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1. Immunomodulation therapy for feline leukemia virus infection. (Abstracts: recently published abstracts)

Author

McCaw, DL, Boon, GD, and Jergens, AE

Subjects
Interferon alpha -- Dosage and administration, Feline leukemia -- Care and treatment, Health, Care and treatment, Dosage and administration
Abstract

Clinically ill feline leukemia virus (FeLV)-infected cats, treated with Staphylococcus protein A (SPA) or oral interferon alpha (IFN), or both, were compared with cats treated with saline (SAL). Nine cats [...]

Published
2001

3. Plasma Granulocyte Colony-Stimulating Factor Concentrations in Neutropenic, Parvoviral Enteritis–Infected Puppies

Author

Clinton D. Lothrop, Colette C. Wagner-Mann, Leah A. Cohn, Boon Gd, Dudley L. McCaw, and J M Rewerts

Subjects
General Veterinary, biology, business.industry, Parvovirus, Canine parvovirus, Inflammation, Granulocyte, Neutropenia, biology.organism_classification, medicine.disease, Enteritis, Granulocyte colony-stimulating factor, medicine.anatomical_structure, Immunology, Medicine, Bone marrow, medicine.symptom, business
Abstract

We evaluated the temporal relationship between neutrophil numbers and plasma granulocyte colony-stimulating factor (G-CSF) concentrations in dogs infected with canine parvovirus, a common infectious cause of neutropenia. G-CSF is produced in response to neutropenia, infection, or inflammation, and results in the production and release of neutrophils from the bone marrow. Adequate numbers of functional neutrophils are necessary for protection from infection, and the timely production of G-CSF is a crucial response to certain diseases. The relationship between peripheral neutrophil numbers and plasma G-CSF concentrations during the course of an infectious disease characterized by neutropenia has not been described previously in dogs. Eight mixed-breed puppies were given an oronasal challenge with canine parvovirus, and peripheral neutrophil numbers as well as plasma G-CSF concentrations were measured daily. G-CSF was not detectable in plasma of any dog before the onset of neutropenia, but G-CSF became detectable just after the onset of neutropenia in the 7 dogs that developed clinical illness. Neutropenia persisted or worsened for at least 2 days after plasma G-CSF became detectable in all 7 dogs. Neutrophil nadir, the highest plasma G-CSF concentrations, and the most severe clinical illness occurred concurrently in most dogs. Although 1 dog died while still neutropenic, plasma G-CSF concentrations declined before resolution of neutropenia in the other 6 dogs, and were again below the limits of detection in 5 of the 6 dogs at the time of resolution.

Published
1999
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5. A comparison of the cytologic and histologic features of meningiomas in four dogs.

Author

Zimmerman KL, Bender HS, Boon GD, Prater MR, Thorn CE, Prater D, Robertson JL, Saunders GK, Sponenberg DP, Inzana KD, Lanz OI, and Wright E

Abstract

The cytologic and histologic features of 2 intracranial and 2 spinal (extramedullary cervical) canine meningiomas were compared. Cerebrospinal fluid analysis in 2 cases revealed mild, mixed cell pleocytosis, primarily composed of small lymphocytes and monocytoid cells, with a moderate increase in total protein concentration. Cytologic features suggestive of meningioma included cells with both epithelial and mesenchymal characteristics and a tendency towards cell clustering. Tumor location also was useful in making a diagnosis. The 4 meningiomas differed histologically from one another, and included angioblastic, psammomatous, meningotheliomatous, and microcystic anaplastic types, which conformed to a classification scheme for human meningiomas. The classification scheme could not be applied to cytologic specimens.

Published
2000
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6. Mechanism-based diagnostic reasoning: thoughts on teaching introductory clinical pathology.

Author

Bender HS, Lockee BB, Danielson JA, Mills EM, Boon GD, Burton JK, Vermeer PJ, Zimmerman KL, and Hilmer KM

Abstract

Teaching introductory clinical pathology to veterinary students is a challenging endeavor that requires a shift in learning strategies from rote memorization to diagnostic reasoning. Educational research has identified discrete cognitive stages required to achieve the automated, unconscious thinking process used by experts. Building on this knowledge, we developed a case-based approach to clinical pathology instruction that actively engages students in the learning process and links performance with positive reward. Simulated cases provide context and create a structure, or "schema", which enhances the learning process by enabling students to synthesize facts and link them with their causal mechanism to reach a defensible diagnostic conclusion. Web-based tools, including the "Problem List Generator" and tutorials, have been developed to facilitate this process. Through the collaborative Biomedical Informatics Research Group, we are working to further develop and evaluate Web-based instructional tools and new educational methods, to clarify the diagnostic reasoning processes used by experienced clinical pathologists, and, ultimately, to better educate our future students to be effective diagnosticians.

Published
2000
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7. Plasma granulocyte colony-stimulating factor concentrations in neutropenic, parvoviral enteritis-infected puppies.

Author

Cohn LA, Rewerts JM, McCaw D, Boon GD, Wagner-Mann C, and Lothrop CD Jr

Subjects
Animals, Disease Progression, Dog Diseases pathology, Dogs, Enteritis immunology, Granulocyte Colony-Stimulating Factor pharmacokinetics, Neutropenia physiopathology, Parvoviridae Infections immunology, Dog Diseases immunology, Enteritis veterinary, Granulocyte Colony-Stimulating Factor blood, Neutropenia veterinary, Parvoviridae Infections veterinary, Parvovirus, Canine
Abstract

We evaluated the temporal relationship between neutrophil numbers and plasma granulocyte colony-stimulating factor (G-CSF) concentrations in dogs infected with canine parvovirus, a common infectious cause of neutropenia. G-CSF is produced in response to neutropenia, infection, or inflammation, and results in the production and release of neutrophils from the bone marrow. Adequate numbers of functional neutrophils are necessary for protection from infection, and the timely production of G-CSF is a crucial response to certain diseases. The relationship between peripheral neutrophil numbers and plasma G-CSF concentrations during the course of an infectious disease characterized by neutropenia has not been described previously in dogs. Eight mixed-breed puppies were given an oronasal challenge with canine parvovirus, and peripheral neutrophil numbers as well as plasma G-CSF concentrations were measured daily. G-CSF was not detectable in plasma of any dog before the onset of neutropenia, but G-CSF became detectable just after the onset of neutropenia in the 7 dogs that developed clinical illness. Neutropenia persisted or worsened for at least 2 days after plasma G-CSF became detectable in all 7 dogs. Neutrophil nadir, the highest plasma G-CSF concentrations, and the most severe clinical illness occurred concurrently in most dogs. Although 1 dog died while still neutropenic, plasma G-CSF concentrations declined before resolution of neutropenia in the other 6 dogs, and were again below the limits of detection in 5 of the 6 dogs at the time of resolution.

Published
1999
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8. Ionized and total magnesium concentrations in blood from dogs with naturally acquired parvoviral enteritis.

Author

Mann FA, Boon GD, Wagner-Mann CC, Ruben DS, and Harrington DP

Subjects
Age Factors, Animals, Cohort Studies, Dog Diseases therapy, Dogs, Enteritis blood, Hydrogen-Ion Concentration, Immunization, Passive, Immunoglobulins, Parvoviridae Infections blood, Parvoviridae Infections therapy, Prognosis, Prospective Studies, Reference Values, Dog Diseases blood, Enteritis veterinary, Magnesium blood, Parvoviridae Infections veterinary, Parvovirus, Canine
Abstract

Objective: To determine whether pretreatment total and ionized blood magnesium concentrations were associated with outcome for dogs with parvoviral enteritis and whether ionized magnesium concentration was related to total magnesium concentration or other laboratory values., Design: Prospective cohort study., Animals: 61 healthy dogs and 72 dogs with parvoviral enteritis., Procedure: Total, ionized, and pH-normalized ionized magnesium concentrations, ionized and pH-normalized ionized calcium concentrations, pH, sodium and potassium concentrations, and Hct were measured prior to treatment. chi 2 Analyses were used to test for associations between outcome and age and between outcome and treatment with antiendotoxin antibody. Pearson's correlation coefficients were calculated to determine whether ionized magnesium concentration was linearly associated with other laboratory values., Results: Total and ionized magnesium concentrations were not significantly different between healthy dogs and dogs with parvoviral enteritis or between dogs surviving and those not surviving parvoviral enteritis. The only laboratory value strongly correlated with ionized magnesium concentration was pH-normalized ionized magnesium concentration. Of the factors tested, none were significantly associated with outcome, except that dogs 16 weeks old or less treated with antiendotoxin antibody were significantly more likely to die than were dogs 16 weeks old or less that were not treated with antiendotoxin antibody., Clinical Implications: Total and ionized blood magnesium concentrations cannot be used to consistently predict outcome for dogs with parvoviral enteritis. Antiendotoxin antibody should be used with caution in dogs 16 weeks old or less.

Published
1998

9. Heritability and biochemistry of gangliosidosis in emus (Dromaius novaehollandiae).

Author

Bermudez AJ, Freischütz B, Yu RK, Nonneman D, Johnson GS, Boon GD, Stogsdill PL, and Ledoux DR

Subjects
Animals, Birds, Blood Coagulation physiology, Brain pathology, Brain ultrastructure, Brain Chemistry, Breeding, Cholesterol blood, DNA analysis, DNA chemistry, DNA genetics, DNA Fingerprinting veterinary, Female, Gangliosides analysis, Gangliosidoses blood, Gangliosidoses genetics, Genes, Lethal genetics, Kidney Tubules pathology, Liver pathology, Liver ultrastructure, Macrophages pathology, Male, Microscopy, Electron methods, Microscopy, Electron veterinary, Muscle, Skeletal pathology, Polymorphism, Restriction Fragment Length, Poultry Diseases pathology, Uric Acid blood, Gangliosidoses veterinary, Poultry Diseases blood, Poultry Diseases genetics
Abstract

The progeny of two emu breeder pairs, which had a history of producing offspring with gangliosidosis, were monitored for 15 mo. DNA fingerprinting revealed that individuals in each breeder pair were not related to each other. One breeder pair had 13 progeny that reached or exceeded the age of 1 mo, and six of these progeny developed gangliosidosis. The mean age at which these affected emus were euthanatized, with distinct neurologic disease, or died was 5.7 mo. The second emu pair had 13 progeny, seven of which developed gangliosidosis, with a mean age of euthanasia/death of 4.6 mo. Affected emus died or were euthanatized from 2 to 8 mo of age. The primary clinical sign in the affected emus was mild to severe ataxia. Severe hemorrhage into the body cavity or the muscles of the thigh was noted in 8 of 13 of the affected emus. Brain ganglioside levels were evaluated in six of the affected emus and six controls. Significant increases (P < 0.05) in gangliosides GM1 and GM3 were noted, with 2.3- and 4.9-fold increases in these two gangliosides, respectively, in affected emus. Furthermore, the diseased emu brains contained ganglioside GM2, whereas this monosialoganglioside was undetectable in the brains of normal controls. Total mean brain ganglioside sialic acid in affected emus was increased 3.3-fold in comparison with controls. Serum chemistries revealed elevated cholesterol and decreased uric acid levels in affected emus. Gangliosidosis in emus is an inherited disease process that, in the current study, caused 50% mortality in the progeny of two emu breeder pairs. The elimination of this lethal gene from emu breeder stock is essential for the long-term economic viability of the United States emu industry.

Published
1997

10. Delivery of laboratory data with World Wide Web technology.

Author

Hahn AW, Leon MA, Klein-Leon S, Allen GK, Boon GD, Patrick TB, and Klimczak JC

Subjects
Animals, Veterinary Medicine, Computer Communication Networks, Hospitals, Animal, Pathology, Veterinary, Records
Abstract

We have developed an experimental World Wide Web (WWW) based system to deliver laboratory results to clinicians in our Veterinary Medical Teaching Hospital. Laboratory results are generated by the clinical pathology section of our Veterinary Medical Diagnostic Laboratory and stored in a legacy information system. This system does not interface directly to the hospital information system, and it cannot be accessed directly by clinicians. Our "meta" system first parses routine print reports and then instantiates the data into a modern, open-architecture relational database using a data model constructed with currently accepted international standards for data representation and communication. The system does not affect either of the existing legacy systems. Location-independent delivery of patient data is via a secure WWW based system which maximizes usability and allows "value-added" graphic representations. The data can be viewed with any web browser. Future extensibility and intra- and inter-institutional compatibility served as key design criteria. The system is in the process of being evaluated using accepted methods of assessment of information technologies.

Published
1997

11. Methodologic considerations for the use of canine in vivo aged biotinylated erythrocytes to study RBC senescence.

Author

Christian JA, Rebar AH, Boon GD, and Low PS

Subjects
Acetamides toxicity, Animals, Carbon Radioisotopes, Chemical and Drug Induced Liver Injury, Dimethyl Sulfoxide, Dogs, Female, Flow Cytometry, Male, Models, Biological, Scintillation Counting, Time Factors, Biotin blood, Erythrocyte Aging
Abstract

Biotinylation of erythrocytes has been developed in rabbits as a tool to retrieve labeled cells following various periods in circulation. This retrieval capability allows biochemical studies to be conducted on red blood cells (RBC) that have aged for desired times in vivo. However, because erythrocyte life span is much shorter in rabbits than in humans, and because cell removal is measurably age-independent in rabbits, we have sought to validate the same protocol in dogs, whose cell life span and age-dependent removal characteristics are similar to humans'. Canine RBC were biotinylated in vivo by infusion of N-hydroxysuccinimidyl biotin dissolved in dimethylacetamide or dimethylsulfoxide. Cell life spans were evaluated using 14C-cyanate labeling followed by scintillation counting or avidin-FITC labeling followed by flow cytometry. Both methods gave identical results. The life span of the biotin-conjugated cells was found to be normal (approximately 110 days), and the stability of the biotin ligand was adequate for efficient retrieval of cells using avidin-coated magnetic beads (magnetic cell sorting [MACS]). From each isolation, approximately 20 microL of packed biotinylated cells of approximately 90% purity (i.e., 10% contamination by unlabeled cells) could be harvested. On average, approximately 60% of the biotinylated cells in any sample could be retrieved. Either multiple isolations or use of larger collection columns will facilitate collection of cell numbers sufficient for biochemical tests. After incorporating several modifications in the previous biotinylation protocol that were required for adaptation to the dog, the methodology can be used to study red cell senescence in an animal that has several pertinent similarities to humans.

Published
1996

12. Hypergammaglobulinemia in a dog.

Author

Michels GM, Boon GD, Jones BD, and Puget B

Subjects
Animals, Antibodies, Bacterial blood, Dog Diseases microbiology, Dogs, Ehrlichia immunology, Ehrlichiosis diagnosis, Hypergammaglobulinemia microbiology, Male, Dog Diseases diagnosis, Ehrlichiosis veterinary, Hypergammaglobulinemia veterinary
Published
1995

13. Ultracentrifugal and electrophoretic characteristics of the plasma lipoproteins of miniature schnauzer dogs with idiopathic hyperlipoproteinemia.

Author

Whitney MS, Boon GD, Rebar AH, Story JA, and Bottoms GD

Subjects
Animals, Blood Protein Electrophoresis veterinary, Cholesterol blood, Densitometry veterinary, Dogs, Electrophoresis, Agar Gel veterinary, Female, Hyperlipoproteinemias blood, Male, Phospholipids blood, Triglycerides blood, Ultracentrifugation veterinary, Dog Diseases blood, Hyperlipoproteinemias veterinary, Lipoproteins blood
Abstract

To better characterize the idiopathic hyperlipoproteinemia of Miniature Schnauzer dogs, the plasma lipoproteins of 20 Miniature Schnauzers (MS) and 11 dogs of other breeds (DOB) were evaluated by ultracentrifugation, electrophoresis, and biochemical tests. Seventeen MS were healthy; 3 had diabetes mellitus. Plasma from 6 of 17 healthy and all 3 diabetic MS was visibly lipemic. Lipemia was slight to marked in healthy lipemic MS, and marked in diabetic ones. All DOB had clear plasma; 8 were healthy and 3 had diabetes. All healthy lipemic MS and diabetic lipemic MS had hypertriglyceridemia associated with excess very low density lipoproteins. Chylomicronemia was present in 4 of 6 healthy lipemic MS and all 3 diabetic lipemic MS. Lipoproteins with ultracentrifugal and electrophoretic characteristics of normal low density lipoprotein were lacking in 4 of 6 healthy lipemic MS. The lipoprotein patterns of 4 of 11 healthy nonlipemic MS were characterized by mild hypertriglyceridemia associated with increased very low density lipoproteins and a lack of lipoproteins with characteristics of normal low density lipoproteins. Lipoprotein patterns of diabetic DOB closely resembled those of healthy DOB; those of diabetic lipemic MS resembled those of markedly lipemic healthy lipemic MS. In conclusion, the hyperlipoproteinemia of Miniature Schnauzers is characterized by increased very low density lipoproteins with or without accompanying chylomicronemia; some affected dogs may have decreased low density lipoproteins.

Published
1993
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14. An overview of hemostasis.

Author

Boon GD

Subjects
Animals, Blood Coagulation, Blood Coagulation Disorders diagnosis, Blood Platelets physiology, Humans, Hemostasis
Abstract

Hemostasis is a remarkable and a remarkably complex mechanism. It can maintain blood in a fluid state intravascularly but very quickly changes blood to a jellylike mass upon disruption of the vasculature. This review will give a synopsis of the 3 phases of hemostasis: platelet, vascular, and coagulation. Fibrinolysis and control mechanisms of hemostasis will also be covered. In addition, brief descriptions of the clinical and laboratory evaluation of patients and the diagnosis of bleeding disorders will be presented.

Published
1993
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15. Antiviral nucleoside toxicity in canine bone marrow progenitor cells and its relationship to drug permeation.

Author

Chan TC, Boon GD, Shaffer L, and Redmond R

Subjects
Animals, Biological Transport, Active, Colony-Forming Units Assay, Didanosine pharmacokinetics, Dipyridamole pharmacology, Dogs, Dose-Response Relationship, Drug, Erythrocytes cytology, Erythrocytes metabolism, Female, Granulocytes cytology, Granulocytes metabolism, Hematopoietic Stem Cells metabolism, In Vitro Techniques, Macrophages cytology, Macrophages metabolism, Zalcitabine pharmacokinetics, Zidovudine pharmacokinetics, Didanosine pharmacology, Hematopoietic Stem Cells drug effects, Zalcitabine pharmacology, Zidovudine pharmacology
Abstract

The most promising nucleoside analogs that are currently undergoing preclinical and clinical testing for anti-HIV activity belong to the dideoxynucleoside group. We have studied the toxicity of 3'-azido,3'-deoxythymidine (AZT), 2',3'-dideoxycytidine (DDC), and 2',3'-dideoxyinosine (DDI) in canine bone marrow progenitor cells in culture. AZT potently inhibited both canine CFU-GM and CFU-E with IC50 values of 2 and 8 mumol/l respectively, while DDC was relatively non-toxic to either progenitor with IC50 of > 200 mumol/l and 80 mumol/l respectively. DDI was mildly toxic to the bone marrow progenitors, with IC50 values of 62 mumol/l for CFU-GM and 70 mumol/l for CFU-E. Dipyridamole, a nucleoside transport inhibitor, did not influence the toxicity of these dideoxynucleosides in either progenitor at concentrations up to 10 mumol/l. Using uridine as the prototype endogenous nucleoside, we have demonstrated that there is a saturable "zero-trans" nucleoside transport system in canine bone marrow mononuclear cells, which is completely inhibited by 1 mumol/l dipyridamole (Ki = 0.02 mumol/l). None of the dideoxynucleosides appeared to be a substrate for this transport system, and dipyridamole did not alter their influx. Permeation of radiolabeled AZT into bone marrow mononuclear cells was slow and non-saturable, while the permeation of DDI was even slower. DDC did not permeate bone marrow cells well, with very little cell accumulation even after 2 hours of equilibration. Our toxicity data from canine bone marrow progenitor cells paralleled the clinical hematotoxicity profiles of these dideoxynucleosides in AIDS patients and suggest that the myelotoxicity of a nucleoside analog is related to its ability to permeate the progenitor cells in question. Canine bone marrow progenitor cultures may serve well as an in vitro model for drug hematotoxicity studies.

Published
1992
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16. Hemoperitoneum secondary to traumatic rupture of an adrenal tumor in a dog.

Author

Evans K, Hosgood G, Boon GD, and Kowalewich N

Subjects
Adenocarcinoma complications, Adenocarcinoma surgery, Adrenal Cortex Neoplasms complications, Adrenal Cortex Neoplasms surgery, Animals, Dog Diseases surgery, Dogs, Hemoperitoneum etiology, Hemoperitoneum surgery, Male, Rupture, Adenocarcinoma veterinary, Adrenal Cortex Neoplasms veterinary, Dog Diseases etiology, Hemoperitoneum veterinary
Abstract

Hemoperitoneum secondary to traumatic rupture of an adrenocortical adenocarcinoma was diagnosed in a 10-year-old male dog. Immediate surgical attention was required to remove the tumor and to control hemorrhage. The dog appeared to develop transient hypoadrenocorticism after surgery, but recovered with short-term exogenous corticosteroid administration. At 6 months after surgery, the dog was clinically normal.

Published
1991

17. Support of an anephric dog for 54 days with ambulatory peritoneal dialysis and a newly designed peritoneal catheter.

Author

Thornhill JA, Hartman J, Boon GD, Riviere JE, Jacobs D, and Ash SR

Subjects
Animals, Dogs, Female, Nephrectomy veterinary, Peritoneal Dialysis, Continuous Ambulatory instrumentation, Uremia therapy, Catheters, Indwelling veterinary, Dog Diseases therapy, Peritoneal Dialysis veterinary, Peritoneal Dialysis, Continuous Ambulatory veterinary, Uremia veterinary
Abstract

A bilaterally nephrectomized dog was successfully supported with peritoneal dialysis for 54 days, using a radically new design of access catheter and a human dialysis schedule designated as continuous ambulatory peritoneal dialysis. The dog remained active and alert with a stabilized blood urea nitrogen of 30 to 40 mg/dl and a serum creatinine concentration of 4 to 6.5 mg/dl. Problems encountered with the peritoneal dialysis included the propensity for developing peritonitis, anorexia, and a significant plasma protein loss in the dialysate fluid as result of leakage across the peritoneum. Protein loss coupled with anorexia produced a catabolic state, and the animal was euthanatized because of this, at postnephrectomy day 54. The development of a new catheter design alleviated the drainage problems of the straight tube Tenckhoff catheter. Its use coupled with the continuous ambulatory peritoneal dialysis schedule and detailed management techniques allowed using the anephric dog as a model of uremia. In addition, peritoneal dialysis could be a viable treatment for animals presenting with acute reversible anuric or oliguric renal failure where conservative medical management with fluids and diuretics has failed to give clinical improvement.

Published
1984

19. Evaluation of a series of testing procedures to predict neonatal isoerythrolysis in the foal.

Author

Becht JL, Page EH, Morter RL, Boon GD, and Thacker HL

Subjects
Agglutination, Animals, Female, Hemolysin Proteins analysis, Horse Diseases immunology, Horses, Male, Pregnancy, Erythroblastosis, Fetal veterinary, Horse Diseases diagnosis, Isoantigens immunology
Abstract

A series of modified (field) tests were compared to a crossmatch between mare and foal for their reliability in predicting neonatal isoerythrolysis (NI) in eight foals born to experimentally alloimmunized mares. In the field tests, mare's serum, plasma and colostrum were combined with foal erythrocytes washed by a modified procedure to determine which combination was the best predictor of impending NI. A consistent grading system for agglutination and hemolysis was employed. The field tests using mare's plasma demonstrated less agglutination and hemolysis than tests where serum was employed. Immediate assessment of agglutination failed to demonstrate agglutinin activity when compared to tests where incubation was included. Rouleaux formation posed a problem in interpretation of minor agglutination, however the grading of hemolysis was simpler, quicker, and more accurate. The field test that was most reliable when compared to the crossmatch and presuckle anti-foal erythrocyte titers in demonstrating agglutinins was the combination of mare's serum and foal's erythrocytes. The tests for hemolysin detection in serum and colostrum which incorporated rabbit sera as a complement source were also reliable.

Published
1983

20. Induction of lesions of selenium-vitamin E deficiency in ducklings fed silver, copper, cobalt, tellurium, cadmium, or zinc: protection by selenium or vitamin E supplements.

Author

Van Vleet JF, Boon GD, and Ferrans VJ

Subjects
Animals, Cadmium adverse effects, Cobalt adverse effects, Copper adverse effects, Diet, Male, Muscles pathology, Poultry Diseases pathology, Poultry Diseases prevention & control, Silver adverse effects, Tellurium adverse effects, Vitamin E Deficiency chemically induced, Vitamin E Deficiency prevention & control, Zinc adverse effects, Ducks, Poultry Diseases chemically induced, Selenium therapeutic use, Trace Elements adverse effects, Vitamin E therapeutic use, Vitamin E Deficiency veterinary
Abstract

In 3 experiments, 684 newly hatched White Pekin ducklings were fed (for 15 to 28 days) a commercial starter mash that was adequate in selenium and vitamin E (Se-E) content, either alone or with supplements of Ag (3,000 mg/kg of feed, as acetate), Cu (1,500 mg/kg, as sulfate), Co (200 or 500 mg/kg, as chloride), Te (500 mg/kg, as tetrachloride), Cd (100 or 500 mg/kg, as sulfate), Zn (3,000 or 6,000 mg/kg, as sulfate), or V (100 mg/kg, as vanadate). The ducklings fed Ag, Cu, Co, Te, Cd, and Zn frequently developed lesions characteristic of Se-E deficiency, such as necrosis of skeletal and cardiac muscle and of smooth muscle of the gizzard and intestine. Complete protection from the muscle lesions produced by Cu, Co, Te, Cd, and Zn supplements was provided by vitamin E (200 IU of alpha-tocopherol acetate/kg) and Se (2 mg/kg, as selenite). Ducklings fed Ag were protected by supplements of vitamin E and partial protection was achieved by Se addition. The birds fed excessive Zn developed pancreatic necrosis and fibrosis that was not prevented by supplements of Se or vitamin E. Terminally, blood glutathione peroxidase activity was low and hepatic Se concentration was increased in the ducklings fed Ag. However, neither blood glutathione peroxidase activity nor hepatic Se concentrations was consistently abnormal in ducklings fed other trace elements, although lesions of Se-E deficiency were often present in these animals.

Published
1981

21. Induction of lesions of selenium-vitamin E deficiency in weanling swine fed silver, cobalt, tellurium, zinc, cadmium, and vanadium.

Author

Van Vleet JF, Boon GD, and Ferrans VJ

Subjects
Animals, Cadmium adverse effects, Cobalt adverse effects, Liver pathology, Male, Muscles pathology, Myocardium pathology, Silver adverse effects, Swine, Swine Diseases pathology, Tellurium adverse effects, Vanadium adverse effects, Vitamin E Deficiency etiology, Vitamin E Deficiency pathology, Zinc adverse effects, Metals adverse effects, Selenium deficiency, Swine Diseases etiology, Vitamin E Deficiency veterinary
Abstract

Forty-two weanling pigs were allotted to 7 groups and fed (for 10 weeks) a commercial ration that was adequate in selenium and vitamin E (Se-E) content, either alone or with supplements of Ag (3,000 mg/kg of feed, as acetate), Co (500 mg/kg, as chloride), Te (500 mg/kg, as tetrachloride), Zn (3,000 mg/kg, as sulfate), Cd (500 mg/kg, as sulfate), or V (200 mg/kg, as vanadate). The pigs fed the Ag supplement died after 25 to 39 days and had lesions characteristic of Se-E deficiency with accumulations of serous transudates in body cavities and hepatic and cardiac necrosis. In the pigs fed the Ag supplement, there was high hepatic Se content terminally; blood glutathione peroxidase (GSH-Px) activity decreased to low levels several weeks before the pigs died with lesions of Se-E deficiency. Macroscopic lesions of Se-E deficiency were not found in pigs fed Co, Te, Zn, Cd, or V. However, evidence of Se-E deficiency, as indicated by microscopically detected necrosis of cardiac and skeletal muscle, was present in 50% to 65% of the pigs fed Co or Te and occasionally in pigs fed Zn, Cd, and V supplements. The pigs fed Te had marked decrease of blood GSH-Px activity over the last 6 weeks of the feeding period. No consistently abnormal values for blood GSH-Px activity or terminal hepatic Se content were observed in pigs fed Co, Zn, Cd, or V. The pigs fed the Zn supplement grew as rapidly as the control pigs. Evidence of V toxicosis was observed as severe growth suppression, mortality, and marked enteritis and cystitis (with accompanying hydroureter in 1 pig).

Published
1981

22. Evaluation of a spectrophotometric method for canine serum lipase determination.

Author

Whitney MS, Boon GD, Rebar AH, and Ford RB

Subjects
Acute Disease, Animals, Clinical Enzyme Tests, Dithionitrobenzoic Acid, Dogs, Evaluation Studies as Topic, Indicators and Reagents, Mechlorethamine, Pancreatitis diagnosis, Reference Values, Spectrophotometry methods, Dog Diseases diagnosis, Lipase blood, Pancreatitis veterinary
Abstract

The British antilewisite butyrate-dithionitrobenzoate (BALB-DTNB) spectrophotometric serum lipase assay was evaluated for precision, accuracy, and diagnostic usefulness in analyzing canine sera. Sera samples from clinically healthy dogs, dogs with experimentally induced pancreatitis, and dogs with spontaneous pancreatitis were analyzed. A titrimetric method of serum lipase determination was used for comparison. Although the BALB-DTNB method was not found to be precise or accurate for determining the lipase activity of canine serum samples, it seemed to be at least as diagnostically useful as the titrimetric procedure. The small sample size requirement and the speed of analysis of the BALB-DTNB procedure are advantages of this method over the titrimetric method, and thus, its use in place of the titrimetric method is justified. A laboratory reference range of 3 to 37 IU/L was determined for canine serum.

Published
1986

23. Experimental production of neonatal isoerythrolysis in the foal.

Author

Becht JL, Page EH, Morter RL, Boon GD, and Thacker HL

Subjects
Agglutinins analysis, Animals, Erythrocyte Count, Erythrocytes immunology, Female, Horse Diseases blood, Horses, Male, Pregnancy, Erythroblastosis, Fetal veterinary, Horse Diseases etiology, Isoantigens immunology
Abstract

Serological evidence with or without clinical signs of neonatal isoerythrolysis was experimentally produced in 6 of 8 foals born to mares allo-immunized with washed erythrocytes from the stallion. Blood group antigens were determined in all mares, stallions and foals, and the incompatible antigenic factor(s) responsible for the disease were defined. In 5 of 8 foals born to alloimmunized mares, a single antigenic factor difference accounted for the erythrocyte incompatibility between mare and foal. The erythrocyte antigen suspected as the most responsible for isoerythrolysis observed was A1. Agglutinin and hemolysin titers were measured in mare serum and colostrum. Of the presuckle anti-foal erythrocyte titers, colostral and hemolysins titers were greater than serum and agglutinin titers respectively. Foals were allowed to nurse and treatment of affected foals was not attempted which allowed full expression of disease and outcome.

Published
1983

24. Effects of acute pancreatitis on circulating lipids in dogs.

Author

Whitney MS, Boon GD, Rebar AH, and Ford RB

Subjects
Acute Disease, Animals, Cholesterol blood, Dogs, Electrophoresis, Female, Lipoproteins blood, Male, Pancreatitis blood, Triglycerides blood, Dog Diseases blood, Lipids blood, Pancreatitis veterinary
Abstract

Effects of acute pancreatitis on circulating lipids in dogs were evaluated by comparing the serum cholesterol and triglyceride concentrations and plasma lipoprotein electrophoretic patterns of 4 dogs with experimentally induced pancreatitis (EIP), 2 (healthy) sham-operated control (SOC) dogs, and 4 dogs with naturally acquired pancreatitis (NAP) with the concentrations and patterns of 23 healthy, nonoperated control (HNC) dogs. Blood samples were collected once from HNC dogs, 1 to 3 times during the course of the disease in dogs with NAP, and prior to and at 6, 12, 24, 48, 72, and 96 hours after induction of pancreatitis in dogs with EIP or after the sham operation in the SOC dogs. The dogs with EIP did not have turbid serum and did not develop hypercholesterolemia or hypertriglyceridemia. Three of the dogs with NAP had turbid serum and hypertriglyceridemia, and 3 had hypercholesterolemia. The electrophoretic tracings of HNC dogs had predominant alpha-1 peaks and small beta peaks; 2 of the HNC dogs also had small alpha-2 peaks. The tracings of dogs with EIP were similar to those of HNC dogs until 48 to 72 hours after induction of pancreatitis, when dogs with EIP developed increased beta lipoproteins, decreased alpha-1 lipoproteins, and movement of lipoproteins into the alpha-2 zone. The tracings of SOC dogs were similar to those of HNC dogs at all times. Compared with HNC dogs, dogs with NAP all had increased beta lipoproteins, and 2 had decreased alpha-2 lipoproteins. Two dogs with NAP had additional lipoprotein alterations, unlike any seen in dogs with EIP.

Published
1987

25. Patulin mycotoxicosis in the rat: toxicology, pathology and clinical pathology.

Author

McKinley ER, Carlton WW, and Boon GD

Subjects
Animals, Blood Gas Analysis, Blood Glucose analysis, Digestive System drug effects, Digestive System pathology, Leukocyte Count, Male, Rats, Rats, Inbred Strains, Sodium blood, Patulin poisoning, Pyrans poisoning
Abstract

Patulin, a secondary metabolite produced by species of the genera Penicillium and Aspergillus, was administered to male Sprague-Dawley rats, weighing 50-60 g, by the oral, sc and ip routes. The 72-hr LD50 values (in mg/kg weight) were: oral, 55.0; sc, 11.0; ip, 10.0. Mortality was greatest 0-24 hr after administration by the oral and sc routes and 49-72 hr after ip dosing. Gross alterations consisted of gastric and intestinal hyperaemia and distention. Histopathological alterations consisted principally of ulceration and inflammation of the stomach. Patulin was administered orally to rats daily or every other day for 2 wk at doses of 50 or 75% of the oral LD50. Mortality in the treated groups was greater than in controls but was similar for all treated groups. No evidence of cumulative toxicity was found and the gross and histopathological alterations were similar to those found in the LD50 studies. Clinicopathological alterations included metabolic alkalosis with respiratory compensation, oliguria, decreased serum sodium, elevated blood glucose, reduced plasma protein and an elevated total leucocyte count which differential leucocyte counts indicated to be due to neutrophilia. The inflammatory alterations observed in the gastro-intestinal tract may be due to the irritant properties of patulin or to an alteration in the gastro-intestinal flora by the antibiotic activity of patulin.

Published
1982
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26. Citrinin mycotoxicosis in the rabbit: clinicopathological alterations.

Author

Hanika C, Carlton WW, Boon GD, and Tuite J

Subjects
Animals, Bicarbonates blood, Blood Glucose analysis, Blood Proteins analysis, Blood Urea Nitrogen, Citrinin adverse effects, Creatinine blood, Hematocrit, Hydrogen-Ion Concentration, Kidney pathology, Leukocyte Count, Male, Mycotoxins adverse effects, Occult Blood, Potassium blood, Rabbits, Rats, Sodium blood, Benzopyrans pharmacology, Citrinin pharmacology, Kidney drug effects, Mycotoxins pharmacology
Abstract

Citrinin, a nephrotoxic mycotoxin, was dissolved in 0.5 N-NaOH neutralized with HCl and given in a single oral dose of 120 mg/kg (Trial I) or 80 or 100 mg/kg (Trial II) to male New Zealand white rabbits weighing 2.0-2.7 kg. In Trial I, sequential measurements of clinicopathological parameters were made over a 24-hr period. Azotaemia and metabolic acidosis with haemoconcentration and hypokalaemia developed within 4-12 hr. In Trial II, clinicopathological and urinary parameters were measured daily for 7 days. Increased blood urea nitrogen and serum-creatine levels and decreased creatinine clearance indicated renal failure; these values were most abnormal on days 2-4, returning to normal or near normal by day 7 in rabbits that survived. Urine analysis indicated tubular dysfunction and necrosis with glucosuria, isosthenuria and cylindruria; most urinary parameters were normal by day 7.

Published
1984
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27. Isoamylases in clinically normal dogs.

Author

Stickle JE, Carlton WW, and Boon GD

Subjects
Amylases blood, Animals, Duodenum enzymology, Female, Ileum enzymology, Isoenzymes blood, Male, Pancreas enzymology, Amylases metabolism, Dogs metabolism, Isoenzymes metabolism
Abstract

Isoenzymes of canine serum amylase were evaluated by electrophoresis on cellulose acetate membranes in a discontinuous buffer system. Two isoamylase groups were identified in the serum of clinically normal dogs. Most of the serum amylase activity was the more cathodal isoamylase. The anodal isoamylase was rarely observed in serum from normal dogs and, when present, accounted for little of the enzymatic activity. Amylase activities of various tissues were determined and isoenzymes were identified. The anodal isoenzyme was found in the pancreas and uterus. The cathodal isoamylase had its origin mainly from the intestinal tract. Activities of other tissues were not greater than was serum amylase activity. Effects of feeding upon total serum amylase activity and isoenzyme composition also were examined over a period of 5 minutes to 7 hours. Feeding did not markedly alter the serum amylase activity.

Published
1980

28. Red cell fragmentation in the dog: an editorial review.

Author

Rebar AH, Lewis HB, DeNicola DB, Halliwell WH, and Boon GD

Subjects
Animals, Dogs, Erythrocyte Membrane, Erythrocytes ultrastructure, Heinz Bodies ultrastructure, Hematologic Diseases blood, Humans, Spherocytes ultrastructure, Vascular Diseases blood, Dog Diseases blood, Erythrocyte Aging, Erythrocytes pathology, Hematologic Diseases veterinary, Vascular Diseases veterinary
Abstract

Red blood cell fragments in blood smears from dogs are described morphologically and pathogenetically. Categories include microangiopathic fragmentation, spherocytic fragmentation. Heinz body fragmentation, metabolic fragmentation associated with systemic disease, and artifactual fragmentation. Microangiopathic fragmentation is associated with direct physical damage to normal circulating red blood cells as they pass through abnormal capillary beds. Spherocytic fragmentation is a common feature of immune-mediated hemolytic anemia and results from the removal of portions of antibody-coated erythrocyte plasma membranes by phagocytes of the reticuloendothelial system. Heinz body fragmentation occurs when rigid particles of oxidized hemoglobin are torn from affected red cells as they circulate through the spleen. Metabolic fragmentation is an ill-defined syndrome most commonly associated with cholesterol loading of red cell membranes caused by lipid metabolism abnormalities. Resulting spiculated red cells are more susceptible to traumatic disruption. All the types of red cell fragmentation described in dogs have been observed and documented in man.

Published
1981
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30. Effects of dexamethasone on endotoxin shock in the anesthetized pony: hematologic, blood gas, and coagulation changes.

Author

Frauenfelder HC, Fessler JF, Moore AB, Bottoms GD, and Boon GD

Subjects
Acidosis etiology, Acidosis veterinary, Animals, Blood Coagulation drug effects, Dexamethasone administration & dosage, Dexamethasone pharmacology, Endotoxins administration & dosage, Female, Hematocrit veterinary, Horse Diseases blood, Horses, Lactates blood, Leukocytosis etiology, Leukocytosis veterinary, Male, Shock, Septic blood, Shock, Septic drug therapy, Dexamethasone therapeutic use, Horse Diseases drug therapy, Shock, Septic veterinary
Abstract

The effects of dexamethasone (1 mg/kg of body weight) on hematologic, blood gas, and blood coagulation values in anesthetized ponies during endotoxin-induced shock were evaluated. Fifteen ponies were assigned to 3 groups of 5 ponies each: group 1, anesthetized nontreated and dexamethasone-treated controls; group 2, endotoxin, nontreated; group 3, endotoxin, dexamethasone treated. The hematologic changes in this endotoxin shock model included leukopenia and hemoconcentration. Significant hematologic effects were not seen in ponies after administration of dexamethasone. However, dexamethasone treatment resulted in an increased trend in total WBC counts and neutrophils. The blood gas changes reflected a respiratory component resulting from anesthesia and a greater metabolic component from the endotoxemia. The plasma lactate increase was significantly (P less than 0.05) less in ponies treated with dexamethasone, compared with plasma lactate in non-treated ponies. During endotoxin shock, the changes observed in the blood coagulation values included a significant (P less than 0.05) prolongation of the activated partial thromboplastin time and thrombin time and an insignificant prolongation of the prothrombin time. Dexamethasone treatment prevented prolongation of thrombin time and permitted only a mild prolongation of activated partial thromboplastin time. Seemingly, corticosteroids are useful in the treatment of clinical endotoxin shock in horses as indicated by their desirable effects on total WBC, neutrophils, cellular metabolism, and blood coagulation.

Published
1982

31. Endotoxin-induced change in hemograms, plasma enzymes, and blood chemical values in anesthetized ponies: effects of flunixin meglumine.

Author

Fessler JF, Bottoms GD, Roesel OF, Moore AB, Frauenfelder HC, and Boon GD

Subjects
Animals, Blood Glucose metabolism, Clonixin analogs & derivatives, Clonixin pharmacology, Creatine Kinase blood, Escherichia coli, Female, Horse Diseases blood, Horses, Hydrocortisone blood, Hydrogen-Ion Concentration, Insulin blood, Isoenzymes, L-Lactate Dehydrogenase blood, Lactates blood, Male, Shock, Septic blood, Shock, Septic drug therapy, Blood drug effects, Clonixin therapeutic use, Horse Diseases drug therapy, Nicotinic Acids therapeutic use, Shock, Septic veterinary
Abstract

A study was made of flunixin meglumine (FM), an analgesic agent with antiprostaglandin activity, in the management of endotoxin-induced changes in ponies. Three groups of 5 ponies each were used: A--controls, B--nontreated ponies with endotoxin-induced shock, and C--ponies with endotoxin-induced shock treated with FM. Shock was induced in anesthetized ponies with IV injections of Escherichia coli endotoxin. Disruption of glucose homeostasis, insulin levels, hemograms, aerobic metabolism, and cell damage as indicated by plasma enzymes were observed. Treatment with FM (5 minutes) after shock was induced did not prevent general tissue damage as indicated by plasma enzymes, but separation of creatine phosphokinase into its 3 isoenzymes revealed a significant increase in the amount of the creatine phosphokinase isoenzyme bb in group B ponies, but not in FM-treated ponies (group C). The source of this isoenzyme is believed to be brain tissue. Acidosis as indicated by lactic acid and venous pH was less in FM-treated ponies than in nontreated (group B) ponies. Blood glucose and insulin concentrations changed in both groups B and C (endotoxin-induced shock), but the patterns of change were different. The only effect of FM on hematologic values was a significant decrease in blood platelet counts. The results of these experiments indicate that FM improved cellular metabolism and reduced brain damage. These effects were believed to be the result of the maintenance of mean arterial blood pressure and enhanced perfusion of vital organs by preventing extensive vasodilation in the gastrointestinal tract.

Published
1982

32. Studies on the sequential development and pathogenesis of citrinin mycotoxicosis in turkeys and ducklings.

Author

Mehdi NA, Carlton WW, Boon GD, and Tuite J

Subjects
Animals, Kidney Diseases etiology, Kidney Diseases pathology, Kidney Diseases veterinary, Liver Diseases etiology, Liver Diseases pathology, Liver Diseases veterinary, Lymphatic Diseases etiology, Lymphatic Diseases pathology, Lymphatic Diseases veterinary, Male, Necrosis, Poultry Diseases pathology, Rats, Benzopyrans toxicity, Citrinin toxicity, Ducks, Mycotoxins toxicity, Poultry Diseases etiology, Turkeys
Abstract

The toxic effects of citrinin in turkeys and ducklings was studied in four trials. Citrinin dissolved in dimethyl sulfoxide-70% ethanol solution (3:1, volume/volume) was administered by gavage to male turkey poults and male white Pekin ducklings. When seven-day-old ducklings were given doses of citrinin between 30 to 110 mg/kg body weight, most of the treated ducklings which died (49/80) did so within four to 12 hours. Blood samples were collected sequentially at 3, 6, 12, and 24 hours after administration from seven-day-old ducklings given the single lethal dose (LD50). The alterations included hyperkalemia (P less than or equal to 0.01) and metabolic acidosis characterized by reduced blood pH (P less than or equal to 0.01) and base excess (P less than or equal to 0.01). Fourteen-day-old turkeys and ducklings given 56 or 57 mg/kg, respectively, were killed at 1, 3, 6, 12, 24, 48, and 72 hours after treatment. The principal alteration in both species was nephrosis that was more severe in turkeys than in ducklings. Tubular necrosis was the dominant lesion at three to 72 hours in turkeys and at six to 24 hours in ducklings. Hepatic and lymphoid lesions occurred in both turkeys and ducklings treated with citrinin.

Published
1984
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33. Effects of repeated endotoxin injections on prostanoids, hemodynamics, endothelial cells, and survival in ponies.

Author

Templeton CB, Bottoms GD, Fessler JF, Turek JJ, and Boon GD

Subjects
6-Ketoprostaglandin F1 alpha blood, Animals, Arteries cytology, Arteries drug effects, Blood Pressure drug effects, Cardiac Output drug effects, Clonixin analogs & derivatives, Clonixin therapeutic use, Endothelium drug effects, Endothelium ultrastructure, Endotoxins administration & dosage, Female, Gastroenteritis microbiology, Gastroenteritis mortality, Gastroenteritis physiopathology, Horse Diseases mortality, Horses, Male, Meglumine therapeutic use, Microscopy, Electron, Regional Blood Flow drug effects, Sepsis mortality, Thromboxane B2 blood, Time Factors, Endotoxins pharmacology, Hemodynamics drug effects, Horse Diseases physiopathology, Prostaglandins blood, Sepsis physiopathology
Abstract

The objectives of this study were to determine the pathophysiological effects of increasing amounts of endotoxin administered intraperitoneally (IP) for 24 hr at which time an intravenous (IV) injection of endotoxin was given. The ability of flunixin meglumine (FM), a nonsteroidal antiinflammatory drug with antiprostaglandin activity, to provide protective effects was also determined. Eight ponies were divided into two groups of four ponies each; one group (untreated) received endotoxin only and the other group (treated) received endotoxin while being treated with flunixin. Hemodynamic and serum prostanoid changes were recorded for 26 hr during which time five IP and one IV endotoxin injections were given. Both groups behaved similarly until the intravenous endotoxin injection at 24 hr. At that time, the protective effects of flunixin became apparent by preventing increases in thromboxane and prostacyclin concentrations and by maintaining cardiac output, systemic arterial blood pressure, and blood flow to critical organs. Electron microscopic examination of pulmonary arteries of untreated animals revealed extensive endothelial cell damage while treatment with FM reduced this damage. A parallel study involving survival time in two groups of eight ponies each was also conducted using the same endotoxin and treatment protocol. At the end of 7 days, two of eight untreated ponies survived while six of eight treated ponies survived. It was concluded that FM prevented the release of prostanoids, maintained hemodynamics and blood flow nearer pre-endotoxin values, reduced vascular endothelial cell damage, and improved survival.

Published
1985

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