Your search keyword '"Kristin N Grimsrud"' showing total 13 results

1. Injection-site Reactions to Sustained-release Meloxicam in Sprague–Dawley Rats

Author

Leslie A Stewart, Laurel A. Beckett, Yueju Li, Kristin N Grimsrud, Kevin C K Lloyd, and Denise M. Imai

Subjects

Male, medicine.medical_specialty, Erythema, 040301 veterinary sciences, medicine.medical_treatment, Pain, Meloxicam, Gastroenterology, Rats, Sprague-Dawley, 0403 veterinary science, Fibrosis, Internal medicine, medicine, Animals, Anesthesia, Prospective Studies, Prospective cohort study, Adverse effect, Saline, business.industry, Anti-Inflammatory Agents, Non-Steroidal, 0402 animal and dairy science, 04 agricultural and veterinary sciences, medicine.disease, 040201 dairy & animal science, Rats, Peripheral, Delayed-Action Preparations, Female, Animal Science and Zoology, Histopathology, Analgesia, medicine.symptom, business, medicine.drug

Abstract

An extended-release formulation of the NSAID meloxicam (MSR) is used to provide 72 h of continuous analgesia in many species, including rodents. Although standard formulations of meloxicam are frequently used in rats with no observable injection-site reactions, the potential adverse effects from MSR have not been characterized sufficiently nor has a prospective study of these effects been performed in rats. To address this deficiency, we evaluated injection-site reactions after a single subcutaneous administration of MSR (n = 16) or sterile saline (SC, n = 6) in the flank of age- and sex-matched Sprague–Dawley rats. Mass and erythema scores were measured daily for 2 wk, and injection sites were collected for histopathology after euthanasia. Rats were randomly selected for euthanasia at 7 d (n = 12) or 14 d (n = 10) after injection to capture the subacute and chronic phases of mass and erythematic lesion formation. No rats in the SC group developed lesions, whereas all 16 MSR-treated rats developed masses. The median time to first mass in the MSR treatment group was 3 d (95% CI, 2–3 d), and nearly 8 d for erythema (95% CI, 6.7–9.1 d). The trajectory of mass lesion severity showed rapid progression from score 1 at onset (day 2 or 3) to score 2 for almost all animals by day 5 or 6. Histopathology was characterized by localized inflammation with central necrosis and peripheral fibrosis, with some sections showing developing draining tracts. Given the high prevalence and severity of localized skin reactions, MSR analgesia should be considered carefully for Sprague–Dawley rats.

Published

2020

2. Generation of desminopathy in rats using CRISPR‐Cas9

Author

Kristin N Grimsrud, Henning T. Langer, Kevin C K Lloyd, Agata A. Mossakowski, Hermann Zbinden-Foncea, Joshua A. Wood, Keith Baar, and Brandon J. Willis

Subjects

Male, 0301 basic medicine, lcsh:Diseases of the musculoskeletal system, Mutant, Injury, Desmin, lcsh:QM1-695, Muscle hypertrophy, Dystrophin, Dysferlin, Mice, 03 medical and health sciences, 0302 clinical medicine, Muscular Diseases, Physiology (medical), medicine, Animals, Orthopedics and Sports Medicine, Muscular dystrophy, Exercise, Force transfer, Syntrophin, biology, business.industry, Precision medicine, Wild type, Original Articles, lcsh:Human anatomy, medicine.disease, Molecular biology, Rats, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation, biology.protein, Original Article, CRISPR-Cas Systems, lcsh:RC925-935, business

Abstract

Author(s): Langer, Henning T; Mossakowski, Agata A; Willis, Brandon J; Grimsrud, Kristin N; Wood, Joshua A; Lloyd, Kevin CK; Zbinden-Foncea, Hermann; Baar, Keith | Abstract: BackgroundDesminopathy is a clinically heterogeneous muscle disease caused by over 60 different mutations in desmin. The most common mutation with a clinical phenotype in humans is an exchange of arginine to proline at position 350 of desmin leading to p.R350P. We created the first CRISPR-Cas9 engineered rat model for a muscle disease by mirroring the R350P mutation in humans.MethodsUsing CRISPR-Cas9 technology, Des c.1045-1046 (AGG g CCG) was introduced into exon 6 of the rat genome causing p.R349P. The genotype of each animal was confirmed via quantitative PCR. Six male rats with a mutation in desmin (n = 6) between the age of 120-150 days and an equal number of wild type littermates (n = 6) were used for experiments. Maximal plantar flexion force was measured in vivo and combined with the collection of muscle weights, immunoblotting, and histological analysis. In addition to the baseline phenotyping, we performed a synergist ablation study in the same animals.ResultsWe found a difference in the number of central nuclei between desmin mutants (1 ± 0.4%) and wild type littermates (0.2 ± 0.1%; P l 0.05). While muscle weights did not differ, we found the levels of many structural proteins to be altered in mutant animals. Dystrophin and syntrophin were increased 54% and 45% in desmin mutants, respectively (P l 0.05). Dysferlin and Annexin A2, proteins associated with membrane repair, were increased two-fold and 32%, respectively, in mutants (P l 0.05). Synergist ablation caused similar increases in muscle weight between mutant and wild type animals, but changes in fibre diameter revealed that fibre hypertrophy in desmin mutants was hampered compared with wild type animals (P l 0.05).ConclusionsWe created a novel animal model for desminopathy that will be a useful tool in furthering our understanding of the disease. While mutant animals at an age corresponding to a preclinical age in humans show no macroscopic differences, microscopic and molecular changes are already present. Future studies should aim to further decipher those biological changes that precede the clinical progression of disease and test therapeutic approaches to delay disease progression.

Published

2020

3. The Mutant Mouse Resource and Research Center (MMRRC): the NIH-supported National Public Repository and Distribution Archive of Mutant Mouse Models in the USA

Author

Samit Patel, Franziska B. Grieder, Ian F Korf, Laura G. Reinholdt, Oleg Mirochnitchenko, Kristin N Grimsrud, Kevin C K Lloyd, Terry Magnuson, Virginia Godfrey, Cat Lutz, Craig L. Franklin, and James M. Amos-Landgraf

Subjects

Resource (biology), Biomedical Research, Library science, Distribution (economics), Stem Cell Research - Embryonic - Non-Human, Scientific experiment, Biology, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Genetics, Animals, Humans, Aetiology, 030304 developmental biology, Genetics & Heredity, 0303 health sciences, business.industry, Animal, Reproducibility of Results, Stem Cell Research, Public repository, United States, Outreach, Disease Models, Animal, Good Health and Well Being, National Institutes of Health (U.S.), Infectious disease (medical specialty), Informatics, Disease Models, HIV/AIDS, business, 030217 neurology & neurosurgery, Research center, 2.6 Resources and infrastructure (aetiology)

Abstract

The Mutant Mouse Resource and Research Center (MMRRC) Program is the pre-eminent public national mutant mouse repository and distribution archive in the USA, serving as a national resource of mutant mice available to the global scientific community for biomedical research. Established more than two decades ago with grants from the National Institutes of Health (NIH), the MMRRC Program supports a Consortium of regionally distributed and dedicated vivaria, laboratories, and offices (Centers) and an Informatics Coordination and Service Center (ICSC) at three academic teaching and research universities and one non-profit genetic research institution. The MMRRC Program accepts the submission of unique, scientifically rigorous, and experimentally valuable genetically altered and other mouse models donated by academic and commercial scientists and organizations for deposition, maintenance, preservation, and dissemination to scientists upon request. The four Centers maintain an archive of nearly 60,000 mutant alleles as live mice, frozen germplasm, and/or embryonic stem (ES) cells. Since its inception, the Centers have fulfilled 13,184 orders for mutant mouse models from 9591 scientists at 6626 institutions around the globe. Centers also provide numerous services that facilitate using mutant mouse models obtained from the MMRRC, including genetic assays, microbiome analysis, analytical phenotyping and pathology, cryorecovery, mouse husbandry, infectious disease surveillance and diagnosis, and disease modeling. The ICSC coordinates activities between the Centers, manages the website (mmrrc.org) and online catalog, and conducts communication, outreach, and education to the research community. Centers preserve, secure, and protect mutant mouse lines in perpetuity, promote rigor and reproducibility in scientific experiments using mice, provide experiential training and consultation in the responsible use of mice in research, and pursue cutting edge technologies to advance biomedical studies using mice to improve human health. Researchers benefit from an expansive list of well-defined mouse models of disease that meet the highest standards of rigor and reproducibility, while donating investigators benefit by having their mouse lines preserved, protected, and distributed in compliance with NIH policies.

Published

2021

4. Injection Reactions after Administration of Sustained-release Meloxicam to BALB/cJ, C57BL/6J, and Crl:CD1(ICR) Mice

Author

Leslie A Stewart, Denise M. Imai, Stephanie R Fuetsch, Laurel A. Beckett, Yueju Li, Kristin N Grimsrud, and Kevin C K Lloyd

Subjects

Male, medicine.medical_specialty, Erythema, medicine.medical_treatment, Injections, Subcutaneous, CD1, Inbred Strains, Anti-Inflammatory Agents, Inflammation, Mice, Inbred Strains, Meloxicam, Medical and Health Sciences, Injections, Rodent Diseases, Subcutaneous injection, Mice, Inbred strain, Internal medicine, medicine, Animals, Anesthesia, Veterinary Sciences, Saline, Sex Characteristics, Agricultural and Veterinary Sciences, business.industry, Subcutaneous, Anti-Inflammatory Agents, Non-Steroidal, Biological Sciences, medicine.disease, Endocrinology, Delayed-Action Preparations, Animal Science and Zoology, Female, medicine.symptom, Panniculitis, business, Non-Steroidal, medicine.drug

Abstract

The sustained-release formulation of meloxicam (MSR) is a compounded NSAID that may provide pain relief for as long as 72 h after administration. MSR injection-site skin reactions have occurred in several species but have not previously been observed in mice. We investigated the development and progression of localized skin reactions after a single injection of MSR in Crl:CD1(ICR), C57BL/6J, and BALB/cJ mice. Each mouse received a subcutaneous injection of MSR (n = 60), standard-formulation meloxicam (MEL; n = 24) or saline (control; SC; n = 24) and was scored daily according to a 5-point system for erythema and mass characteristics. Mice were euthanized at either 7 or 14 d after injection and underwent postmortem analysis. MSR-treated mice had more erythematous and mass reactions than did MEL and SC mice. Mass lesions developed in 49 MSR mice (82%; 95% CI, 70% to 90%), 5 MEL animals (21%; 95% CI, 7% to 42%), and 1 SC mouse. MSR-treated BALB/cJ developed erythematous lesions less frequently than similarly treated Crl:CD1(ICR) or C57BL/6J. Lesions often were ventrolateral to the injection site. The median times to the appearance of mass and erythematous lesions were 2 d and 3 d, respectively. Histologically, the erythematous and mass reactions correlated with necrotizing to pyogranulomatous injection-site panniculitis. Inflammation severity scores at 7 and 14 d after injection were greater in the MSR-treated group than the other 2 groups. No strain- or sex-associated differences emerged except that inflammation severity scores at day 14 were higher in Crl:CD1(ICR) females than males. The character of the inflammatory response in MSR-treated mice did not differ between 7 and 14 d after injection, indicating that MSR-induced inflammation is slow to resolve. The ventral migration and delayed onset of MSR injection-site reactions could result in their being attributed to another cause or not being identified. Researchers and clinicians should be aware of the potential for slowly resolving injection-site reactions with MSR.

Published

2021

5. Hypoglycemia after Bariatric Surgery in Mice and Optimal Dosage and Efficacy of Glucose Supplementation

Author

Kristin N Grimsrud, Kevin C K Lloyd, Zoe Y Hsi, and Leslie A Stewart

Subjects

Male, medicine.medical_specialty, 040301 veterinary sciences, Injections, Subcutaneous, Gastric Bypass, Hypoglycemia, Inbred C57BL, Medical and Health Sciences, General Biochemistry, Genetics and Molecular Biology, Injections, 0403 veterinary science, Subcutaneous injection, Mice, Pharmacokinetics, Pain assessment, Diabetes mellitus, Medicine, Animals, Obesity, Veterinary Sciences, Adverse effect, Metabolic and endocrine, Original Research, General Veterinary, Agricultural and Veterinary Sciences, business.industry, Animal, Subcutaneous, Prevention, Diabetes, 04 agricultural and veterinary sciences, Biological Sciences, medicine.disease, Pathophysiology, Surgery, Mice, Inbred C57BL, Disease Models, Animal, Editorial, Glucose, Disease Models, Female, business

Abstract

The Roux-en-Y Gastric Bypass (RYGB) mouse model is a vital tool for studying the pathophysiology of bariatric surgery and contributes greatly to research on obesity and diabetes. However, complications including postsurgical hypoglycemia can have profoundly negative effects. Unlike in humans, blood glucose (BG) is not typically managed in postoperative rodents, despite their critical role as translational models; without this management, rodents can experience hypoglycemia, potentially impairing wound healing, decreasing survivability, complicating interpretation of research data, and limiting translational utility. In this project, we sought to identify an optimal method for minimally invasive administration of dextrose in C57BL/6N (n = 16; 8 male, 8 female) mice. To do so, we characterized BG pharmacokinetic profiles after subcutaneous and oral–transmucosal (OTM) administration of dextrose. Compared with OTM dosage, the subcutaneous route provided more consistent and reliable delivery of glucose and did not cause significant adverse reactions. We then evaluated the frequency of hypoglycemic events after RYGB in C57BL/6N mice (n = 16; 8 male, 8 female) and the effects of subcutaneous dextrose supplementation on morbidity and mortality. BG measurement and behavioral pain assessment (grimace test) were performed for 3 d after surgery. Hypoglycemic (BG ≤ 60 mg/dL) animals were assigned to dose (5% dextrose SC) or no-dose treatment groups. Nearly all (87%) mice became hypoglycemic; 2 of these mice died. No significant intergroup difference in grimace score or mortality was detected. Overall, our results demonstrate that hypoglycemia is a frequent adverse event after RYGB in mice and that subcutaneous injection of dextrose is a safe and effective way to manage hypoglycemia. Further studies are necessary to optimize the intervention threshold and optimal dosage; regardless, we recommend glycemic management after RYGB surgery in mice.

Published

2020

6. Development of outbred CD1 mouse colonies with distinct standardized gut microbiota profiles for use in complex microbiota targeted studies

Author

Kristin N Grimsrud, Marcia L. Hart, Allison R. Rogala, Kevin C K Lloyd, Aaron C. Ericsson, Craig L. Franklin, Virginia Godfrey, and Judith N. Nielsen

Subjects

Male, 0301 basic medicine, Rodent, Offspring, CD1, lcsh:Medicine, Breeding, Gut flora, Inbred C57BL, Article, Mice, 03 medical and health sciences, Models, biology.animal, Animals, Microbiome, lcsh:Science, Genetics, Multidisciplinary, biology, Animal, lcsh:R, Embryo, Fecal Microbiota Transplantation, Embryo Transfer, biology.organism_classification, Housing, Animal, Phenotype, Gastrointestinal Microbiome, Mice, Inbred C57BL, 030104 developmental biology, Models, Animal, Housing, Amplicon sequencing, Female, lcsh:Q, Biotechnology

Abstract

Studies indicate that the gut microbiota (GM) can significantly influence both local and systemic host physiologic processes. With rising concern for optimization of experimental reproducibility and translatability, it is essential to consider the GM in study design. However, GM profiles can vary between rodent producers making consistency between models challenging. To circumvent this, we developed outbred CD1 mouse colonies with stable, complex GM profiles that can be used as donors for a variety of GM transfer techniques including rederivation, co-housing, cross-foster, and fecal microbiota transfer (FMT). CD1 embryos were surgically transferred into CD1 or C57BL/6 surrogate dams that varied by GM composition and complexity to establish four separate mouse colonies harboring GM profiles representative of contemporary mouse producers. Using targeted 16S rRNA amplicon sequencing, subsequent female offspring were found to have similar GM profiles to surrogate dams. Furthermore, breeding colonies of CD1 mice with distinct GM profiles were maintained for nine generations, demonstrating GM stability within these colonies. To confirm GM stability, we shipped cohorts of these four colonies to collaborating institutions and found no significant variation in GM composition. These mice are an invaluable experimental resource that can be used to investigate GM effects on mouse model phenotype.

Published

2018

7. Complex electrophysiological remodeling in postinfarction ischemic heart failure

Author

Leighton T. Izu, Luiz Belardinelli, Claus S. Sondergaard, Kenneth S. Ginsburg, Bence Hegyi, Jouko Levijoki, Zhong Jian, Rafael Shimkunas, Donald M. Bers, W. Douglas Boyd, András Varró, Leigh G. Griffiths, Tamás Bányász, Ye Chen-Izu, Julie Bossuyt, Julius Gy. Papp, Kristin N Grimsrud, Nipavan Chiamvimonvat, Zana Coulibaly, and Piero Pollesello

Subjects

0301 basic medicine, medicine.medical_specialty, Swine, Cells, Myocardial Infarction, Action Potentials, Arrhythmias, 030204 cardiovascular system & hematology, Cardiovascular, 03 medical and health sciences, action potential, 0302 clinical medicine, Internal medicine, medicine, Animals, Myocyte, Repolarization, Myocytes, Cardiac, Elméleti orvostudományok, Myocardial infarction, ionic currents, Cells, Cultured, Heart Disease - Coronary Heart Disease, Heart Failure, Myocytes, Cultured, Multidisciplinary, Inward-rectifier potassium ion channel, Chemistry, ischemic heart failure, Arrhythmias, Cardiac, Orvostudományok, electrophysiology, medicine.disease, Electrophysiological Phenomena, Electrophysiology, Heart Disease, 030104 developmental biology, PNAS Plus, Heart failure, Cardiology, Calcium, High incidence, Ischemic heart, Cardiac

Abstract

© 2018 National Academy of Sciences. All Rights Reserved. Heart failure (HF) following myocardial infarction (MI) is associated with high incidence of cardiac arrhythmias. Development of therapeutic strategy requires detailed understanding of electrophysiological remodeling. However, changes of ionic currents in ischemic HF remain incompletely understood, especially in translational largeanimal models. Here, we systematically measure the major ionic currents in ventricular myocytes from the infarct border and remote zones in a porcine model of post-MI HF. We recorded eight ionic currents during the cell's action potential (AP) under physiologically relevant conditions usingselfAP-clamp sequential dissection. Compared with healthy controls, HF-remote zone myocytes exhibited increased late Na+ current, Ca2+-activated K+ current, Ca2+-activated Cl- current, decreased rapid delayed rectifier K+current, and altered Na+/Ca2+exchange current profile. In HF-border zone myocytes, the above changes also occurred but with additional decrease of L-type Ca2+current, decrease of inward rectifier K+current, and Ca2+release-dependent delayed after-depolarizations. Our data reveal that the changes in any individual current are relatively small, but the integrated impacts shift the balance between the inward and outward currents to shorten AP in the border zone but prolong AP in the remote zone. This differential remodeling in post-MI HF increases the inhomogeneity of AP repolarization, which may enhance the arrhythmogenic substrate. Our comprehensive findings provide a mechanistic framework for understanding why single-channel blockers may fail to suppress arrhythmias, and highlight the need to consider the rich tableau and integration of many ionic currents in designing therapeutic strategies for treating arrhythmias in HF.

Published

2018

8. Pharmacokinetic profile in relation to anaesthesia characteristics after a 5% micellar microemulsion of propofol in the horse

Author

Scott D Stanley, Pedro Boscan, Kristin N Grimsrud, Marlis L. Rezende, Eugene Steffey, and Khursheed R. Mama

Subjects

Male, Chemistry, Pharmaceutical, Sedation, Pharmacology, Drug Administration Schedule, Pharmacokinetics, Infusion Procedure, medicine, Animals, Horses, Infusions, Intravenous, Propofol, Micelles, ED50, business.industry, Half-life, Horse, Venous blood, Anesthesiology and Pain Medicine, Anesthesia, Anesthesia Recovery Period, Anesthesia, Intravenous, Emulsions, Female, medicine.symptom, business, Anesthetics, Intravenous, Half-Life, medicine.drug

Abstract

Background To define the pharmacokinetic profile of propofol 5% microemulsion formulation in horses. Methods First, propofol was administered as bolus injection (2 mg kg−1) to six xylazine-sedated horses. Secondly, after sedation and bolus injection, propofol was maintained with continuous infusion for 3 h [8.1 (sd 3.2) mg kg−1 h−1] to the same six horses. Thirdly, in two horses, a commercial propofol was used for comparison. Response to noxious stimulation was used to evaluate analgesia. Venous blood samples were obtained to measure propofol plasma concentration using liquid chromatography-mass spectrometry analysis. The plasma concentrations were related to the anaesthesia characteristics to determine the ED50. Results The pharmacokinetic profile of propofol is best characterized by a non-compartmental model. The mean (confidence interval) for area under plasma concentration–time curve, elimination half-life, mean residence time, and clearance was 41 min µg ml−1 (±7.7), 44.8 min (±21.3), 13.7 min (±3.2), and 45.8 ml min−1 kg−1 (±6.5), respectively. Linear regression analysis showed a correlation between plasma concentration and infusion rate (r2=0.47). Most propofol infusion rates did not inhibit the response to noxious stimulation and rates above 11.9 mg kg−1 h−1 caused involuntary muscle contractions. Better recoveries were associated with lower propofol plasma concentrations. Propofol plasma concentration frequently increased when horses woke from anaesthesia. Conclusions Caution is warranted when propofol is used for continuous infusion due to variable kinetics, myoclonal activity, poor analgesia, and less desirable recovery quality.

Published

2010

9. Transgenerational effects of binge drinking in a primate model: implications for human health

Author

Kristin N Grimsrud, Catherine A. VandeVoort, Uros Midic, Namdori R. Mtango, and Keith E. Latham

Subjects

Pregnancy Rate, Health Status, Poison control, Reproductive health and childbirth, Substance Misuse, Alcohol Use and Health, Models, Pregnancy, Cohort Effect, media_common, Pediatric, Obstetrics and Gynecology, Alcoholism, medicine.anatomical_structure, Models, Animal, Public Health and Health Services, Female, medicine.medical_specialty, media_common.quotation_subject, Cumulus cells, Clinical Sciences, Binge drinking, Article, Binge Drinking, Andrology, reproduction, Paediatrics and Reproductive Medicine, medicine, Animals, Humans, Blastocyst, Obstetrics & Reproductive Medicine, Ovulation, Gynecology, Ethanol, business.industry, Animal, Contraception/Reproduction, Embryo culture, Oocyte, medicine.disease, Macaca mulatta, Pregnancy rate, Good Health and Well Being, Reproductive Medicine, granulosa cells, Infertility, Oocytes, business, fetal alcohol syndrome, transcriptome, cDNA array

Abstract

Objective To determine if binge ethanol consumption before ovulation affects oocyte quality, gene expression, and subsequent embryo development. Design Binge levels of ethanol were given twice weekly for 6 months, followed by a standard in vitro fertilization cycle and subsequent natural mating. Setting National primate research center. Animal(s) Adult female rhesus monkeys. Intervention(s) Binge levels of ethanol, given twice weekly for 6 months before a standard in vitro fertilization cycle with or without embryo culture. With in vivo development, ethanol treatment continued until pregnancy was identified. Main Outcome Measure(s) Oocyte and cumulus/granulosa cell gene expression, embryo development to blastocyst, and pregnancy rate. Result(s) Embryo development in vitro was reduced; changes were found in oocyte and cumulus cell gene expression; and spontaneous abortion during very early gestation increased. Conclusion(s) This study provides evidence that binge drinking can affect the developmental potential of oocytes even after alcohol consumption has ceased.

Published

2015

10. Pharmacokinetic and pharmacodynamic analysis comparing diverse effects of detomidine, medetomidine, and dexmedetomidine in the horse: a population analysis

Author

Kristin N Grimsrud, S. Ait-Oudhia, Marlis L. Rezende, Khursheed R. Mama, Scott D Stanley, Blythe Durbin-Johnson, David M. Rocke, and William J. Jusko

Subjects

Male, Population, Pharmacology, Models, Biological, Article, Dose-Response Relationship, Pharmacokinetics, Models, In vivo, medicine, Animals, Veterinary Sciences, Horses, Dexmedetomidine, education, Detomidine, education.field_of_study, General Veterinary, Dose-Response Relationship, Drug, Chemistry, Imidazoles, Adrenergic alpha-2 Receptor Antagonists, Medetomidine, Biological, Dose–response relationship, Pharmacodynamics, Female, Drug, medicine.drug

Abstract

The present study characterizes the pharmacokinetic (PK) and pharmacodynamic (PD) relationships of the α2-adrenergic receptor agonists detomidine (DET), medetomidine (MED) and dexmedetomidine (DEX) in parallel groups of horses from in vivo data after single bolus doses. Head height (HH), heart rate (HR), and blood glucose concentrations were measured over 6 h. Compartmental PK and minimal physiologically based PK (mPBPK) models were applied and incorporated into basic and extended indirect response models (IRM). Population PK/PD analysis was conducted using the Monolix software implementing the stochastic approximation expectation maximization algorithm. Marked reductions in HH and HR were found. The drug concentrations required to obtain inhibition at half-maximal effect (IC50 ) were approximately four times larger for DET than MED and DEX for both HH and HR. These effects were not gender dependent. Medetomidine had a greater influence on the increase in glucose concentration than DEX. The developed models demonstrate the use of mechanistic and mPBPK/PD models for the analysis of clinically obtainable in vivo data.

Published

2014

11. Pharmacokinetics and pharmacodynamics of intravenous dexmedetomidine in the horse

Author

Scott D Stanley, Kristin N Grimsrud, Marlis L. Rezende, Khursheed R. Mama, and Eugene Steffey

Subjects

Pharmacology, Bradycardia, Male, General Veterinary, business.industry, Analgesic, Horse, Physiological responses, Nociception, Pharmacokinetics, Pharmacodynamics, Anesthesia, Area Under Curve, Injections, Intravenous, medicine, Adrenergic alpha-2 Receptor Agonists, Animals, Female, Horses, Dexmedetomidine, medicine.symptom, business, medicine.drug

Abstract

The aim of the study was to describe the pharmacokinetics and selected pharmacodynamics of intravenous dexmedetomidine in horses. Eight adult horses received 5 μg/kg dexmedetomidine IV. Blood samples were collected before and for 10 h after drug administration to determine dexmedetomidine plasma concentrations. Pharmacokinetic parameters were calculated using noncompartmental analysis. Data from one outlier were excluded from the statistical summary. Behavioral and physiological responses were recorded before and for 6 h after dexmedetomidine administration. Dexmedetomidine concentrations decreased rapidly (elimination half-life of 8.03 ± 0.84 min). Time of last detection varied from 30 to 60 min. Bradycardia was noted at 4 and 10 min after drug administration (26 ± 8 and 29 ± 8 beats/min respectively). Head height decreased by 70% at 4 and 10 min and gradually returned to baseline. Ability to ambulate was decreased for 60 min following drug administration, and mechanical nociceptive threshold was increased during 30 min. Blood glucose peaked at 30 min (134 ± 24 mg/dL) and borborygmi were decreased for the first hour after dexmedetomidine administration. Dexmedetomidine was quickly eliminated as indicated by the rapid decrease in plasma concentrations. Physiological, behavioral, and analgesic effects observed after dexmedetomidine administration were of short duration.

Published

2013

12. Pharmacokinetics and pharmacodynamics of intravenous medetomidine in the horse

Author

Eugene Steffey, Khursheed R. Mama, Scott D Stanley, and Kristin N Grimsrud

Subjects

Blood Glucose, Male, Alpha-adrenergic agonist, Respiratory rate, Sedation, Pharmacokinetics, Respiratory Rate, Heart Rate, Bradycardia, Medicine, Animals, Horses, Volume of distribution, General Veterinary, business.industry, Horse, Analgesics, Non-Narcotic, Medetomidine, Anesthesia, Pharmacodynamics, Injections, Intravenous, Female, medicine.symptom, Analgesia, business, medicine.drug

Abstract

Objective To describe the pharmacodynamics and pharmacokinetics following an intravenous (IV) bolus dose of medetomidine in the horse. Study design Prospective experimental trial. Animals Eight, mature healthy horses age 11.7 ± 4.6 (mean ± SD) years, weighing 557 ± 54 kg. Methods Medetomidine (10 μg kg −1 ) was administered IV. Blood was sampled at fixed time points from before drug administration to 48 hours post administration. Behavioral, physiological and biochemical data were obtained at predetermined time points from 0 minutes to 24 hours post administration. An algometer was also used to measure threshold responses to noxious stimuli. Medetomidine concentrations were determined by liquid chromatography-Mass Spectrometry and used for calculation of pharmacokinetic parameters using noncompartmental and compartmental analysis. Results Pharmacokinetic analysis estimated that medetomidine peaked (8.86 ± 3.87 ng mL −1 ) at 6.4 ± 2.7 minutes following administration and was last detected at 165 ± 77 minutes post administration. Medetomidine had a clearance of 39.6 ± 14.6 mL kg −1 minute −1 and a volume of distribution of 1854 ± 565 mL kg −1 . The elimination half-life was 29.1 ± 12.5 minutes. Glucose concentration reached a maximum of 176 ± 46 mg dL −1 approximately 1 hour post administration. Decreased heart rate, respiratory rate, borborygmi, packed cell volume, and total protein concentration were observed following administration. Horses lowered their heads from 107 ± 12 to 20 ± 10 cm within 10 minutes of drug administration and gradually returned to normal. Horse mobility decreased after drug administration. An increased mechanical threshold was present from 10 to 45 minutes and horses were less responsive to sound. Conclusion and clinical relevance Behavioral and physiological effects following intravenous administration positively correlate with pharmacokinetic profiles from plasma medetomidine concentrations. Glucose concentration gradually transiently increased following medetomidine administration. The analgesic effect of the drug appeared to have a very short duration.

Published

2011

13. Pharmacokinetics of detomidine and its metabolites following intravenous and intramuscular administration in horses

Author

Sara M Thomasy, Khursheed R. Mama, Scott D Stanley, and Kristin N Grimsrud

Subjects

Volume of distribution, Detomidine, Cross-Over Studies, business.industry, Sedation, Area under the curve, Imidazoles, Horse, General Medicine, Pharmacology, Crossover study, Injections, Intramuscular, Pharmacokinetics, Anesthesia, Area Under Curve, Injections, Intravenous, medicine, Animals, Hypnotics and Sedatives, Horses, medicine.symptom, business, Intramuscular injection, medicine.drug, Half-Life

Abstract

Summary Reasons for performing study: Detomidine is commonly used i.v. for sedation and analgesia in horses, but the pharmacokinetics and metabolism of this drug have not been well described. Objectives: To describe the pharmacokinetics of detomidine and its metabolites, 3-hydroxy-detomidine (OH-detomidine) and detomidine 3-carboxylic acid (COOH-detomidine), after i.v. and i.m. administration of a single dose to horses. Methods: Eight horses were used in a balanced crossover design study. In Phase 1, 4 horses received a single dose of i.v. detomidine, administered 30 μg/kg bwt and 4 a single dose i.m. 30 ug/kg bwt. In Phase 2, treatments were reversed. Plasma detomidine, OH-detomidine and COOH-detomidine were measured at predetermined time points using liquid chromatography-mass spectrometry. Results: Following i.v. administration, detomidine was distributed rapidly and eliminated with a half-life (t1/2(el)) of approximately 30 min. Following i.m. administration, detomidine was distributed and eliminated with t1/2(el) of approximately one hour. Following, i.v. administration, detomidine clearance had a mean, median and range of 12.41, 11.66 and 10.10–18.37 ml/min/kg bwt, respectively. Detomidine had a volume of distribution with the mean, median and range for i.v. administration of 470, 478 and 215–687 ml/kg bwt, respectively. OH-detomidine was detected sooner than COOH-detomidine; however, COOH-detomidine had a much greater area under the curve. Conclusions and potential relevance: These pharmacokinetic parameters provide information necessary for determination of peak plasma concentrations and clearance of detomidine in mature horses. The results suggest that, when a longer duration of plasma concentration is warranted, the i.m. route should be considered.

Published

2009