evaluate chemically-induced risk to neural substrates in young humans. The guidelines for conventional DNT assays have been established by regulatory agencies to provide a flexible scaffold for conducting such studies; recent experience has launched new efforts to update these recommendations. The present document was produced by an ad hoc subcommittee of the Society of Toxicologic Pathology (STP) tasked with examining conventional methods used in DNT neuropathology in order to define the ‘best practices’ for dealing with the diverse requirements of both national (EPA) and international (OECD) regulatory bodies. Recommendations (including citations for relevant neurobiological and technical references) address all aspects of the DNT neuropathology examination: study design; tissue fixation, collection, processing, and staining; qualitative and quantitative evaluation; statistical analysis; proper control materials; study documentation; and personnel training. If followed, these proposals will allow pathologists to meet the need for a sound risk assessment (balanced to address both regulatory issues and scientific considerations) in this field today while providing direction for the research needed to further refine DNT neuropathology ‘best practices’ in the future.

Published

2006

36. Adenosine A1 Receptor Knockout Mice Develop Lethal Status Epilepticus after Experimental Traumatic Brain Injury

Author

Vincent Vagni, C. Edward Dixon, Patrick M. Kochanek, Jurgen Schnermann, Patricia K. Crumrine, Edwin K. Jackson, Christopher B. Washington, Keri L. Janesko, Robert S. B. Clark, Gregg E. Homanics, Robert H. Garman, and Larry W. Jenkins

Subjects

Male, medicine.medical_specialty, Genotype, Traumatic brain injury, medicine.medical_treatment, Status epilepticus, Hematocrit, Mice, Epilepsy, Adenosine A1 receptor, Sex Factors, Internal medicine, Animals, Medicine, Mice, Knockout, Hematologic Tests, medicine.diagnostic_test, Receptor, Adenosine A1, business.industry, Hemodynamics, Electroencephalography, Epilepsy, Post-Traumatic, medicine.disease, Adenosine receptor, Adenosine, Treatment Outcome, Endocrinology, Anticonvulsant, Neurology, Brain Injuries, Anesthesia, Female, Neurology (clinical), medicine.symptom, Cardiology and Cardiovascular Medicine, business, medicine.drug

Abstract

Adenosine, acting at A1 receptors, exhibits anticonvulsant effects in experimental epilepsy—and inhibits progression to status epilepticus (SE). Seizures after traumatic brain injury (TBI) may contribute to pathophysiology. Thus, we hypothesized that endogenous adenosine, acting via A1 receptors, mediates antiepileptic benefit after experimental TBI. We subjected A1-receptor knockout (ko) mice, heterozygotes, and wild-type (wt) littermates ( n = 115) to controlled cortical impact (CCI). We used four outcome protocols in male mice: (1) observation for seizures, SE, and mortality in the initial 2 h, (2) assessment of seizure score (electroencephalogram (EEG)) in the initial 2 h, (3) assessment of mortality at 24 h across injury levels, and (4) serial assessment of arterial blood pressure, heart rate, blood gases, and hematocrit. Lastly, to assess the influence of gender on this observation, we observed female mice for seizures, SE, and mortality in the initial 2 h. Seizure activity was noted in 83% of male ko mice in the initial 2 h, but was seen in no heterozygotes and only 33% of wt ( P < 0.05). Seizures in wt were brief (1 to 2 secs). In contrast, SE involving lethal sustained (>1 h) tonic clonic activity was uniquely seen in ko mice after CCI (50% incidence in males), ( P < 0.05). Seizure score was twofold higher in ko mice after CCI versus either heterozygote or wt ( P < 0.05). An injury-intensity dose–response for 24 h mortality was seen in ko mice ( P < 0.05). Physiologic parameters were similar between genotypes. Seizures were seen in 100% of female ko mice after CCI versus 14% of heterozygotes and 25% wt ( P < 0.05) and SE was restricted to the ko mice (83% incidence). Our data suggest a critical endogenous anticonvulsant action of adenosine at A1 receptors early after experimental TBI.

Published

2005

37. Evaluation of Large-Sized Brains for Neurotoxic Endpoints

Author

Robert H. Garman

Subjects

Pathology, medicine.medical_specialty, 040301 veterinary sciences, Neuropathology, Biology, Toxicology, 030226 pharmacology & pharmacy, Specimen Handling, Pathology and Forensic Medicine, 0403 veterinary science, Lesion, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Animals, Molecular Biology, Histological Techniques, Brain, 04 agricultural and veterinary sciences, Cell Biology, Anatomy, chemistry, Models, Animal, Neurotoxicity Syndromes, Fluoro-Jade stain, medicine.symptom, Artifacts

Abstract

Sampling of large-sized brains (eg, dog, primate) for microscopic examination is frequently inadequate to detect localized neurotoxic injury. Furthermore, the examination of H&E-stained sections alone will often be insufficient for the detection of subtle neuropathogic alteration. It is imperative for any pathologist evaluating brain sections to have knowledge of microscopic neuroanatomy and to also have some understanding of basic neurochemistry. When a focus of degeneration is detected within the brain, the pathologist needs to ascertain not only the specific anatomic location of this focus but also the neuroanatomic regions that project to and receive output from the injured focus. Because of the complexity of brain circuitry and the fact that the brain contains many distinctive neuron populations, many more brain sections are required for adequate microscopic evaluation than for any other body organ. Deciding which and how many areas should be examined, microscopically, from a large size brain is often problematic. Although any sampling protocol will be influenced by what is known about the test chemical, it has been well established that certain regions of the brain (eg, hippocampus and other components of the limbic system, basal ganglia, Purkinje neurons) are more susceptible than others to a variety of physical, metabolic, and chemical insults. Knowledge of these regional sensitivities will assist in guiding the pathologist in the development of an adequate sampling protocol.

Published

2003

38. The Neuropathologic Effects in Rats and Neurometabolic Effects in Humans of Large-Dose Remifentanil

Author

Robert H. Garman, Hiroto Kuwabara, John Barbaccia, Jeffery P. Hogg, W. Andrew Kofke, Ahmed F. Attaallah, Elizabeth Sinz, and Naresh Gupta

Subjects

Male, medicine.medical_specialty, Central nervous system, Receptors, Opioid, mu, Remifentanil, Rats, Sprague-Dawley, Central nervous system disease, Limbic system, Piperidines, Limbic System, medicine, Animals, Humans, Dose-Response Relationship, Drug, business.industry, Brain, Electroencephalography, medicine.disease, Rats, Analgesics, Opioid, Glucose, Anesthesiology and Pain Medicine, medicine.anatomical_structure, Opioid, Anesthesia, Toxicity, Hypermetabolism, Histopathology, business, medicine.drug

Abstract

Given in clinically relevant large doses to rats, mu-opioids produce limbic system hypermetabolism and histopathology. This investigation extends these observations, in both rats and humans, for the short-acting drug remifentanil, which allows more precise control and assessment of the effects of duration of opioid exposure. We performed two series of experiments: one in rats for neuropathologic effects and the second in humans for neurometabolic effects. Fifty mechanically ventilated rats received saline solution or remifentanil 20-160 microg x kg(-1) x min(-1) for 3 h, followed by neuropathologic evaluation 7 days later. Four volunteers underwent induction of anesthesia and endotracheal intubation with propofol and rocuronium administration followed by remifentanil infusion at 1-3 microg x kg(-1) x min(-1) with positron emission tomography evaluation of cerebral metabolic rate for glucose. In rats, dose-related electroencephalogram activation was evident and 19 of 40 remifentanil-treated rats showed brain damage, primarily in the limbic system (P0.01). In humans, cerebral metabolic rate for glucose in the temporal lobe increased from 6.29 +/- 0.32 to 7.68 +/- 1.05 mg x 100 g(-1) x min(-1) (P0.05). These data indicate that prolonged large-dose remifentanil infusion is neurotoxic in rats with congruent metabolic effects with brief infusion in humans and suggest that some adverse effects reported in rats may be clinically relevant.This study demonstrates dose-related remifentanil neurotoxicity in physiologically controlled rats with congruent brain metabolic effects in four humans undergoing positron emission tomography evaluation during brief large-dose remifentanil anesthesia. These data suggest that some adverse effects reported in rats may be clinically relevant.

Published

2002

39. Fundamentals of translational neuroscience in toxicologic pathology: optimizing the value of animal data for human risk assessment

Author

Wolfgang Kaufmann, James P. Morrison, Ingrid D. Pardo, Alok K. Sharma, Brad Bolon, Deepa Rao, and Robert H. Garman

Subjects

Value (ethics), Pathology, medicine.medical_specialty, Less invasive, Neuropathology, Toxicology, Risk Assessment, Pathology and Forensic Medicine, Translational Research, Biomedical, Animal data, Toxicity Tests, Medicine, Animals, Humans, Molecular Biology, business.industry, Translational medicine, Neurosciences, Cell Biology, Disease Models, Animal, medicine.anatomical_structure, Neurotoxicity Syndromes, business, Risk assessment, Translational neuroscience, Neuroanatomy

Abstract

A half-day Society of Toxicologic Pathology continuing education course on “Fundamentals of Translational Neuroscience in Toxicologic Pathology” presented some current major issues faced when extrapolating animal data regarding potential neurological consequences to assess potential human outcomes. Two talks reviewed functional–structural correlates in rodent and nonrodent mammalian brains needed to predict behavioral consequences of morphologic changes in discrete neural cell populations. The third lecture described practical steps for ensuring that specimens from rodent developmental neurotoxicity tests will be processed correctly to produce highly homologous sections. The fourth talk detailed demographic factors (e.g., species, strain, sex, and age); physiological traits (body composition, brain circulation, pharmacokinetic/pharmacodynamic patterns, etc.); and husbandry influences (e.g., group housing) known to alter the effects of neuroactive agents. The last presentation discussed the appearance, unknown functional effects, and potential relevance to humans of polyethylene glycol (PEG)–associated vacuoles within the choroid plexus epithelium of animals. Speakers provided real-world examples of challenges with data extrapolation among species or with study design considerations that may impact the interpretability of results. Translational neuroscience will be bolstered in the future as less invasive and/or more quantitative techniques are devised for linking overt functional deficits to subtle anatomic and chemical lesions.

Published

2014

40. Pleomorphic xanthoastrocytoma within the medulla oblongata of a young dog

Author

E. T. Hostnik, Bernard S Jortner, S. A. Kube, Robert H. Garman, and D. Hager

Subjects

Male, Pathology, medicine.medical_specialty, Tetraparesis, Nystagmus, Dissection (medical), Astrocytoma, Dogs, Medicine, Animals, Pleomorphic xanthoastrocytoma, Medulla Oblongata, General Veterinary, medicine.diagnostic_test, business.industry, Brain Neoplasms, Magnetic resonance imaging, Anatomy, medicine.disease, Magnetic Resonance Imaging, Vestibular Diseases, Medulla oblongata, Vertical nystagmus, medicine.symptom, business

Abstract

A 13-week-old male intact Poodle mix dog developed an acute onset of vestibular ataxia, tetraparesis, and vomiting. The patient presented ambulatory, tetraparetic, and ataxic with a head tilt to the left and a disconjugate nystagmus (rotary nystagmus with fast phase to the right in right eye and vertical nystagmus in left eye). There were absent postural reactions in the left pelvic and left thoracic limbs and decreased right-sided postural reactions. Magnetic resonance imaging demonstrated an intra-axial mass within the left midcaudal medulla oblongata. On gross dissection, there was a left-sided neoplasm in the medulla oblongata with surrounding hemorrhage. The histologic findings indicated that the mass was a pleomorphic xanthoastrocytoma. This tumor, an uncommon variant of an astrocytoma most often seen in children and young adult humans, has yet to be described in dogs.

Published

2014

41. Methods to identify and characterize developmental neurotoxicity for human health risk assessment. II: neuropathology

Author

Luz Claudio, Jerry F. Hardisty, Andrew S. Fix, Karl F. Jensen, Robert H. Garman, Bernard S. Jortner, and Susan A. Ferenc

Subjects

Developmental neurotoxicity, Nervous system, Pathology, medicine.medical_specialty, Health, Toxicology and Mutagenesis, Public Health, Environmental and Occupational Health, H&E stain, Neuropathology, Biology, Human health, medicine.anatomical_structure, medicine, book.journal, Risk assessment, Developmental neurobiology, book, Neuroanatomy

Abstract

Neuropathologic assessment of chemically induced developmental alterations in the nervous system for regulatory purposes is a multifactorial, complex process. This calls for careful qualitative and quantitative morphologic study of numerous brains at several developmental stages in rats. Quantitative evaluation may include such basic methods as determination of brain weight and dimensions as well as the progressively more complex approaches of linear, areal, or stereologic measurement of brain sections. Histologic evaluation employs routine stains (such as hematoxylin and eosin), which can be complemented by a variety of special and immunohistochemical procedures. These brain studies are augmented by morphologic assessment of selected peripheral nervous system structures. Studies of this nature require a high level of technical skill as well as special training on the part of the pathologist. The pathologist should have knowledge of normal microscopic neuroanatomy/neuronal circuitry and an understanding of basic principles of developmental neurobiology, such as familiarity with the patterns of physiologic or programmed cell de

Published

2001

42. Delayed, spontaneous hypothermia reduces neuronal damage after asphyxial cardiac arrest in rats

Author

Steven H. Graham, Robert H. Garman, Howard Ferimer, Clifton W. Callaway, Patrick M. Kochanek, Shawn D. Hicks, Robert W. Hickey, Peter Safar, and Henry Alexander

Subjects

Male, medicine.medical_specialty, Time Factors, Resuscitation, Thalamus, Hippocampus, Cerebellar Purkinje cell, Hypothermia, Critical Care and Intensive Care Medicine, Body Temperature, Rats, Sprague-Dawley, Lesion, Asphyxia, Random Allocation, Internal medicine, medicine, Animals, Single-Blind Method, Hypoxia, Brain, Temporal cortex, business.industry, Subiculum, Heart Arrest, Rats, Disease Models, Animal, medicine.anatomical_structure, Endocrinology, Anesthesia, Neuron, medicine.symptom, business

Abstract

Core temperature is reduced spontaneously after asphyxial cardiac arrest in rats. To determine whether spontaneous hypothermia influences neurologic damage after asphyxial arrest, we compared neurologic outcome in rats permitted to develop spontaneous hypothermia vs. rats managed with controlled normothermia.Male Sprague-Dawley rats were asphyxiated for 8 mins and resuscitated. After extubation, a cohort of rats was managed with controlled normothermia (CN) by placement in a servo-controlled incubator set to maintain rectal temperature at 37.4 degrees C for 48 hrs. CN rats were compared with permissive hypothermia (PH) rats that were returned to an ambient temperature environment after extubation. Rats were killed at either 72 hrs (PH72hr, n = 14; CN72hr, n = 9) or 6 wks (PH6wk, n = 6, CN6wk, n = 6) after resuscitation. PH72 rats were historic controls for the CN72 rats, whereas PH6 and CN6 rats were randomized and studied contemporaneously.A clinical neurodeficit score (NDS) was determined daily. A pathologist blinded to group scored 40 hematoxylin and eosin -stained brain regions for damage by using a 5-point scale (0 = none, 5 = severe). Quantitative analysis of CA1 hippocampus injury was performed by counting normal-appearing neurons in a defined subsection of CA1.Mean rectal temperatures measured in the PH6wk rats (n = 6) were 36.9, 34.8, 35.5, 36.7, and 37.4 degrees C at 2, 8, 12, 24, and 36 hrs, respectively. Mortality rate (before termination) was lower in PH compared with CN (0/20 vs. 7/15; p.005). PH demonstrated a more favorable progression of NDS (p = .04) and less weight loss (p.005) compared with CN. Median histopathology scores were lower (less damage) in PH72hr vs. CN72hr for temporal cortex (0 vs. 2.5), parietal cortex (0 vs. 2), thalamus (0 vs. 3), CA1 hippocampus (1.5 vs. 4.5), CA2 hippocampus (0 vs. 3.5), subiculum (0 vs. 4), and cerebellar Purkinje cell layer (2 vs. 4) (all p.05). There was almost complete loss of normal-appearing CA1 neurons in CN72hr rats (6 +/- 2 [mean +/- SD] normal neurons compared with 109 +/- 12 in naïve controls). In contrast, PH72hr rats demonstrated marked protection (97 +/- 23 normal-appearing neurons) that was still evident, although attenuated, at 6 wks (42 +/- 24 normal-appearing neurons, PH6wk).Rats resuscitated from asphyxial cardiac arrest develop delayed, mild to moderate, prolonged hypothermia that is neuroprotective.

Published

2000

43. Lack of Selective Developmental Neurotoxicity in Rat Pups from Dams Treated by Gavage with Chlorpyrifos

Author

Alan M. Hoberman, Jacques P.J. Maurissen, T. R. Hanley, and Robert H. Garman

Subjects

medicine.medical_specialty, Dose, Developmental toxicity, Biology, Toxicology, Endocrinology, medicine.anatomical_structure, Lactation, Internal medicine, Toxicity, medicine, Gestation, Weaning, Habituation, medicine.symptom, Weight gain

Abstract

Pregnant Sprague-Dawley rats were given chlorpyrifos (O:, O-diethyl-O:-[3,5,6-trichloro-2-pyridinyl] phosphorothioate; CPF) in corn oil by gavage from gestation day 6 (GD 6) through lactation day 10 (LD 10) at dosages of 0, 0.3, 1, or 5 mg/kg/day in a developmental neurotoxicity study that conformed to U.S. Environmental Protection Agency 1991 guidelines. GD 0 was the day when evidence of mating was observed and postnatal day 0 (PND 0) was the day of birth. Toxicity was limited to the highest dosage level (5 mg/kg/day) and, in the dams, consisted of muscle fasciculation, hyperpnea, and hyperreactivity. A nonsignificant overall trend toward weight gain and feed consumption was also observed in the high-dosage dams, with a statistically significant Group x Time interaction for reduced weight gain in the 5-mg/kg/day group near the end of gestation. Although many developmental indices were normal, pups from high-dosage dams had increased mortality soon after birth, gained weight more slowly than controls, and had several indications of slightly delayed maturation. The early deaths and delayed maturation were attributed to maternal toxicity, though a possible contributing role of direct pup toxicity in delayed development cannot be eliminated. In spite of the apparent delay in physical development, high-dosage pups tested just after weaning had normal learning and memory as tested on a T-maze spatial delayed-alternation task. Habituation, a primitive form of learning, was tested in 2 tasks (motor activity and auditory startle) and was not affected. No overt effects were noted in either dams or pups at 1 or 0.3 mg/kg/day. Based on these data, chlorpyrifos produced maternal and developmental toxicity in the 5-mg/kg/day-dosage group. There was no evidence of selective developmental neurotoxicity following exposure to chlorpyrifos.

Published

2000

44. Histopathology of Nasal Olfactory Mucosa from Selected Inhalation Toxicity Studies Conducted with Volatile Chemicals

Author

Larry G. Lomax, Kevin T. Morgan, Robert H. Garman, Jack R. Harkema, and Jerry F. Hardisty

Subjects

Male, medicine.medical_specialty, Pathology, 040301 veterinary sciences, Olfaction, Acetates, Methylmethacrylate, Biology, Toxicology, 030226 pharmacology & pharmacy, Pathology and Forensic Medicine, Rats, Sprague-Dawley, 0403 veterinary science, Lesion, 03 medical and health sciences, Olfactory mucosa, 0302 clinical medicine, Olfactory Mucosa, medicine, Animals, Regeneration, Organic Chemicals, Molecular Biology, Nose, Inflammation, Inhalation exposure, Inhalation Exposure, Metaplasia, Hyperplasia, Inhalation, Esters, 04 agricultural and veterinary sciences, Cell Biology, Rats, Inbred F344, Rats, medicine.anatomical_structure, Female, Histopathology, Atrophy, Nasal Cavity, Propionates, medicine.symptom, Olfactory epithelium

Abstract

In recent years, histopathologic changes have been reported in the olfactory mucosa of rodents exposed, by inhalation, to a variety of volatile chemicals. In order to better characterize these lesions, a panel of experienced pathologists reviewed microscopic lesions of the olfactory epithelium of rats reported in 10 inhalation studies conducted with 8 different chemicals. The objectives were to determine if the olfactory epithelial lesions are morphologically similar or different for the chemicals of interest, to develop and recommend appropriate diagnostic criteria and nomenclature to characterize the morphology of these olfactory lesions, and to provide specific criteria for judging the degree of severity of the olfactory changes in these studies. The results indicated that the distribution and nature of the lesions were similar in all the examined studies in which olfactory changes were observed. Recommended standardized nomenclature and diagnostic criteria and a uniform method for scoring lesion severity based on the extent of distribution and severity of tissue damage are presented.

Published

1999

45. Lack of developmental neurotoxicity of MN rgp 120/HIV-1 administered subcutaneously to neonatal rats

Author

Alan M. Hoberman, Michael Peterson, Mildred S. Christian, Laurel M. Hardy, John A. Foss, Robert H. Garman, and Jeanine L. Bussiere

Subjects

medicine.medical_specialty, Offspring, Injections, Subcutaneous, medicine.medical_treatment, HIV Envelope Protein gp120, Motor Activity, Toxicology, Rats, Sprague-Dawley, Embryonic and Fetal Development, Subcutaneous injection, Blood serum, Pregnancy, Internal medicine, Avoidance Learning, medicine, Animals, Sexual Maturation, Alum adjuvant, Maze Learning, AIDS Vaccines, Vaccines, Synthetic, Behavior, Animal, business.industry, Body Weight, Brain, Teratology, Rats, Milk, Endocrinology, Animals, Newborn, In utero, Prenatal Exposure Delayed Effects, Female, business, Adjuvant, Postpartum period

Abstract

The potential for neurotoxic effects was evaluated in rat off-spring after exposure in utero and/or during the neonatal period to a recombinant subunit vaccine of gp120 prepared from the MN strain of HIV-1 (MN rgp 120/HIV-1). Thirty pregnant female rats were given MN rgp120/HIV-1 with alum adjuvant, and 30 rats were given vehicle, once every 3 days from Day 1 of presumed gestation until parturition. One pup/sex/litter from treated and control group dams were given a daily subcutaneous injection, from Day 1 through Day 22 postpartum (PP) of vehicle, MN rgp120/HIV-1, MN rgp120/HIV-1 with alum, or MN rgp120/HIV-1 with QS-21 adjuvant. Neurobehavioral and physical development were evaluated (preweaning reflex and development, sexual maturation, motor activity, acoustic startle, passive avoidance, functional observational battery, and water M-maze testing), and tissues were processed for anatomical examination (whole and regional brain weights, and neuropathology). Administration of MN rgp120/HIV-1, with or without adjuvant, to pups did not cause any persistent effect on any parameter evaluated. Neurohistological examination did not reveal any pathological effects related to treatment. Thus, MN rgp120/HIV-1 alone or formulated as a vaccine does not cause neurotoxicity or developmental toxicity in neonatal rats after exposure in utero and/or during the neonatal period.

Published

1999

46. Opioid neurotoxicity: fentanyl-induced exacerbation of cerebral ischemia in rats

Author

Robert H. Garman, W. Andrew Kofke, Marie E. Rose, and Rosalyn Garman

Subjects

Male, Neurotoxins, Ischemia, Brain damage, Loading dose, Brain Ischemia, Fentanyl, Rats, Sprague-Dawley, Brain ischemia, medicine, Animals, Cerebral perfusion pressure, Molecular Biology, Analysis of Variance, Dose-Response Relationship, Drug, Maintenance dose, business.industry, General Neuroscience, medicine.disease, Rats, Analgesics, Opioid, Treatment Outcome, Opioid, Anesthesia, Neurology (clinical), medicine.symptom, business, Developmental Biology, medicine.drug

Abstract

We tested the hypothesis that fentanyl would worsen ischemia-induced brain damage. In two sequential protocols forty rats were physiologically monitored and controlled. In protocol 1, rats were randomized (n=10/group) to 30 min of control (N2O plus 0.4% halothane), low dose fentanyl (loading dose [LD] 50 micrograms kg-1, maintenance dose [MD] 2 micrograms kg-1 min-1), or high-dose fentanyl (LD 800 micrograms kg-1, MD 32 micrograms kg-1 min-1). After 15 min of fentanyl or sham infusion trimethaphan 0.5 mg was given i.v. and 3 min later bilateral carotid artery occlusion and blood withdrawal-induced hypotension were maintained for 12 min. At 18 h postischemia rats underwent cerebral perfusion fixation. Brain areas were graded from 0 (normal) to 5. In addition to analysis of specific regions, neuropathologic scores were also summated over all brain regions and analyzed to compute a summed neuropathologic score. In protocol 2, five control and five high-dose fentanyl rats were treated identically except that post-ischemic oxygenation was maintained for 6 h and cerebral perfusion-fixation was performed 6 h post-ischemia. Only the caudate/putamen was examined in protocol 2. Fentanyl worsened lesions in both fentanyl groups' summed neuropathologic scores (P=0.002) in protocol 1 and specifically, in the caudate/putamen (P

Published

1999

47. [Untitled]

Author

Gary M. Whitford, David H. Pashley, and Robert H. Garman

Subjects

Pathology, medicine.medical_specialty, Necrosis, Physiology, Stomach, Gastroenterology, Biology, Mucus, Molecular biology, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Edema, Toxicity, medicine, Gastric mucosa, medicine.symptom, Swelling, Fluoride

Abstract

These studies were done to determine the effectsof fluoride (F) on the structure and function of thecanine gastric mucosa and the possible protectiveeffects of 16,16-dimethylprostaglandin E2(dmPGE2). A portion of the stomach with its vascularsupply intact was mounted in a two-compartment chamber,one side of which contained a control solution. Minoreffects were caused by exposure to 1 mmol/liter F. Both 5 and 10 mmol/liter F caused markedincreases in the fluxes of water and Na, K, and H ions;mucus secretion; and tissue swelling and redness. Theextent of these changes did not increase appreciably upon exposure to 50 or 100 mmol/liter F.Histological findings included marked thinning of thesurface cell layer, reduced uptake of PAS stain,localized exfoliation and necrosis of surface cells,acute gastritis, and edema. It was concluded that:(1) the threshold F concentration for effects on thestructure and function of the gastric mucosa wasapproximately 1 mmol/liter; (2) the maximum ornear-maximum effects were caused by 10 mmol/liter F; (3) theeffects persisted for at least 6 hr after the exposure;and (4) dmPGE2 (0.5 μg/ml) did notattenuate the effects induced by F.

Published

1997

48. Contributors

Author

E. Terence Adams, Rick Adler, Carl L. Alden, Phillip M. Bartholomew, Joydeep Basu, Val R. Beasley, Brian R. Berridge, Timothy A. Bertram, Hyo-eun Bhang, Hugh E. Black, Brad Bolon, Gary A. Boorman, Denise I. Bounous, Rogely Waite Boyce, William M. Bracken, Amy E. Brix, Danielle Brown, Mark T. Butt, Glenn H. Cantor, Bruce D. Car, Vincent Castranova, Russell C. Cattley, Curtis Chan, Robert E. Chapin, Samuel M. Cohen, Steve Colegate, Daniel Cook, Paul S. Cooke, Torrie A. Crabbs, Dianne M. Creasy, James W. Crissman, John M. Cullen, Dimitry M. Danilenko, Barbara Davis, Myrtle A. Davis, T. Zane Davis, Ronald A. DeLellis, Nancy D. Denslow, Kelly L. Diegel, David C. Dorman, Richard R. Dubielzig, Stephen K. Durham, Sandy Eldridge, Susan A. Elmore, Jeffrey I. Everitt, Suzanne Fenton, Duncan C. Ferguson, Reuel Field, George L. Foley, William R. Foster, Jerry D. Frantz, Kathy Gabrielson, Shayne C. Gad, Elizabeth J. Galbreath, Dale R. Gardner, Robert H. Garman, Santokh Gill, Peter Glerup, Dale L. Goad, Mary Elizabeth Pecquet Goad, Nanna Grand, Benjamin T. Green, Kathryn E. Gropp, Hans Jørgen G. Gundersen, Diane Gunson, Ramesh C. Gupta, Sharon M. Gwaltney-Brant, Jeffery O. Hall, Wendy Halpern, Gordon C. Hard, Jerry F. Hardisty, Jack R. Harkema, Philip W. Harvey, Wanda M. Haschek, Kathleen Heinz-Taheny, Ronald A. Herbert, Eugene Herman, Mark Hoenerhoff, Ann Hubbs, David Hutto, Evan B. Janovitz, Kanwar Nasir M. Khan, Kevin P. Keenan, Roy L. Kerlin, John M. Kreeger, Kannan Krishnan, C. Frieke Kuper, Stephen T. Lee, Lois D. Lehman-McKeeman, Xiantang Li, Eric D. Lombardini, Calvert Louden, John W. Ludlow, David E. Malarkey, Peter C. Mann, Robert R. Maronpot, Kevin S. McDorman, Mark A. Melanson, Robert Mercer, Rosanna Mirabile, Ronald W. Moch, James P. Morrison, Daniel Morton, Laura Dill Morton, Sureshkumar Muthupalani, Kristen J. Nikula, Ricardo Ochoa, Michelle E. Pacheco-Thompson, Olga M. Pulido, Kip E. Panter, George A. Parker, Dale W. Porter, Douglas Reid Patterson, James A. Pfister, Carl A. Pinkert, Lila Ramaiah, Deepa B. Rao, Donald G. Robertson, Jennifer Rojko, Thomas J. Rosol, Colin G. Rousseaux, Daniel G. Rudmann, Christine Ruehl-Fehlert, Linda Sargent, Christina M. Satterwhite, Kenneth A. Schafer, Philip F. Solter, Robert C. Sills, Liz Simon, Mikala Skydsgaard, Graham S. Smith, Krishnan Sriram, Bryan L. Stegelmeier, John M. Sullivan, Catherine Sutcliffe, James A. Swenberg, Polina Sysa-Shah, Leandro Teixeira, Noriko Tsuchiya, John L. Vahle, John F. Van Vleet, Aurore Varela, Kenneth A. Voss, Robin M. Walker, Matthew A. Wallig, Gail L. Walter, Kevin D. Welch, Paul White, Christopher T. Winkelmann, Zbigniew W. Wojcinski, and Jeffrey C. Wolf

Published

2013

49. Opioid Neurotoxicity

Author

Richard L. Stiller, Robert H. Garman, Marie E. Rose, W A Kofke, and R Garman

Subjects

Male, Narcotics, medicine.medical_treatment, Nitrous Oxide, Blood Pressure, Brain damage, Loading dose, Body Temperature, Fentanyl, Rats, Sprague-Dawley, Random Allocation, Eosinophilia, Intubation, Intratracheal, Limbic System, medicine, Animals, Single-Blind Method, Cerebral perfusion pressure, Saline, Neurons, Cell Death, Dose-Response Relationship, Drug, business.industry, Maintenance dose, Brain, Electroencephalography, Respiration, Artificial, Rats, Oxygen, Anesthesiology and Pain Medicine, Opioid, Anesthesia, Anesthetics, Inhalation, Nerve Degeneration, Brain Damage, Chronic, Halothane, medicine.symptom, business, medicine.drug

Abstract

Opioids, when administered in large doses, produce brain damage, primarily in the limbic system and association areas in rats. This investigation examined the relationship between opioid dose and severity and frequency of brain damage in rats. Forty male Sprague-Dawley rats were anesthetized with halothane/N2O and underwent tracheal intubation, mechanical ventilation, arterial/venous cannulation, and insertion of a rectal temperature probe and biparietal electroencephalogram electrodes. After surgery, halothane was discontinued and O2/N2O 30%/70% was administered for 1 h. Rats were then randomly assigned to one of eight groups. The control group received a loading dose (LD) of 4 mL/kg of 0.9% normal saline solution (NSS) and a maintenance dose (MD) of 4 mL.kg-1.h-1 NSS. The other groups were given fentanyl lypophilized and reconstituted in NSS with the LD ranging from 50 to 3200 micrograms/kg and the MD from 2 to 128 micrograms.kg-1.min-1. After 2 h of fentanyl or NSS infusion; all rats received 100% O2 and, when alert, their tracheas were extubated; after 7 days the rats underwent cerebral perfusion fixation, followed by light microscopic evaluation. Histopathologic lesions (primarily eosinophilic neuron degeneration) were subjectively graded by a pathologist unaware of the experimental treatment; the grades were based on the percentage of dead neurons. There were no lesions observed in the brain areas in any of the control or 200-8 (LD, microgram/kg; MD, microgram.kg-1.min-1) groups. Eleven of 20 rats in the 400-16, 800-32, 1600-64, and 3200-18 groups showed evidence of brain damage primarily in limbic system structures and association areas (P < 0.05). Our data confirm that fentanyl produces limbic system brain damage in rats, and that the damage occurs over a broad range of doses.

Published

1996

50. Opioid Neurotoxicity

Author

W. Andrew Kofke, Robert H. Garman, Janine Janosky, and Marie E. Rose

Subjects

Anesthesiology and Pain Medicine

Published

1996