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1. Association of the FGF4L2 retrogene with fibrocartilaginous embolic myelopathy in dogs

Author

Colleen Embersics, Danika Bannasch, Kevin Batcher, Elizabeth C. Boudreau, Molly Church, Andrew Miller, Simon Platt, Jey Koehler, Natasha Olby, John Rossmeisl, Daniel Rissi, Robert Grahn, Jonas Donner, and Peter J. Dickinson

Subjects
canine, chondrodystrophy, FCE, fibroblast growth factor, Veterinary medicine, SF600-1100
Abstract

Abstract Background Fibrocartilaginous embolic myelopathy (FCE) is a well‐documented condition in dogs although rarely reported in chondrodystrophic breeds. Genetic associations have not been defined. Objectives Define the association of the chondrodystrophy‐associated FGF4L2 retrogene with histopathologically confirmed cases of FCE. Animals Ninety‐eight dogs with a histopathologic diagnosis of FCE. Methods Retrospective multicenter study. Dogs were genotyped for the FGF4L2 and FGF4L1 retrogenes using DNA extracted from formalin‐fixed, paraffin‐embedded tissue. Associations between breed, FCE and retrogene status were investigated with reference to a hospital population and known breed and general population allele frequencies. Results FGF4L2 genotype was defined in 89 FCE cases. Fibrocartilaginous embolic myelopathy was present in 22 dogs from FGF4L2‐segregating breeds with allele frequencies of ≥5%; however, all dogs were wild type. Two Labrador retrievers with FCE carried FGF4L2 alleles. Frequency of the FGF4L2 allele was significantly (P

Published
2024
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2. Oral cytarabine ocfosfate pharmacokinetics and assessment of leukocyte biomarkers in normal dogs

Author

Danielle M. Zwueste, Karen M. Vernau, William Vernau, Bruno H. Pypendop, Heather K. Knych, Carlos A. Rodrigues, Amir Kol, Maria Questa, and Peter J. Dickinson

Subjects
Ara‐C, Ara‐CTP, canine, Cytosar, HPLC, prodrug, Veterinary medicine, SF600-1100
Abstract

Abstract Background Cytosine arabinoside (Ara‐C) is a nucleoside analog prodrug utilized for immunomodulatory effects mediated by its active metabolite Ara‐CTP. Optimal dosing protocols for immunomodulation in dogs have not been defined. Cytarabine ocfosfate (CO) is a lipophilic prodrug of Ara‐C that can be administered PO and provides prolonged serum concentrations of Ara‐C. Objectives Provide pharmacokinetic data for orally administered CO and determine accumulation and functional consequences of Ara‐CTP within peripheral blood leukocytes. Animals Three healthy female hound dogs and 1 healthy male Beagle. Methods Prospective study. Dogs received 200 mg/m2 of CO PO q24h for 7 doses. Serum and cerebrospinal fluid (CSF) CO and Ara‐C concentrations were measured by liquid chromatography‐tandem mass spectroscopy (LC‐MS/MS). Complete blood counts, flow cytometry, and leukocyte activation assays were done up to 21 days. Incorporation of Ara‐CTP within leukocyte DNA was determined by LC‐MS/MS. Results Maximum serum concentration (Cmax) for Ara‐C was 456.1‐724.0 ng/mL (1.88‐2.98 μM) and terminal half‐life was 23.3 to 29.4 hours. Cerebrospinal fluid: serum Ara‐C ratios ranged from 0.54 to 1.2. Peripheral blood lymphocyte concentrations remained within the reference range, but proliferation rates poststimulation were decreased at 6 days. Incorporation of Ara‐CTP was not saturated and remained >25% of peak concentration at 13 days. Conclusions and Clinical Importance Oral CO may produce prolonged serum Ara‐C half‐lives at concentrations sufficient to induce functional changes in peripheral leukocytes and is associated with prolonged retention of DNA‐incorporated Ara‐CTP. Application of functional and active metabolite assessment is feasible and may provide more relevant data to determine optimal dosing regimens for Ara‐C‐based treatments.

Published
2023
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3. Intra- and Intertumoral Microglia/Macrophage Infiltration and Their Associated Molecular Signature Is Highly Variable in Canine Oligodendroglioma: A Preliminary Evaluation

Author

Ryan G. Toedebusch, Ning-Wei Wei, Kulani T. Simafranca, Jennie A. Furth-Jacobus, Ingrid Brust-Mascher, Susan L. Stewart, Peter J. Dickinson, Kevin D. Woolard, Chai-Fei Li, Karen M. Vernau, Frederick J. Meyers, and Christine M. Toedebusch

Subjects
dog, one health, galectin-3, transforming growth factor beta-1, glioblastoma, pediatric high-grade glioma, Veterinary medicine, SF600-1100
Abstract

The goal of this study was to define the glioma-associated microglia/macrophage (GAM) response and associated molecular landscape in canine oligodendrogliomas. Here, we quantified the intratumoral GAM density of low- and high-grade oligodendrogliomas compared to that of a normal brain, as well as the intratumoral concentration of several known GAM-derived pro-tumorigenic molecules in high-grade oligodendrogliomas compared to that in a normal brain. Our analysis demonstrated marked intra- and intertumoral heterogeneity of GAM infiltration. Correspondingly, we observed significant variability in the intratumoral concentrations of several GAM-associated molecules, unlike what we previously observed in high-grade astrocytomas. However, high-grade oligodendroglioma tumor homogenates (n = 6) exhibited an increase in the pro-tumorigenic molecules hepatocyte growth factor receptor (HGFR) and vascular endothelial growth factor (VEGF), as we observed in high-grade astrocytomas. Moreover, neoplastic oligodendrocytes displayed robust expression of GAL-3, a chimeric galectin implicated in driving immunosuppression in human glioblastoma. While this work identifies shared putative therapeutic targets across canine glioma subtypes (HGFR, GAL-3), it highlights several key differences in the immune landscape. Therefore, a continued effort to develop a comprehensive understanding of the immune microenvironment within each subtype is necessary to inform therapeutic strategies going forward.

Published
2023
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4. Antiviral treatment using the adenosine nucleoside analogue GS‐441524 in cats with clinically diagnosed neurological feline infectious peritonitis

Author

Peter J. Dickinson, Michael Bannasch, Sara M. Thomasy, Vishal D. Murthy, Karen M. Vernau, Molly Liepnieks, Elizabeth Montgomery, Kelly E. Knickelbein, Brian Murphy, and Niels C. Pedersen

Subjects
antiviral, cat, corona virus, ophthalmology, Veterinary medicine, SF600-1100
Abstract

Abstract Feline infectious peritonitis (FIP) is caused by a mutant biotype of the feline enteric coronavirus. The resulting FIP virus (FIPV) commonly causes central nervous system (CNS) and ocular pathology in cases of noneffusive disease. Over 95% of cats with FIP will succumb to disease in days to months after diagnosis despite a variety of historically used treatments. Recently developed antiviral drugs have shown promise in treatment of nonneurological FIP, but data from neurological FIP cases are limited. Four cases of naturally occurring FIP with CNS involvement were treated with the antiviral nucleoside analogue GS‐441524 (5‐10 mg/kg) for at least 12 weeks. Cats were monitored serially with physical, neurologic, and ophthalmic examinations. One cat had serial magnetic resonance imaging (MRI), cerebrospinal fluid (CSF) analysis (including feline coronavirus [FCoV]) titers and FCoV reverse transcriptase [RT]‐PCR) and serial ocular imaging using Fourier‐domain optical coherence tomography (FD‐OCT) and in vivo confocal microscopy (IVCM). All cats had a positive response to treatment. Three cats are alive off treatment (528, 516, and 354 days after treatment initiation) with normal physical and neurologic examinations. One cat was euthanized 216 days after treatment initiation following relapses after primary and secondary treatment. In 1 case, resolution of disease was defined based on normalization of MRI and CSF findings and resolution of cranial and caudal segment disease with ocular imaging. Treatment with GS‐441524 shows clinical efficacy and may result in clearance and long‐term resolution of neurological FIP. Dosages required for CNS disease may be higher than those used for nonneurological FIP.

Published
2020
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5. Clinicopathological characteristics of histiocytic sarcoma affecting the central nervous system in dogs

Author

Izumi Toyoda, William Vernau, Beverly K. Sturges, Karen M. Vernau, John Rossmeisl, Kurt Zimmerman, Chelsea M. Crowe, Kevin Woolard, Michelle Giuffrida, Robert J. Higgins, and Peter J. Dickinson

Subjects
canine, central nervous system, cerebrospinal fluid, neoplasia, Veterinary medicine, SF600-1100
Abstract

Abstract Background Histiocytic sarcoma affecting the central nervous system (CNS HS) in dogs may present as primary or disseminated disease, often characterized by inflammation. Prognosis is poor, and imaging differentiation from other CNS tumors can be problematic. Objective To characterize the clinicopathological inflammatory features, breed predisposition, and survival in dogs with CNS HS. Animals One hundred two dogs with HS, 62 dogs with meningioma. Methods Retrospective case series. Records were reviewed for results of cerebrospinal fluid (CSF) analysis, CBC, treatment, and outcome data. Results Predisposition for CNS HS was seen in Bernese Mountain Dogs, Golden Retrievers, Rottweilers, Corgis, and Shetland Sheepdogs (P ≤ .001). Corgis and Shetland Sheepdogs had predominantly primary tumors; Rottweilers had exclusively disseminated tumors. Marked CSF inflammation was characteristic of primary rather than disseminated HS, and neoplastic cells were detected in CSF of 52% of affected dogs. Increased neutrophil to lymphocyte ratios were seen in all groups relative to controls (P

Published
2020
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6. Case Report: MRI, Clinical, and Pathological Correlates of Bromethalin Toxicosis in Three Dogs

Author

Vishal D. Murthy, Ehren McLarty, Kevin D. Woolard, Rell L. Parker, Gregg Kortz, Jamie N. King, Robert H. Poppenga, Marguerite F. Knipe, and Peter J. Dickinson

Subjects
biopsy, bromethalin, canine, corticospinal tract, desmethylbromethalin, leukoencephalopathy, Veterinary medicine, SF600-1100
Abstract

Bromethalin toxicosis is an increasingly common clinical presentation in dogs that may be fatal depending on the extent of intoxication. Antemortem diagnosis of bromethalin toxicosis was achieved in three dogs by demonstration of the active metabolite desmethylbromethalin in fat or serum. Magnetic resonance imaging (MRI) findings were consistent with a diffuse leukoencephalopathy with restricted diffusion and prominent involvement of the corticospinal motor tracts on T2-weighted and diffusion-weighted sequences. Imaging findings were confirmed in one non-surviving dog at necropsy. Resolution of MRI abnormalities was demonstrated in one surviving dog that was consistent with the associated resolution of clinical signs. Initial findings in these dogs support further investigation of specific MRI patterns in cases of leukoencephalopathy to aid differential diagnosis. While antemortem detection of bromethalin and its metabolites confirms exposure, quantitation may be informative as a prognostic biomarker.

Published
2022
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7. Coronavirus Infection of the Central Nervous System: Animal Models in the Time of COVID-19

Author

Peter J. Dickinson

Subjects
GS-441524, remdesivir, SARS-CoV-2, feline infectious peritonitis (FIP), treatment, Veterinary medicine, SF600-1100
Abstract

Naturally occurring coronaviral infections have been studied for several decades in the context of companion and production animals, and central nervous system involvement is a common finding, particularly in cats with feline infectious peritonitis (FIP). These companion and production animal coronaviruses have many similarities to recent human pandemic-associated coronaviruses such as SARS-CoV, MERS-CoV, and SARS-CoV2 (COVID-19). Neurological involvement is being increasingly recognized as an important clinical presentation in human COVID-19 patients, often associated with para-infectious processes, and potentially with direct infection within the CNS. Recent breakthroughs in the treatment of coronaviral infections in cats, including neurological FIP, have utilized antiviral drugs similar to those currently in human COVID-19 clinical trials. Differences in specific coronavirus and host factors are reflected in major variations in incidence and mechanisms of CNS coronaviral infection and pathology between species; however, broad lessons relating to treatment of coronavirus infection present within the CNS may be informative across species.

Published
2020
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8. Current Understanding of the Genetics of Intervertebral Disc Degeneration

Author

Peter J. Dickinson and Danika L. Bannasch

Subjects
chondrodystrophy, fibroblast growth factor 4, heritable, intervertebral disc degeneration, retrogene, Veterinary medicine, SF600-1100
Abstract

Premature degeneration of the intervertebral disc and its association with specific chondrodystrophic dog breeds has been recognized for over a century. Several lines of evidence including disease breed predisposition, studies suggesting heritability of premature intervertebral disc degeneration (IVDD) and association of a dog chromosome 12 (CFA 12) locus with intervertebral disc calcification have strongly supported a genetic component in IVDD in dogs. Recent studies documenting association of IVDD with an overexpressing FGF4 retrogene on CFA 12 have opened up new areas of investigation to further define the pathophysiology of premature IVDD. While preliminary data from studies investigating FGF4 retrogenes in IVDD implicate FGF4 overexpression as a major disease factor, they have also highlighted knowledge gaps in our understanding of intervertebral disc herniation which is a complex and multifactorial disease process.

Published
2020
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9. FGF4L2 retrogene copy number is associated with intervertebral disc calcification and vertebral geometry in Nova Scotia Duck Tolling Retrievers

Author

Catarina A. Bianchi, Denis J. Marcellin-Little, Peter J. Dickinson, Tanya C. Garcia, Chai-Fei Li, Kevin Batcher, and Danika L. Bannasch

Subjects
General Veterinary, General Medicine
Abstract

OBJECTIVES To evaluate the effects of the chondrodystrophy-associated FGF4L2 retrogene on intervertebral disc (IVD) calcification and vertebral geometry. ANIMALS 22 Nova Scotia Duck Tolling Retrievers (NSDTR) with no FGF4L2 retrogene (n = 7, wild-type dogs), 1 retrogene copy (8, heterozygous dogs), or 2 retrogene copies (7, homozygous dogs). PROCEDURES Computed tomography (CT) scans of the vertebral column were analyzed using computer-aided design (CAD) software. IVD calcification, vertebral column length, and vertebral geometry of the third cervical (C3), 13th thoracic (T13), and first lumbar (L1) vertebrae were compared. RESULTS IVD calcification was not found in wild-type dogs. IVD calcification was more frequent in homozygous dogs than heterozygous (P = .008) or wild-type dogs (P < .001) and in heterozygous dogs compared to wild-type dogs (P < .001). Four IVDs were subclinically herniated in 3 dogs (2 homozygous, 1 heterozygous). Calcified IVD had a greater volume and surface area in heterozygous dogs than homozygous dogs. C3 vertebral canal height-to-width ratio was greater in homozygous dogs than heterozygous dogs (P = .044) and wild-type dogs (P = .010). CLINICAL RELEVANCE IVD calcification and vertebral geometry can be analyzed using CAD software. The presence of 1 or 2 FGF4L2 copies in the absence of the FGF4L1 retrogene has an additive effect on the number of calcified IVD and a minor effect on vertebral geometry in NSDTR dogs. Data support the use of FGF4L2 phenotyping to reduce clinical disease in segregating breeds and to monitor the introduction of wild-type alleles into fixed breed populations.

Published
2023
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10. Establishment and characterization of two novel patient‐derived lines from canine high‐grade glioma

Author

Morgan S. Schrock, Abigail A. Zalenski, Miranda M. Tallman, Luke Kollin, Anna Bratasz, Griffin Weeks, Margaret A. Miller, Courtney N. Sweeney, G. Elizabeth Pluhar, Michael R. Olin, William C. Kisseberth, R. Timothy Bentley, Peter J. Dickinson, Daniel York, Amy Webb, Xu Wang, Sarah Moore, Monica Venere, and Matthew K. Summers

Subjects
General Veterinary
Published
2023
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11. Immunohistochemical Characterization of Procaspase-3 Overexpression as a Druggable Target With PAC-1, a Procaspase-3 Activator, in Canine and Human Brain Cancers

Author

Lisa J. Schlein, Bahaa Fadl-Alla, Holly C. Pondenis, Stéphane Lezmi, Charles G. Eberhart, Amy K. LeBlanc, Peter J. Dickinson, Paul J. Hergenrother, and Timothy M. Fan

Subjects
glioma, meningioma, brain cancer, procaspase-3, PAC-1, canine comparative, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Gliomas and meningiomas are the most common brain neoplasms affecting both humans and canines, and identifying druggable targets conserved across multiple brain cancer histologies and comparative species could broadly improve treatment outcomes. While satisfactory cure rates for low grade, non-invasive brain cancers are achievable with conventional therapies including surgery and radiation, the management of non-resectable or recurrent brain tumors remains problematic and necessitates the discovery of novel therapies that could be accelerated through a comparative approach, such as the inclusion of pet dogs with naturally-occurring brain cancers. Evidence supports procaspase-3 as a druggable brain cancer target with PAC-1, a pro-apoptotic, small molecule activator of procaspase-3 that crosses the blood-brain barrier. Procaspase-3 is frequently overexpressed in malignantly transformed tissues and provides a preferential target for inducing cancer cell apoptosis. While preliminary evidence supports procaspase-3 as a viable target in preclinical models, with PAC-1 demonstrating activity in rodent models and dogs with spontaneous brain tumors, the broader applicability of procaspase-3 as a target in human brain cancers, as well as the comparability of procaspase-3 expressions between differing species, requires further investigation. As such, a large-scale validation of procaspase-3 as a druggable target was undertaken across 651 human and canine brain tumors. Relative to normal brain tissues, procaspase-3 was overexpressed in histologically diverse cancerous brain tissues, supporting procaspase-3 as a broad and conserved therapeutic target. Additionally, procaspase-3 expressing glioma and meningioma cell lines were sensitive to the apoptotic effects of PAC-1 at biologically relevant exposures achievable in cancer patients. Importantly, the clinical relevance of procaspase-3 as a potential prognostic variable was demonstrated in human astrocytomas of variable histologic grades and associated clinical outcomes, whereby tumoral procaspase-3 expression was negatively correlated with survival; findings which suggest that PAC-1 might provide the greatest benefit for patients with the most guarded prognoses.

Published
2019
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12. Whole genome variant association across 100 dogs identifies a frame shift mutation in DISHEVELLED 2 which contributes to Robinow-like syndrome in Bulldogs and related screw tail dog breeds.

Author

Tamer A Mansour, Katherine Lucot, Sara E Konopelski, Peter J Dickinson, Beverly K Sturges, Karen L Vernau, Shannon Choi, Joshua A Stern, Sara M Thomasy, Sophie Döring, Frank J M Verstraete, Eric G Johnson, Daniel York, Robert B Rebhun, Hsin-Yi Henry Ho, C Titus Brown, and Danika L Bannasch

Subjects
Genetics, QH426-470
Abstract

Domestic dog breeds exhibit remarkable morphological variations that result from centuries of artificial selection and breeding. Identifying the genetic changes that contribute to these variations could provide critical insights into the molecular basis of tissue and organismal morphogenesis. Bulldogs, French Bulldogs and Boston Terriers share many morphological and disease-predisposition traits, including brachycephalic skull morphology, widely set eyes and short stature. Unlike other brachycephalic dogs, these breeds also exhibit vertebral malformations that result in a truncated, kinked tail (screw tail). Whole genome sequencing of 100 dogs from 21 breeds identified 12.4 million bi-allelic variants that met inclusion criteria. Whole Genome Association of these variants with the breed defining phenotype of screw tail was performed using 10 cases and 84 controls and identified a frameshift mutation in the WNT pathway gene DISHEVELLED 2 (DVL2) (Chr5: 32195043_32195044del, p = 4.37 X 10-37) as the most strongly associated variant in the canine genome. This DVL2 variant was fixed in Bulldogs and French Bulldogs and had a high allele frequency (0.94) in Boston Terriers. The DVL2 variant segregated with thoracic and caudal vertebral column malformations in a recessive manner with incomplete and variable penetrance for thoracic vertebral malformations between different breeds. Importantly, analogous frameshift mutations in the human DVL1 and DVL3 genes cause Robinow syndrome, a congenital disorder characterized by similar craniofacial, limb and vertebral malformations. Analysis of the canine DVL2 variant protein showed that its ability to undergo WNT-induced phosphorylation is reduced, suggesting that altered WNT signaling may contribute to the Robinow-like syndrome in the screwtail breeds.

Published
2018
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16. Dose summation and image registration strategies for radiobiologically and anatomically corrected dose accumulation in pelvic re-irradiation

Author

M. Nix, Peter J Dickinson, Stephen Gregory, Julien Uzan, Louise Murray, Michael Aldred, Lynn Aspin, Ane L Appelt, Stina Svensson, Bashar Al-Qaisieh, and John Lilley

Subjects
Re-Irradiation, Radiobiology, Dose accumulation, Equivalent dose, business.industry, Cumulative dose, Radiotherapy Planning, Computer-Assisted, medicine.medical_treatment, Image registration, Radiotherapy Dosage, Hematology, General Medicine, Pelvis, Radiation therapy, Oncology, medicine, Humans, Radiology, Nuclear Medicine and imaging, Dose Fractionation, Radiation, Radiation treatment planning, Nuclear medicine, business
Abstract

Background Re-irradiation (reRT) is a promising technique for patients with localized recurrence in a previously irradiated area but presents major challenges. These include how to deal with anatomical change between two courses of radiotherapy and integration of radiobiology when summating original and re-irradiation doses. The Support Tool for Re-Irradiation Decisions guided by Radiobiology (STRIDeR) project aims to develop a software tool for use in a commercial treatment planning system to facilitate more informed reRT by accounting for anatomical changes and incorporating radiobiology. We evaluated three approaches to dose summation, incorporating anatomical change and radiobiology to differing extents. Methods In a cohort of 21 patients who previously received pelvic re-irradiation the following dose summation strategies were compared: (1) Rigid registration (RIR) and physical dose summation, to reflect the current clinical approach, (2) RIR and radiobiological dose summation in equivalent dose in 2 Gy fractions (EQD2), and (3) Patient-specific deformable image registration (DIR) with EQD2 dose summation. Results RIR and physical dose summation (Strategy 1) resulted in high cumulative organ at risk (OAR) doses being 'missed' in 14% of cases, which were highlighted by EQD2 dose summation (Strategy 2). DIR (with EQD2 dose summation; Strategy 3) resulted in improved OAR overlap and distance to agreement metrics compared to RIR (with EQD2 dose summation; Strategy 2) and was consistently preferred in terms of clinical utility. DIR was considered to have a clinically important impact on dose summation in 38% of cases. Conclusion Re-irradiation cases require individualized assessment when considering dose summation with the previous treatment plan. Fractionation correction is necessary to meaningfully assess cumulative doses and reduce the risk of unintentional OAR overdose. DIR can add clinically relevant information in selected cases, especially for significant anatomical change. Robust solutions for cumulative dose assessment offer the potential for future improved understanding of cumulative OAR tolerances.

Published
2021
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17. Serum phosphorylated neurofilament heavy chain as a diagnostic biomarker for progressive myelomalacia in dogs with thoracolumbar intervertebral disc herniation

Author

Michelle A. Giuffrida, Chai-Fei Li, Peter J Dickinson, Jacqueline Kroll, Christine M Toedebusch, Jill Hicks, and Vishal D. Murthy

Subjects
medicine.medical_specialty, Veterinary medicine, Urology, Intermediate Filaments, canine, Intervertebral disc herniation, Standard Article, chondrodystrophy, Spinal Cord Diseases, Cohort Studies, Myelopathy, Dogs, myelopathy, SF600-1100, medicine, Diagnostic biomarker, Animals, Deep pain, Veterinary Sciences, Dog Diseases, Prospective Studies, Intervertebral Disc, Neurofilament heavy chain, General Veterinary, business.industry, Neurological status, Curve analysis, medicine.disease, Standard Articles, spinal cord injury, Neurology, SMALL ANIMAL, prognosis, business, Myelomalacia, Biomarkers, Intervertebral Disc Displacement
Abstract

BackgroundSerum phosphorylated neurofilament-heavy chain (pNF-H) has not been longitudinally evaluated in dogs that develop progressive myelomalacia (PMM) after Type I intervertebral disc herniation (IVDH).ObjectivesTo determine if serum pNF-H concentrations would predict outcome of neuroligical disease in dogs with acute, severe thoracolumbar myelopathy secondary to Type I IVDH.AnimalsThirty-nine client-owned dogs with thoracolumbar myelopathy secondary to IVDH.MethodsProspective controlled cohort study. Serum was collected from dogs undergoing hemilaminectomy at multiple timepoints. Final neurological status was established at 12 months and groups were stratified accordingly. Comparisons between outcome and pNF-H concentration at each timepoint was examined using Kruskal-Wallis analysis of variance on ranks and receiver operator characteristics curve analysis.ResultsMedian serum pNF-H concentrations were not significantly different between deep pain negative dogs that did or did not recover at any timepoint (baseline: 0.37 ng/mL [0-0.9 ng/mL] vs 0 ng/mL [0-0.9 ng/mL], P > 1; 24 hours: 1.25 ng/mL [0.35-7.23 ng/mL] vs 1.53 ng/mL [0-11.94 ng/mL], P > 1; 48 hours: 1.22 ng/mL [0.63-6.62 ng/mL] vs 2.12 ng/mL [0-20.72 ng/mL], P > 1; 72 hours: 2.77 ng/mL [1.33-6.62 ng/mL] vs 16.69 ng/mL [4.02-40.12 ng/mL], P > 1). Dogs that developed PMM had significantly higher serum pNF-H concentrations after surgery compared to all other cohorts at 24 hours: 39.88 ng/mL (25.74-50.68 ng/mL); P

Published
2021

25. Expression and therapeutic targeting of BMI1 in canine gliomas

Author

Sami Al‐Nadaf, Kyle S. Peacott‐Ricardos, Peter J. Dickinson, Robert B. Rebhun, and Daniel York

Subjects
Polycomb Repressive Complex 1, Thiazoles, Dogs, General Veterinary, Animals, Dog Diseases, Glioma, Heterocyclic Compounds, 2-Ring
Abstract

The BMI1 proto-oncogene, polycomb ring finger protein (BMI1) is a key component of the epigenetic polycomb repressor complex 1, and has been associated with aggressive behaviour and chemotherapeutic resistance in various malignances including human gliomas. Similar to humans, spontaneous canine gliomas carry a poor prognosis with limited therapeutic options. BMI1 expression and the effects of BMI1 inhibition have not been evaluated in canine gliomas. Here, we demonstrate that BMI1 is highly expressed in canine gliomas. Although increased BMI1 protein expression correlated with higher glioma grade in western blot assays, this correlation was not observed in a larger sample set using immunohistochemical analysis. The BMI1 inhibitor, PTC-209, suppressed BMI1 expression in established canine glioma cell lines and resulted in antiproliferative activity when used alone and in combination with chemotherapeutic agents. PTC-209 targeting of BMI1 activated the retinoblastoma (RB) pathway through downregulation of total and phosphorylated RB, independent of INK4A/ARF signalling, likely through BMI1-inhibition mediated upregulation of p21. These data support the rationale for targeting of BMI1 signalling and the use of canine glioma as a translational therapeutic model for human disease.

Published
2022

26. Expression of microRNAs in plasma and in extracellular vesicles derived from plasma for dogs with glioma and dogs with other brain diseases

Author

Hirohito Yano, Hideo Akiyoshi, Peter J Dickinson, Sadatoshi Maeda, Toshiyuki Tanaka, Ryota Asahina, Kohei Nakata, Hiroaki Kamishina, Momoko Narita, and Hidetaka Nishida

Subjects
Brain Diseases, Pathology, medicine.medical_specialty, General Veterinary, Plasma samples, 040301 veterinary sciences, Chemistry, 0402 animal and dairy science, Glioma, 04 agricultural and veterinary sciences, General Medicine, medicine.disease, 040201 dairy & animal science, Extracellular vesicles, 0403 veterinary science, Extracellular Vesicles, MicroRNAs, Plasma, Dogs, microRNA, medicine, Animals, Dog Diseases
Abstract

OBJECTIVE To measure expression of microRNAs (miRNAs) in plasma and in extracellular vesicles (EVs) derived from plasma for dogs with glioma and dogs with other brain diseases. SAMPLE Plasma samples from 11 dogs with glioma and 19 control dogs with various other brain diseases. PROCEDURES EVs were isolated from plasma samples by means of ultracentrifugation. Expression of 4 candidate reference miRNAs (let-7a, miR-16, miR-26a, and miR-103) and 4 candidate target miRNAs (miR-15b, miR-21, miR-155, and miR-342-3p) was quantified with reverse transcription PCR assays. Three software programs were used to select the most suitable reference miRNAs from among the 4 candidate reference miRNAs. Expression of the 4 target miRNAs was then calculated relative to expression of the reference genes in plasma and EVs, and relative expression was compared between dogs with glioma and control dogs with other brain diseases. RESULTS The most suitable reference miRNAs were miR-16 for plasma and let-7a for EVs. Relative expression of miR-15b in plasma and in EVs was significantly higher in dogs with glioma than in control dogs. Relative expression of miR-342-3p in EVs was significantly higher in dogs with glioma than in control dogs. CONCLUSIONS AND CLINICAL RELEVANCE Results suggested that miR-15b and miR-342-3p have potential as noninvasive biomarkers for differentiating glioma from other intracranial diseases in dogs. However, more extensive analysis of expression in specific glioma subtypes and grades, compared with expression in more defined control populations, will be necessary to assess their clinical relevance.

Published
2020
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28. The Effects of

Author

Danika, Bannasch, Kevin, Batcher, Fabienne, Leuthard, Michael, Bannasch, Petra, Hug, Denis J, Marcellin-Little, Peter J, Dickinson, Michaela, Drögemüller, Cord, Drögemüller, and Tosso, Leeb

Subjects
Dogs, Animals, Intervertebral Disc Displacement
Abstract

Two

Published
2022

31. Neuro-Oncology

Author

Peter J Dickinson, Stephen B. Tatter, Ralph B. D'Agostino, Waldemar Debinski, Denise Herpai, Mindy Quigley, Thomas E. Cecere, John H. Rossmeisl, Jonathan Hinckley, John L. Robertson, Small Animal Clinical Sciences, and Biomedical Sciences and Pathobiology

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Center of excellence, Oncology and Carcinogenesis, Brain tumor, canine, EphA2, Convection, 03 medical and health sciences, 0302 clinical medicine, Dogs, Drug Delivery Systems, Internal medicine, medicine, AcademicSubjects/MED00300, Animals, Oncology & Carcinogenesis, bacterial cytotoxins, business.industry, Brain Neoplasms, Cytotoxins, Receptor, EphA2, IL13RA2, glioblastoma, Neurosciences, Cancer, Glioma, medicine.disease, EPH receptor A2, animal models, 030104 developmental biology, interstitial drug delivery, Basic and Translational Investigations, AcademicSubjects/MED00310, Neurology (clinical), Translational science, Convection-Enhanced Delivery, business, 030217 neurology & neurosurgery, Glioblastoma, Receptor
Abstract

Background. The interleukin-13 receptor alpha 2 (IL13RA2) and ephrin type A receptor 2 (EPHA2) are attractive therapeutic targets, being expressed in similar to 90% of canine and human gliomas, and absent in normal brain. Clinical trials using an earlier generation IL-13 based cytotoxin showed encouraging clinical effects in human glioma, but met with technical barriers associated with the convection-enhanced delivery (CED) method. In this study, IL-13 mutant and ephrin A1 (EFNA1)-based bacterial cytotoxins targeted to IL13RA2 and EPHA2 receptors, respectively, were administered locoregionally by CED to dogs with intracranial gliomas to evaluate their safety and preliminary efficacy. Methods. In this phase I, 3 + 3 dose escalation trial, cytotoxins were infused by CED in 17 dogs with gliomas expressing IL13RA2 or EPHA2 receptors. CED was performed using a shape-fitting therapeutic planning algorithm, reflux-preventing catheters, and real-time intraoperative MRI monitoring. The primary endpoint was to determine the maximum tolerated dose of the cytotoxic cocktail in dogs with gliomas. Results. Consistent intratumoral delivery of the cytotoxic cocktail was achieved, with a median target coverage of 70% (range, 40-94%). Cytotoxins were well tolerated over a dose range of 0.012-1.278 mu g/mL delivered to the target volume (median, 0.099 mu g/mL), with no dose limiting toxicities observed. Objective tumor responses, up to 94% tumor volume reduction, were observed in 50% (8/16) of dogs, including at least one dog in each dosing cohort >0.05 mu g/mL. Conclusions. This study provides preclinical data fundamental to the translation of this multireceptor targeted therapeutic approach to the human clinic. Wake Forest University Translational Sciences Institute, National Cancer Institute [R01CA139099, R01CA74145, P01CA207206]; Comprehensive Cancer Center of Wake Forest University Brain Tumor Center of Excellence; Hearn Fund for Brain Tumor Research; Pratto Fund for Brain Tumor Research; Dallas Ray Swing Brain Tumor Fund Published version This work was supported by grants from the Wake Forest University Translational Sciences Institute, National Cancer Institute (R01CA139099, R01CA74145, P01CA207206), the Comprehensive Cancer Center of Wake Forest University Brain Tumor Center of Excellence, Hearn Fund for Brain Tumor Research, Pratto Fund for Brain Tumor Research, and Dallas Ray Swing Brain Tumor Fund.

Published
2021

33. STEM-27. A PERIVASCULAR STEM CELL UNDERLIES VERTEBRATE MENINGEAL TUMORIGENESIS

Author

Joanna J. Phillips, Ophir D. Klein, Stephen Magill, Shawn L. Hervey-Jumper, David R. Raleigh, Martha A Cady, Brisa Palikuqi, Aparna Bhaduri, C.H. Lucas, Peter J Dickinson, Abrar Choudhury, and Elizabeth E. Crouch

Subjects
Cancer Research, biology, Meninges, Vertebrate, medicine.disease_cause, Cell biology, medicine.anatomical_structure, Oncology, Cancer stem cell, biology.animal, otorhinolaryngologic diseases, medicine, Immunohistochemistry, Tumor growth, Neurology (clinical), Stem cell, Carcinogenesis, Protein overexpression
Abstract

BACKGROUND Meningiomas are the most common primary intracranial tumors in humans and dogs, but biologic drivers and cell types underlying meningeal tumorigenesis are incompletely understood. Here we integrate meningioma single-cell RNA sequencing with stem cell approaches to define a perivascular stem cell underlying vertebrate meningeal tumorigenesis. METHODS Single-cell RNA sequencing was performed on 57,114 cells from 8 human meningiomas, 54,607 cells from 3 dog meningiomas, and human meningioma xenografts in mice. Results were validated using immunofluorescence (IF), immunohistochemistry (IHC), and deconvolution of bulk RNA sequencing of 200 human meningiomas. Mechanistic and functional studies were performed using clonogenic and limiting dilution assays, xenografts, and genetically engineered mouse models. RESULTS Copy number variant identification from human meningioma single cells distinguished tumor cells with loss of chr22q from non-tumor cells with intact chr22q. A single cluster distinguished by expression of Notch3 and other cancer stem cell genes had an intermediate level of loss of chr22q, suggesting this cluster may represent meningioma stem cells. In support of this hypothesis, pseudotime trajectory analysis demonstrated transcriptomic progression starting from Notch3+ cells and encompassing all other meningioma cell types. Notch3+ meningioma cells had transcriptomic concordance to mural pericytes, and IF/IHC of prenatal and adult human meninges, as well as lineage tracing using a Notch3-CreERT2 allele in mice, confirmed Notch3+ cells were restricted to the perivascular stem cell niche in mammalian meningeal development and homeostasis. Integrating human and dog meningioma single cells revealed Notch3+ cells in tumor and non-tumor clusters in dog meningiomas. Notch3 IF/IHC and cell-type deconvolution of bulk RNA sequencing showed Notch3+ cells were enriched in high-grade human meningiomas. Notch3 overexpression in human meningioma cells increased clonogenic growth in vitro, and increased tumorigenesis and tumor growth in vivo, decreasing overall survival. CONCLUSIONS Notch3+ stem cells in the perivascular niche underlie vertebrate meningeal tumorigenesis.

Published
2021
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34. Glioma-associated microglia/macrophages augment tumorigenicity in canine astrocytoma, a naturally occurring model of human glioma

Author

Christine M Toedebusch, Blaire Consales, Kevin D. Woolard, Vishal D. Murthy, Ryan Toedebusch, Ori Nagasaka, Marguerite Knipe, Beverly K. Sturges, Chai-Fei Li, Nicole Vinson, Peter J Dickinson, Pamela J. Lein, Karen M. Vernau, Ana Cristina Grodzki, and John C. Snyder

Subjects
0301 basic medicine, transforming growth factor, canine, microglia, Biology, 03 medical and health sciences, 0302 clinical medicine, Immune system, Rare Diseases, Downregulation and upregulation, Glioma, glioma, medicine, AcademicSubjects/MED00300, 2.1 Biological and endogenous factors, Aetiology, beta 1, neoplasms, Cancer, Microglia, transforming growth factor beta 1, Neurosciences, Astrocytoma, Transforming growth factor beta, medicine.disease, Phenotype, nervous system diseases, Brain Disorders, Brain Cancer, 030104 developmental biology, medicine.anatomical_structure, Canine Glioma, 030220 oncology & carcinogenesis, Basic and Translational Investigations, Cancer research, biology.protein, AcademicSubjects/MED00310
Abstract

Background Glioma-associated microglia/macrophages (GAMs) markedly influence glioma progression. Under the influence of transforming growth factor beta (TGFB), GAMs are polarized toward a tumor-supportive phenotype. However, neither therapeutic targeting of GAM recruitment nor TGFB signaling demonstrated efficacy in glioma patients despite efficacy in preclinical models, underscoring the need for a comprehensive understanding of the TGFB/GAM axis. Spontaneously occurring canine gliomas share many features with human glioma and provide a complementary translational animal model for further study. Given the importance of GAM and TGFB in human glioma, the aims of this study were to further define the GAM-associated molecular profile and the relevance of TGFB signaling in canine glioma that may serve as the basis for future translational studies. Methods GAM morphometry, levels of GAM-associated molecules, and the canonical TGFB signaling axis were compared in archived samples of canine astrocytomas versus normal canine brain. Furthermore, the effect of TGFB on the malignant phenotype of canine astrocytoma cells was evaluated. Results GAMs diffusely infiltrated canine astrocytomas. GAM density was increased in high-grade tumors that correlated with a pro-tumorigenic molecular signature and upregulation of the canonical TGFB signaling axis. Moreover, TGFB1 enhanced the migration of canine astrocytoma cells in vitro. Conclusions Canine astrocytomas share a similar GAM-associated immune landscape with human adult glioma. Our data also support a contributing role for TGFB1 signaling in the malignant phenotype of canine astrocytoma. These data further support naturally occurring canine glioma as a valid model for the investigation of GAM-associated therapeutic strategies for human malignant glioma.

Published
2021

35. Genome-wide association mapping in dogs enables identification of the homeobox gene, NKX2-8, as a genetic component of neural tube defects in humans.

Author

Noa Safra, Alexander G Bassuk, Polly J Ferguson, Miriam Aguilar, Rochelle L Coulson, Nicholas Thomas, Peta L Hitchens, Peter J Dickinson, Karen M Vernau, Zena T Wolf, and Danika L Bannasch

Subjects
Genetics, QH426-470
Abstract

Neural tube defects (NTDs) is a general term for central nervous system malformations secondary to a failure of closure or development of the neural tube. The resulting pathologies may involve the brain, spinal cord and/or vertebral column, in addition to associated structures such as soft tissue or skin. The condition is reported among the more common birth defects in humans, leading to significant infant morbidity and mortality. The etiology remains poorly understood but genetic, nutritional, environmental factors, or a combination of these, are known to play a role in the development of NTDs. The variable conditions associated with NTDs occur naturally in dogs, and have been previously reported in the Weimaraner breed. Taking advantage of the strong linkage-disequilibrium within dog breeds we performed genome-wide association analysis and mapped a genomic region for spinal dysraphism, a presumed NTD, using 4 affected and 96 unaffected Weimaraners. The associated region on canine chromosome 8 (pgenome =3.0 × 10(-5)), after 100,000 permutations, encodes 18 genes, including NKX2-8, a homeobox gene which is expressed in the developing neural tube. Sequencing NKX2-8 in affected Weimaraners revealed a G to AA frameshift mutation within exon 2 of the gene, resulting in a premature stop codon that is predicted to produce a truncated protein. The exons of NKX2-8 were sequenced in human patients with spina bifida and rare variants (rs61755040 and rs10135525) were found to be significantly over-represented (p=0.036). This is the first documentation of a potential role for NKX2-8 in the etiology of NTDs, made possible by investigating the molecular basis of naturally occurring mutations in dogs.

Published
2013
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36. Rapid inverse planning for pressure-driven drug infusions in the brain.

Author

Kathryn H Rosenbluth, Alastair J Martin, Stephan Mittermeyer, Jan Eschermann, Peter J Dickinson, and Krystof S Bankiewicz

Subjects
Medicine, Science
Abstract

Infusing drugs directly into the brain is advantageous to oral or intravenous delivery for large molecules or drugs requiring high local concentrations with low off-target exposure. However, surgeons manually planning the cannula position for drug delivery in the brain face a challenging three-dimensional visualization task. This study presents an intuitive inverse-planning technique to identify the optimal placement that maximizes coverage of the target structure while minimizing the potential for leakage outside the target. The technique was retrospectively validated using intraoperative magnetic resonance imaging of infusions into the striatum of non-human primates and into a tumor in a canine model and applied prospectively to upcoming human clinical trials.

Published
2013
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37. Genome-wide association analysis identifies a mutation in the thiamine transporter 2 (SLC19A3) gene associated with Alaskan Husky encephalopathy.

Author

Karen M Vernau, Jonathan A Runstadler, Emily A Brown, Jessie M Cameron, Heather J Huson, Robert J Higgins, Cameron Ackerley, Beverly K Sturges, Peter J Dickinson, Birgit Puschner, Cecilia Giulivi, G Diane Shelton, Brian H Robinson, Salvatore DiMauro, Andrew W Bollen, and Danika L Bannasch

Subjects
Medicine, Science
Abstract

Alaskan Husky Encephalopathy (AHE) has been previously proposed as a mitochondrial encephalopathy based on neuropathological similarities with human Leigh Syndrome (LS). We studied 11 Alaskan Husky dogs with AHE, but found no abnormalities in respiratory chain enzyme activities in muscle and liver, or mutations in mitochondrial or nuclear genes that cause LS in people. A genome wide association study was performed using eight of the affected dogs and 20 related but unaffected control AHs using the Illumina canine HD array. SLC19A3 was identified as a positional candidate gene. This gene controls the uptake of thiamine in the CNS via expression of the thiamine transporter protein THTR2. Dogs have two copies of this gene located within the candidate interval (SLC19A3.2 - 43.36-43.38 Mb and SLC19A3.1 - 43.411-43.419 Mb) on chromosome 25. Expression analysis in a normal dog revealed that one of the paralogs, SLC19A3.1, was expressed in the brain and spinal cord while the other was not. Subsequent exon sequencing of SLC19A3.1 revealed a 4bp insertion and SNP in the second exon that is predicted to result in a functional protein truncation of 279 amino acids (c.624 insTTGC, c.625 C>A). All dogs with AHE were homozygous for this mutation, 15/41 healthy AH control dogs were heterozygous carriers while 26/41 normal healthy AH dogs were wild type. Furthermore, this mutation was not detected in another 187 dogs of different breeds. These results suggest that this mutation in SLC19A3.1, encoding a thiamine transporter protein, plays a critical role in the pathogenesis of AHE.

Published
2013
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38. A Missense Variant in ALDH5A1 Associated with Canine Succinic Semialdehyde Dehydrogenase Deficiency (SSADHD) in the Saluki Dog

Author

Dennis P. O'Brien, Vidhya Jagannathan, Karen M. Vernau, Eduard A. Struys, Phillip L. Pearl, C. Titus Brown, Kevin D. Woolard, G. Diane Shelton, Tamer A. Mansour, Cord Drögemüller, Anna Letko, Thomas J. Van Winkle, Danika L. Bannasch, Derek D. Cissell, Emily A. Brown, K. Michael Gibson, Kaspar Matiasek, Florian König, Peter J Dickinson, Birthe Roos, Miriam Aguilar, Michael R Broome, Clinical chemistry, AGEM - Endocrinology, metabolism and nutrition, AGEM - Inborn errors of metabolism, and Amsterdam Neuroscience - Cellular & Molecular Mechanisms

Subjects
0301 basic medicine, Succinic semialdehyde dehydrogenase deficiency, Male, Developmental Disabilities, Succinic semialdehyde, chemistry.chemical_compound, GABA, 0302 clinical medicine, Cerebrospinal fluid, Missense mutation, GWAS, 2.1 Biological and endogenous factors, Aetiology, 610 Medicine & health, Genetics (clinical), gamma-Aminobutyric Acid, Cerebrospinal Fluid, SSADHD, 630 Agriculture, Inborn Errors, Brain, encephalopathy, 4-hydroxybutyric acid, Phenotype, whole-genome sequencing, Neurological, 590 Animals (Zoology), Female, Succinate-Semialdehyde Dehydrogenase, Metabolic Networks and Pathways, Biotechnology, medicine.medical_specialty, lcsh:QH426-470, ALDH5A1, precision medicine, Encephalopathy, Mutation, Missense, Biology, Article, 03 medical and health sciences, Dogs, Rare Diseases, Seizures, Internal medicine, medicine, inborn error of metabolism, succinic semialdehyde, Genetics, Aldehyde dehydrogenase 5 family, member A1, Animals, Amino Acid Sequence, Genetic Testing, Amino Acid Metabolism, Inborn Errors, Animal, Human Genome, Neurosciences, medicine.disease, Hyperintensity, inherited, Brain Disorders, Amino Acid Metabolism, lcsh:Genetics, Disease Models, Animal, 030104 developmental biology, Endocrinology, Orphan Drug, chemistry, Inborn error of metabolism, Disease Models, Mutation, 570 Life sciences, biology, Missense, 030217 neurology & neurosurgery, Genome-Wide Association Study
Abstract

Dogs provide highly valuable models of human disease due to the similarity in phenotype presentation and the ease of genetic analysis. Seven Saluki puppies were investigated for neurological abnormalities including seizures and altered behavior. Magnetic resonance imaging showed a diffuse, marked reduction in cerebral cortical thickness, and symmetrical T2 hyperintensity in specific brain regions. Cerebral cortical atrophy with vacuolation (status spongiosus) was noted on necropsy. Genome-wide association study of 7 affected and 28 normal Salukis revealed a genome-wide significantly associated region on CFA 35. Whole-genome sequencing of three confirmed cases from three different litters revealed a homozygous missense variant within the aldehyde dehydrogenase 5 family member A1 (ALDH5A1) gene (XM_014110599.2: c.866G&gt, A, XP_013966074.2: p.(Gly288Asp). ALDH5A1 encodes a succinic semialdehyde dehydrogenase (SSADH) enzyme critical in the gamma-aminobutyric acid neurotransmitter (GABA) metabolic pathway. Metabolic screening of affected dogs showed markedly elevated gamma-hydroxybutyric acid in serum, cerebrospinal fluid (CSF) and brain, and elevated succinate semialdehyde in urine, CSF and brain. SSADH activity in the brain of affected dogs was low. Affected Saluki dogs had striking similarities to SSADH deficiency in humans although hydroxybutyric aciduria was absent in affected dogs. ALDH5A1-related SSADH deficiency in Salukis provides a unique translational large animal model for the development of novel therapeutic strategies.

Published
2020
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39. Antiviral treatment using the adenosine nucleoside analogue GS-441524 in cats with clinically diagnosed neurological feline infectious peritonitis

Author

Vishal D. Murthy, Karen M. Vernau, Brian G Murphy, Elizabeth Montgomery, Molly L. Liepnieks, Sara M Thomasy, Michael J. Bannasch, Niels C Pedersen, Kelly E. Knickelbein, and Peter J Dickinson

Subjects
Male, Feline coronavirus, Pathology, medicine.medical_specialty, 040301 veterinary sciences, Central nervous system, cat, Case Report, Infectious Disease, Case Reports, 030204 cardiovascular system & hematology, medicine.disease_cause, Antiviral Agents, Virus, Feline Infectious Peritonitis, 0403 veterinary science, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, Adenosine Triphosphate, medicine, Animals, corona virus, Veterinary Sciences, CATS, lcsh:Veterinary medicine, General Veterinary, Nucleoside analogue, business.industry, Neurosciences, 04 agricultural and veterinary sciences, antiviral, Feline infectious peritonitis, Brain Disorders, ophthalmology, medicine.anatomical_structure, Infectious Diseases, Good Health and Well Being, Cats, lcsh:SF600-1100, Biomedical Imaging, Female, SMALL ANIMAL, business, Off Treatment, medicine.drug
Abstract

Feline infectious peritonitis (FIP) is caused by a mutant biotype of the feline enteric coronavirus. The resulting FIP virus (FIPV) commonly causes central nervous system (CNS) and ocular pathology in cases of noneffusive disease. Over 95% of cats with FIP will succumb to disease in days to months after diagnosis despite a variety of historically used treatments. Recently developed antiviral drugs have shown promise in treatment of nonneurological FIP, but data from neurological FIP cases are limited. Four cases of naturally occurring FIP with CNS involvement were treated with the antiviral nucleoside analogue GS‐441524 (5‐10 mg/kg) for at least 12 weeks. Cats were monitored serially with physical, neurologic, and ophthalmic examinations. One cat had serial magnetic resonance imaging (MRI), cerebrospinal fluid (CSF) analysis (including feline coronavirus [FCoV]) titers and FCoV reverse transcriptase [RT]‐PCR) and serial ocular imaging using Fourier‐domain optical coherence tomography (FD‐OCT) and in vivo confocal microscopy (IVCM). All cats had a positive response to treatment. Three cats are alive off treatment (528, 516, and 354 days after treatment initiation) with normal physical and neurologic examinations. One cat was euthanized 216 days after treatment initiation following relapses after primary and secondary treatment. In 1 case, resolution of disease was defined based on normalization of MRI and CSF findings and resolution of cranial and caudal segment disease with ocular imaging. Treatment with GS‐441524 shows clinical efficacy and may result in clearance and long‐term resolution of neurological FIP. Dosages required for CNS disease may be higher than those used for nonneurological FIP.

Published
2020

40. Clinicopathological characteristics of histiocytic sarcoma affecting the central nervous system in dogs

Author

Kevin D. Woolard, Robert Higgins, William Vernau, John H. Rossmeisl, Michelle A. Giuffrida, Peter J Dickinson, Beverly K. Sturges, Kurt L. Zimmerman, Karen M. Vernau, Chelsea M. Crowe, and Izumi Toyoda

Subjects
Male, Pathology, medicine.medical_specialty, Palliative treatment, Lymphocyte, Central nervous system, canine, Inflammation, Standard Article, Histiocytic sarcoma, California, cerebrospinal fluid, Central Nervous System Neoplasms, Cerebrospinal fluid, Rare Diseases, Dogs, medicine, Animals, Disseminated disease, Dog Diseases, Veterinary Sciences, Cancer, Retrospective Studies, lcsh:Veterinary medicine, General Veterinary, business.industry, Neurosciences, Records, medicine.disease, central nervous system, Survival Analysis, Standard Articles, Brain Disorders, neoplasia, medicine.anatomical_structure, Neurology, lcsh:SF600-1100, Female, Sarcoma, SMALL ANIMAL, Histiocytic Sarcoma, medicine.symptom, business, Meningioma
Abstract

Author(s): Toyoda, Izumi; Vernau, William; Sturges, Beverly K; Vernau, Karen M; Rossmeisl, John; Zimmerman, Kurt; Crowe, Chelsea M; Woolard, Kevin; Giuffrida, Michelle; Higgins, Robert J; Dickinson, Peter J | Abstract: BackgroundHistiocytic sarcoma affecting the central nervous system (CNS HS) in dogs may present as primary or disseminated disease, often characterized by inflammation. Prognosis is poor, and imaging differentiation from other CNS tumors can be problematic.ObjectiveTo characterize the clinicopathological inflammatory features, breed predisposition, and survival in dogs with CNS HS.AnimalsOne hundred two dogs with HS, 62 dogs with meningioma.MethodsRetrospective case series. Records were reviewed for results of cerebrospinal fluid (CSF) analysis, CBC, treatment, and outcome data.ResultsPredisposition for CNS HS was seen in Bernese Mountain Dogs, Golden Retrievers, Rottweilers, Corgis, and Shetland Sheepdogs (P ≤ .001). Corgis and Shetland Sheepdogs had predominantly primary tumors; Rottweilers had exclusively disseminated tumors. Marked CSF inflammation was characteristic of primary rather than disseminated HS, and neoplastic cells were detected in CSF of 52% of affected dogs. Increased neutrophil to lymphocyte ratios were seen in all groups relative to controls (P l.008) but not among tumor subtypes. Definitive versus palliative treatment resulted in improved survival times (P l .001), but overall prognosis was poor.Conclusions and clinical importanceClinicopathological differences between primary and disseminated HS suggest that tumor biological behavior and origin may be different. Corgis and Shetland Sheepdogs are predisposed to primary CNS HS, characterized by inflammatory CSF. High total nucleated cell count and the presence of neoplastic cells support the use of CSF analysis as a valuable diagnostic test. Prognosis for CNS HS is poor, but further evaluation of inflammatory mechanisms may provide novel therapeutic opportunities.

Published
2020

41. A Missense Mutation in the Vacuolar Protein Sorting 11 (VPS11) Gene Is Associated with Neuroaxonal Dystrophy in Rottweiler Dogs

Author

James R. Mickelson, Cord Drögemüller, Anna Letko, C. Titus Brown, Danika L. Bannasch, Tamer A. Mansour, Peter J Dickinson, Carrie J. Finno, Katherine L. Lucot, and Katherine M. Minor

Subjects
0301 basic medicine, Vacuolar protein sorting, Candidate gene, Haplotype, Biology, Molecular biology, 03 medical and health sciences, 030104 developmental biology, Genetics, Missense mutation, NAD+ kinase, Allele, Molecular Biology, Allele frequency, Genetics (clinical), Rottweiler
Abstract

Canine neuroaxonal dystrophy (NAD) is a recessive, degenerative neurological disease of young adult Rottweiler dogs (Canis lupus familiaris) characterized pathologically by axonal spheroids primarily targeting sensory axon terminals. A genome-wide association study of seven Rottweilers affected with NAD and 42 controls revealed a significantly associated region on canine chromosome 5 (CFA 5). Homozygosity within the associated region narrowed the critical interval to a 4.46 Mb haplotype (CFA5:11.28 Mb – 15.75 Mb; CanFam3.1) that associated with the phenotype. Whole-genome sequencing of two histopathologically confirmed canine NAD cases and 98 dogs unaffected with NAD revealed a homozygous missense mutation within the Vacuolar Protein Sorting 11 (VPS11) gene (g.14777774T > C; p.H835R) that was associated with the phenotype. These findings present the opportunity for an antemortem test for confirming NAD in Rottweilers where the allele frequency was estimated at 2.3%. VPS11 mutations have been associated with a degenerative leukoencephalopathy in humans, and VSP11 should additionally be included as a candidate gene for unexplained cases of human NAD.

Published
2018
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42. PO-1204 Adjuvant immunotherapy after concurrent chemoradiotherapy for stage 3 NSCLC, outcomes from a large cancer centre

Author

P. Jain, K. Clarke, Peter J Dickinson, Kevin Franks, F. Sun, M. Teo, and H. Mason

Subjects
Oncology, medicine.medical_specialty, business.industry, medicine.medical_treatment, Hematology, Immunotherapy, Concurrent chemoradiotherapy, Internal medicine, Cancer centre, medicine, Radiology, Nuclear Medicine and imaging, Stage (cooking), business, Adjuvant
Published
2021
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43. The Effects of FGF4 Retrogenes on Canine Morphology

Author

Danika Bannasch, Kevin Batcher, Fabienne Leuthard, Michael Bannasch, Petra Hug, Denis J. Marcellin-Little, Peter J. Dickinson, Michaela Drögemüller, Cord Drögemüller, and Tosso Leeb

Subjects
conformation, dwarfism, 630 Agriculture, 610 Medicine & health, chondrodystrophy, chondrodysplasia, height, body size, Dogs, Genetics, 590 Animals (Zoology), 570 Life sciences, biology, Animals, Intervertebral Disc Displacement, Genetics (clinical)
Abstract

Two FGF4 retrogenes (FGF4L1 on chromosome 18 and FGF4L2 on chromosome 12) have been identified to cause dwarfism across many dog breeds. Some breeds are nearly homozygous for both retrogenes (e.g., Dachshunds) and others are homozygous for just one (e.g., Beagles and Scottish Terriers). Since most breeds do not segregate both of these retrogenes, it is challenging to evaluate their individual effects on long bone length and body size. We identified two dog breeds selected for hunting ability, the Alpine Dachsbracke and the Schweizer Niederlaufhund, that segregate both of these retrogenes. Using individual measurements of height at the shoulder, back length, head width, thorax depth and width, and thoracic limb measurements, we evaluated the combined effects of FGF4 retrogenes within these breeds. We applied multivariable linear regression analysis to determine the effects of retrogene copy numbers on the measurements. Copy numbers of both retrogenes had significant effects reducing height at the shoulders and antebrachial length, with FGF4L1 having a much greater effect than FGF4L2. FGF4L1 alone influenced the degree of carpal valgus and FGF4L2 alone increased head width. Neither retrogene had an effect on thorax width or depth. Selectively breeding dogs with FGF4L1 and without FGF4L2 would likely lead to a reduction in the FGF4L2-related risk of intervertebral disc herniation while maintaining the reduction in leg length resulting from FGF4L1.

Published
2022
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44. Expression and targeting of transcription factor ATF5 in dog gliomas

Author

Daniel York, Peter J Dickinson, James M. Angelastro, C. D. Sproul, and N. Chikere

Subjects
0301 basic medicine, General Veterinary, Activating transcription factor, Biology, medicine.disease, Blot, 03 medical and health sciences, 030104 developmental biology, Canine Glioma, Cell culture, Glioma, medicine, Cancer research, Viability assay, Stem cell, Transcription factor
Abstract

Background Activating transcription factor 5 (ATF5) is a transcription factor that is highly expressed in undifferentiated neural progenitor/stem cells as well as a variety of human cancers including gliomas. Aims In this study, we examined the expression and localization of ATF5 protein in canine gliomas, and targeting of ATF5 function in canine glioma cell lines. Materials and Methods Paraffin-embedded canine brain glioma tissue sections and western blots of tumours and glioma cells were immunoassayed with anti-ATF5 antibody. Viability of glioma cells was tested with a synthetic cell-penetrating ATF5 peptide (CP-d/n ATF5) ATF5 antagonist. Results ATF5 protein expression was in the nucleus and cytoplasm and was present in normal adult brain and tumour samples, with significantly higher expression in tumours as shown by western immunoblotting. CP-d/n ATF5 was found to decrease cell viability in canine glioma cell lines in vitro in a dose-dependent manner. Conclusion Similarities in expression of ATF5 in rodent, dog and human tumours, and cross species efficacy of the CP-d/n ATF5 peptide support the development of this ATF5-targeting approach as a novel and translational therapy in dog gliomas.

Published
2017
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45. Current Understanding of the Genetics of Intervertebral Disc Degeneration

Author

Peter J Dickinson and Danika L. Bannasch

Subjects
Chondrodystrophy, 040301 veterinary sciences, Review, Intervertebral disc herniation, Disease, chondrodystrophy, Bioinformatics, 0403 veterinary science, 03 medical and health sciences, Genetics, 2.1 Biological and endogenous factors, Medicine, Veterinary Sciences, Aetiology, 030304 developmental biology, 0303 health sciences, retrogene, lcsh:Veterinary medicine, fibroblast growth factor 4, General Veterinary, intervertebral disc degeneration, business.industry, Multifactorial disease, Intervertebral disc, 04 agricultural and veterinary sciences, heritable, medicine.disease, Good Health and Well Being, medicine.anatomical_structure, Intervertebral disc calcification, lcsh:SF600-1100, Veterinary Science, business
Abstract

Premature degeneration of the intervertebral disc and its association with specific chondrodystrophic dog breeds has been recognized for over a century. Several lines of evidence including disease breed predisposition, studies suggesting heritability of premature intervertebral disc degeneration (IVDD) and association of a dog chromosome 12 (CFA 12) locus with intervertebral disc calcification have strongly supported a genetic component in IVDD in dogs. Recent studies documenting association of IVDD with an overexpressing FGF4 retrogene on CFA 12 have opened up new areas of investigation to further define the pathophysiology of premature IVDD. While preliminary data from studies investigating FGF4 retrogenes in IVDD implicate FGF4 overexpression as a major disease factor, they have also highlighted knowledge gaps in our understanding of intervertebral disc herniation which is a complex and multifactorial disease process.

Published
2020

46. Comparative Molecular Life History of Spontaneous Canine and Human Gliomas

Author

C. Elizabeth Boudreau, Hoon Kim, Frederick S. Varn, Kevin D. Woolard, Emmanuel Martinez-Ledesma, Kevin J. Anderson, Roel G.W. Verhaak, Kevin C. Johnson, Xiaoyang Ling, Amy B. Heimberger, John H. Rossmeisl, Chew Yee Ngan, Ching C. Lau, Andrew D. Miller, C. Ryan Miller, Emre Kocakavuk, Jonathan M. Levine, Rebecca A. Packer, Brian F. Porter, Cynthia Kassab, James P. Long, Peter J Dickinson, Christina Mazcko, Floris P. Barthel, Daniel R. Rissi, Amanda R. Taylor, Margaret Chapman, Jennifer W. Koehler, Samirkumar B. Amin, Amy K. LeBlanc, and Mary Barter

Subjects
life history, 0301 basic medicine, Cancer Research, Somatic cell, Medizin, comparative genomics, Receptor tyrosine kinase, Transcriptome, computational biology, 0302 clinical medicine, adult glioma, Exome, Cancer, biology, Brain Neoplasms, Glioma, Isocitrate Dehydrogenase, Oncology, Canine Glioma, 030220 oncology & carcinogenesis, pediatric glioma, mutagenesis, IDH1, comparative oncology, Oncology and Carcinogenesis, canine glioma, Article, 03 medical and health sciences, Rare Diseases, Dogs, Genetics, medicine, Animals, Humans, Oncology & Carcinogenesis, neoplasms, Comparative genomics, Human Genome, Neurosciences, DNA Methylation, medicine.disease, Brain Disorders, nervous system diseases, Brain Cancer, 030104 developmental biology, Mutation, biology.protein, Cancer research, Tumor Suppressor Protein p53
Abstract

Sporadic gliomas in companion dogs provide a window on the interaction between tumorigenic mechanisms and host environment. We compared the molecular profiles of canine gliomas with those of human pediatric and adult gliomas to characterize evolutionarily conserved mammalian mutational processes in gliomagenesis. Employing whole-genome, exome, transcriptome, and methylation sequencing of 83 canine gliomas, we found alterations shared between canine and human gliomas such as the receptor tyrosine kinases, TP53 and cell-cycle pathways, and IDH1 R132. Canine gliomas showed high similarity with human pediatric gliomas per robust aneuploidy, mutational rates, relative timing of mutations, and DNA-methylation patterns. Our cross-species comparative genomic analysis provides unique insights into glioma etiology and the chronology of glioma-causing somatic alterations.

Published
2020

47. Multiple FGF4 Retrocopies Recently Derived within Canids

Author

Danika L. Bannasch, Peter J Dickinson, Kevin Batcher, Sheida Hadji Rasouliha, Tosso Leeb, Kimberly Maciejczyk, Kristin E. Brzeski, Anna Letko, and Cord Drögemüller

Subjects
0301 basic medicine, Canis lupus familiaris, retrocopy, FGF4, pseudogene, Retrotransposon, Intervertebral Disc Degeneration, 0403 veterinary science, Gene duplication, Dog Diseases, 610 Medicine & health, Genetics (clinical), media_common, retrogene, biology, 630 Agriculture, 04 agricultural and veterinary sciences, duplication, 590 Animals (Zoology), Canis rufus, Intervertebral Disc Displacement, Biotechnology, lcsh:QH426-470, Retroelements, 040301 veterinary sciences, Evolution, Pseudogene, Population, Fibroblast Growth Factor 4, Article, Evolution, Molecular, 03 medical and health sciences, Dogs, retrotransposition, Genetics, media_common.cataloged_instance, Animals, Domestication, Gene, Canis lupusfamiliaris, Whole Genome Sequencing, Haplotype, Molecular, biology.organism_classification, lcsh:Genetics, 030104 developmental biology, Genetics, Population, Haplotypes, Evolutionary biology, 570 Life sciences
Abstract

Two transcribed retrocopies of the fibroblast growth factor 4 (FGF4) gene have previously been described in the domestic dog. An FGF4 retrocopy on chr18 is associated with disproportionate dwarfism, while an FGF4 retrocopy on chr12 is associated with both disproportionate dwarfism and intervertebral disc disease (IVDD). In this study, whole-genome sequencing data were queried to identify other FGF4 retrocopies that could be contributing to phenotypic diversity in canids. Additionally, dogs with surgically confirmed IVDD were assayed for novel FGF4 retrocopies. Five additional and distinct FGF4 retrocopies were identified in canids including a copy unique to red wolves (Canis rufus). The FGF4 retrocopies identified in domestic dogs were identical to domestic dog FGF4 haplotypes, which are distinct from modern wolf FGF4 haplotypes, indicating that these retrotransposition events likely occurred after domestication. The identification of multiple, full length FGF4 retrocopies with open reading frames in canids indicates that gene retrotransposition events occur much more frequently than previously thought and provide a mechanism for continued genetic and phenotypic diversity in canids.

Published
2020
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48. Pathologic Features of the Intervertebral Disc in Young Nova Scotia Duck Tolling Retrievers Confirms Chondrodystrophy Degenerative Phenotype Associated With Genotype

Author

Denis J. Marcellin-Little, Kevin Batcher, Brian G Murphy, Danika L. Bannasch, Peter J Dickinson, and Stephen Raverty

Subjects
Chondrodystrophy, Pathology, medicine.medical_specialty, Genotype, 040301 veterinary sciences, Fibroblast Growth Factor 4, canine, Intervertebral Disc Degeneration, chondrodystrophy, Biology, Short stature, 0403 veterinary science, 03 medical and health sciences, Dogs, chondrodysplasia, genetic diseases, medicine, Cartilaginous Tissue, Genetics, Animals, 2.1 Biological and endogenous factors, Dog Diseases, Veterinary Sciences, Aetiology, Intervertebral Disc, Chromosome 12, 030304 developmental biology, 0303 health sciences, General Veterinary, Pain Research, Intervertebral disc, 04 agricultural and veterinary sciences, Nova Scotia Duck-Tolling Retriever, medicine.disease, Phenotype, Fisheries Sciences, FGF4 retrogene, medicine.anatomical_structure, intervertebral disc, medicine.symptom, Chronic Pain, Cartilage Diseases
Abstract

Chondrodystrophy results in predictable and progressive biochemical and structural changes to the intervertebral disc, resulting in early onset degeneration and dystrophic mineralization of the disc. Accelerated degeneration and mineralization of the intervertebral disc are common in multiple dog breeds and can result in compromised function, herniation, pain, and a variety of neurological sequelae. A mutation responsible for chondrodystrophy in dogs has been identified as an aberrant fibroblast growth factor 4 ( FGF4) retrogene insertion on chromosome 12 (CFA12) and is associated with short stature of the Nova Scotia Duck Tolling Retriever. Segregation of the CFA12 FGF4 retrogene in this dog breed provides an opportunity to examine the effect of retrogene presence on radiographic and histologic appearance of chondrodystrophic disc degeneration within a single breed. Here we found that in the intervertebral discs isolated from 2 dogs with the CFA12 FGF4 genotype, the nucleus pulposus was largely replaced by cartilaginous tissue, and physaliferous notochordal cells were rarely if ever identified. These findings are in contrast to the normal histologic findings in 2 breed-matched dogs lacking the mutation. The findings are consistent with premature chondroid degeneration of the intervertebral disc and suggest that the presence of the CFA12 FGF4 retrogene is sufficient to cause the chondrodystrophic phenotype.

Published
2019

49. Comparative molecular life history of spontaneous canine and human gliomas

Author

C. Ryan Miller, Amanda R. Taylor, Amy B. Heimberger, Rebecca A. Packer, John H. Rossmeisl, Hoon Kim, Floris P. Barthel, Emmanuel Martinez-Ledesma, Roel G.W. Verhaak, Andrew D. Miller, Frederick S. Varn, Kevin J. Anderson, C. Elizabeth Boudreau, Christina Mazcko, Peter J Dickinson, Jonathan M. Levine, Samirkumar B. Amin, Chew Yee Ngan, Emre Kocakavuk, Xiaoyang Ling, Amy K. LeBlanc, Mary Barter, Cynthia Kassab, Kevin C. Johnson, Jennifer W. Koehler, Margaret Chapman, Brian F. Porter, and Daniel R. Rissi

Subjects
Tumor microenvironment, IDH1, Somatic cell, Biology, Cell cycle, medicine.disease, nervous system diseases, Canine Glioma, Glioma, DNA methylation, Cancer research, medicine, Exome, neoplasms
Abstract

SummarySporadic gliomas in companion dogs provide a window on the interaction between tumorigenic mechanisms and host environment. We compared the molecular profiles of canine gliomas with those of human pediatric and adult gliomas to characterize evolutionarily conserved mammalian mutational processes in gliomagenesis. Employing whole genome-, exome-, transcriptome-and methylation-sequencing of 81 canine gliomas, we found alterations shared between canine and human gliomas such as the receptor tyrosine kinases, p53 and cell cycle pathways, and IDH1 R132. Canine gliomas showed high similarity with human pediatric gliomas per robust aneuploidy, mutational rates, relative timing of mutations, and DNA methylation patterns. Our cross-species comparative genomic analysis provides unique insights into glioma etiology and the chronology of glioma-causing somatic alterations.SignificanceDiffuse gliomas are the most common malignant brain tumors, with high-grade tumors carrying a dismal prognosis. Preclinical models have proven themselves as poor predictors of clinical efficacy. Spontaneous glioma in dogs provides an attractive alternative model, because of their comparable tumor microenvironment and tumor life history. We determined the similarities and differences between human and canine gliomas through genomic profiling, and leveraged our datasets to identify conserved somatic drivers, mutational processes and temporal ordering of somatic glioma events across species. We show that canine gliomas resemble human gliomas at (epi-)genetic levels and are more reminiscent of pediatric than adult disease, thus rationalizing sporadic canine glioma as a preclinical model tailored to measuring treatment efficacies in patients with canine or human glioma.

Published
2019
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50. Intracranial pressure monitoring in normal dogs using subdural and intraparenchymal miniature strain-gauge transducers

Author

Irina Udaltsova, Linda D Tripp, Richard A Lecouteur, Beverly K. Sturges, and Peter J Dickinson

Subjects
Intracranial Pressure, Standard Article, 030204 cardiovascular system & hematology, 0403 veterinary science, 0302 clinical medicine, Catheters, Indwelling, microsensor, Transducers, Pressure, Medicine, Prospective Studies, Intracranial pressure, integumentary system, musculoskeletal, neural, and ocular physiology, 04 agricultural and veterinary sciences, Equipment Design, humanities, Standard Articles, Catheter, Transducer, Neurology, Indwelling, Cerebrovascular Circulation, intracranial hypertension, Intracranial pressure monitoring, Female, Codman, Mean arterial pressure, Catheters, Monitoring, 040301 veterinary sciences, Transducers, canine, 03 medical and health sciences, Dogs, Pressure, Animals, Veterinary Sciences, Cerebral perfusion pressure, Physiologic, Strain gauge, Monitoring, Physiologic, Miniaturization, General Veterinary, business.industry, Neurosciences, Reproducibility of Results, Brain Disorders, nervous system diseases, Blood pressure, SMALL ANIMAL, Nuclear medicine, business, Head
Abstract

Author(s): Sturges, Beverly K; Dickinson, Peter J; Tripp, Linda D; Udaltsova, Irina; LeCouteur, Richard A | Abstract: BackgroundMonitoring of intracranial pressure (ICP) is a critical component in the management of intracranial hypertension. Safety, efficacy, and optimal location of microsensor devices have not been defined in dogs.Hypothesis/objectiveAssessment of ICP using a microsensor transducer is feasible in anesthetized and conscious animals and is independent of transducer location. Intraparenchymal transducer placement is associated with more adverse effects.AnimalsSeven adult, bred-for-research dogs.MethodsIn a prospective investigational study, microsensor ICP transducers were inserted into subdural and intraparenchymal locations at defined rostral or caudal locations within the rostrotentorial compartment under general anesthesia. Mean arterial pressure and ICP were measured continuously during physiological maneuvers, and for 20 hours after anesthesia.ResultsBaseline mean ± SD values for ICP and cerebral perfusion pressure were 7.2 ± 2.3 and 78.9 ± 7.6 mm Hg, respectively. Catheter position did not have a significant effect on ICP measurements. There was significant variation from baseline ICP accompanying physiological maneuvers (P l .001) and with normal activities, especially with changes in head position (P l .001). Pathological sequelae were more evident after intraparenchymal versus subdural placement.Conclusions and clinical importanceUse of a microsensor ICP transducer was technically straightforward and provided ICP measurements within previously reported reference ranges. Results support the use of an accessible dorsal location and subdural positioning. Transient fluctuations in ICP are normal events in conscious dogs and large variations associated with head position should be accounted for when evaluating animals with intracranial hypertension.

Published
2019

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