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2. Mouse organoids as an in vitro tool to study the in vivo intestinal response to cytotoxicants

Author

Jardi, F., primary, Kelly, C., additional, Teague, C., additional, Fowler-Williams, H., additional, Sevin, D. C., additional, Rodrigues, D., additional, Jo, H., additional, Ferreira, S., additional, Herpers, B., additional, Van Heerden, M., additional, de Kok, T., additional, Pin, C., additional, Lynch, A., additional, Duckworth, C. A., additional, De Jonghe, S., additional, Lammens, L., additional, and Pritchard, D. M., additional

Published
2022
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6. Optimization of a 5-Fluorouracil-induced intestinal injury model in mice to construct a multi-scale predictive model of drug-induced intestinal toxicity

Author

Jardi, F., Van Heerden, M., Vereyken, L., Erkens, T., Rodrigues, D. F., Kleinjans, J. C. S., de Kok, T. M., Ferreria, S., Gardner, I., Fisher, C., Pritchard, M., Lynch, A., Sevin, D., Beattie, K., Pin, C., Lammens, L., de Jonghe, S., Toxicogenomics, RS: MHeNs - R3 - Neuroscience, RS: GROW - R1 - Prevention, RS: FSE MaCSBio, RS: FPN MaCSBio, and RS: FHML MaCSBio

Published
2019

7. Legacy data sharing to improve drug safety assessment

Author

Sanz, F., Pognan, F., Steger-Hartmann, T., Díaz, C., Cases, M., Pastor, M., Marc, P., Wichard, J., Briggs, K., Watson, D.K., Kleinöder, T., Yang, C., Amberg, A., Beaumont, M., Brookes, A.J., Brunak, S., Cronin, M.T.D., Ecker, G.F., Escher, S., Greene, N., Guzmán, A., Hersey, A., Jacques, P., Lammens, L., Mestres, J., Muster, W., Northeved, H., Pinches, M., Saiz, J., Sajot, N., Valencia, A., Lei, J. van der, Vermeulen, N.P.E., Vock, E., Wolber, G., Zamora, I., and Publica

Abstract

The sharing of legacy preclinical safety data among pharmaceutical companies and its integration with other information sources offers unprecedented opportunities to improve the early assessment of drug safety. Here, we discuss the experience of the eTOX project, which was established through the Innovative Medicines Initiative to explore this possibility.

Published
2017

8. 'La escuela es el futuro' Een onderzoek naar de kwaliteit van basisonderwijs in een autonoom gebied.

Author

Lammens, L., van Gijsel, M. (Thesis Advisor), Lammens, L., and van Gijsel, M. (Thesis Advisor)

Abstract

Een onderzoek in een gedeeltelijk autonoom gebied naar de relatie hiervan met de kwaliteit van het onderwijs, in Puerto Cabezas, Nicaragua. Centraal staan de concepten verantwoordelijkheid, kennisoverdracht en ontwikkeling en de beleving van de lokale bevolking van deze concepten. Gedeelde verantwoordelijkheid in het onderwijs zorgt er voor dat niet iedere partij zijn taken nakomt, waardoor de nalatigheid zorgt voor achterstallig onderhoud, het gebrek aan lesmateriaal en een kwalitatief slechte lerarenopleiding. Het nationale onderwijs zorgt ervoor dat de voertaal Spaans is, terwijl de lokale bevolking van Puerto Cabezas voornamelijk Miskitu spreekt. Belangrijk voor kennisoverdracht en de ontwikkeling van het gebied is dat er een vorm van onderwijs bestaat die aansluit bij de lokale cultuur en tradities van de Miskitu. Hierdoor kunnen kinderen zich ontwikkelen en richten op een perspectiefrijke toekomst.

Published
2012

9. Vie privée et intégration des données de santé synthèse de rapport

Author

UCL - SSS/IRSS - Institut de recherche santé et société, Doumont, Dominique, Cols, F., D'Hoore, William, Coppieters, Y., Ingenbleek, A., Lammens, L., Deboosere, P., Levêque, A., UCL - SSS/IRSS - Institut de recherche santé et société, Doumont, Dominique, Cols, F., D'Hoore, William, Coppieters, Y., Ingenbleek, A., Lammens, L., Deboosere, P., and Levêque, A.

Abstract

Le présent rapport est subdivisé en deux chapitres : l’un consacré au cadre légal belge en matière de protection de la vie privée lors du traitement de données à caractère personnel et l’autre consacré à la plate-forme électronique d’échange de données relatives à la santé (plate-forme eHealth). Le premier chapitre définit des concepts clés en lien direct avec l’application de la loi sur la protection de la vie privée en Belgique. Il décrit également les champs d’application (territorial, temporel, personnel et matériel). Il est également fait mention de situations d’exception pour lesquelles des dispositions sont prises. Enfin, une importante partie de ce premier chapitre est consacrée aux conditions de licéité du traitement de données à caractère personnel. Le second chapitre rend compte des « origines » du projet eHealth, plate-forme électronique d’échange de données relatives à la santé en Belgique. Il décrit également les différentes modalités d’accès à cette plate-forme ainsi que les applications principales. La plate-forme eHealth poursuit 3 objectifs majeurs : optimaliser la qualité et la continuité des prestations de soins de santé de même que la sécurité du patient, promouvoir la simplification des formalités administratives pour tous les acteurs de santé, dot entre autres les prestataires et établissements de soins et enfin soutenir la politique en matière de santé. Les droits et obligations de la plate-forme eHealth ainsi que les modes de gestion de cette plate-forme sont également détaillés dans ce second chapitre

Published
2010

10. Les attentes des salariés de la région Nord- Pas de Calais en matière d’ARTT: synthèse et conclusions

Author

Cordonnier, L., Henguelle, Valérie, Jacobe, F., Lammens, L., Mauroy, H., Université d'Artois (UA), and Justin-Labonne, Virginie

Subjects
[SHS.GESTION]Humanities and Social Sciences/Business administration, [SHS] Humanities and Social Sciences, [SHS.GESTION] Humanities and Social Sciences/Business administration, ComputingMilieux_MISCELLANEOUS, [SHS]Humanities and Social Sciences
Abstract

International audience

Published
1997

11. Les préférences des salariés de la région Nord- Pas de Calais en matière d’aménagement et de réduction du temps de travail

Author

Cordonnier, L., Henguelle, Valérie, Jacobe, F., Lammens, L., Mauroy, H., Centre Lillois d’Études et de Recherches Sociologiques et Économiques - UMR 8019 (CLERSÉ), Université de Lille-Centre National de la Recherche Scientifique (CNRS), Conseil général Nord Pas de Calais, CLERSE, and Centre National de la Recherche Scientifique (CNRS)-Université de Lille

Subjects
[SHS]Humanities and Social Sciences
Published
1997

15. Impact of gavage dosing procedure and gastric content on adverse respiratory effects and mortality in rat toxicity studies

Author

Eichenbaum, G., primary, Damsch, S., additional, Looszova, A., additional, Vandenberghe, J., additional, Van den Bulck, K., additional, Roels, K., additional, Megens, A., additional, Knight, E., additional, Hillsamer, V., additional, Feyen, B., additional, Kelley, M. F., additional, Tonelli, A., additional, and Lammens, L., additional

Published
2010
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17. Miscellaneous

Author

De Jonghe, S., primary, Lammens, L., additional, Raoof, A., additional, Steemans, K., additional, Broeckaert, F., additional, Verbeeck, J., additional, Van Goethem, F., additional, and Hanton, G., additional

Published
2009
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21. Impact of gavage dosing procedure and gastric content on adverse respiratory effects and mortality in rat toxicity studies.

Author

Eichenbaum, G., Damsch, S., Looszova, A., Vandenberghe, J., Van den Bulck, K., Roels, K., Megens, A., Knight, E., Hillsamer, V., Feyen, B., Kelley, M. F., Tonelli, A., and Lammens, L.

Subjects
DRUG toxicity, TUBE feeding complications, LABORATORY rats, GASTROESOPHAGEAL reflux, NASOPHARYNX, GASTRIC acid
Abstract

Unscheduled mortality preceded by adverse respiratory clinical signs in rats dosed by oral gavage may not only be caused by technical gavage error or systemic toxicity but may also be caused by gastro-esophageal reflux and subsequent aspiration of high concentrations of drug formulation. In a 3 week oral gavage rat toxicity study for an early drug development compound, preterminal deaths (approximately 20% of animals) at high doses (≥1000 mg kg) and concentrations (≥60 mg ml) were preceded by recurrent dyspnea, rales or excessive salivation, without evidence of accidental intrapulmonary gavage error. Histological evaluation revealed extensive necrosis and inflammatory changes in the upper respiratory tract, especially in the nasal turbinates and/or nasopharynx. The presence of food particles in inflammatory exudates suggested a retrograde aspiration of stomach content with test formulation via the nasopharyngeal duct into the posterior region of the nose. In contrast, no mortality or adverse respiratory effects were observed in rats following 2 week intravenous administration at comparable exposures or oral gavage administration at lower concentrations (≤20 mg ml). In a pharmacology study, the compound caused a dose-dependent increase in gastric content (partly due to inhibition of gastric emptying), providing a pharmacological basis for the suspected gavage-mediated gastroesophageal reflux. Reducing the dose volume and dosing fasted animals substantially reduced or eliminated the respiratory effects and mortality at the high test article concentrations, demonstrating that the adverse effects are related to the gavage method. Copyright © 2010 John Wiley & Sons, Ltd. Unscheduled mortality preceded by adverse respiratory clinical signs in rats dosed by oral gavage may not only be caused by technical gavage error or systemic toxicity but may also be caused by gastro-esophageal reflux and subsequent aspiration of high concentrations of drug formulation. Reducing the dose volume and dosing fasted animals may substantially reduce or eliminated the respiratory effects and mortality at the high test article concentrations, demonstrating that the adverse effects are related to the gavage method and reflux. [ABSTRACT FROM AUTHOR]

Published
2011
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26. Miscellaneous: P17: Lethal rhinitis/sinusitis in rodents by aspiration of formulation in gavage studies: Importance of evaluation of the nose.

Author

De Jonghe, S., Lammens, L., Raoof, A., Steemans, K., Broeckaert, F., Verbeeck, J., Van Goethem, F., and Hanton, G.

Subjects
HUMAN life cycle, DEAD bodies (Law), GIFTS causa mortis, INHERITANCE & succession
Abstract

For repeated dose oral gavage studies in rodents, OECD guidelines do not include the nasal turbinates in the list of recommended tissues for histopathologic examination. During the past few years, unexpected high mortality was noted with two different compounds in rodents for which the cause of death was mainly based on histological evaluation of the nose. For compound A (a solution in PEG 400), unexpected high mortality was encountered early in the carcinogenicity studies. The dose-related increase in mortality correlated with an increase in inflammatory and necrotic or ulcerative changes within the respiratory tract of the preterminal deaths, often involving the nose and sinuses. For several animals rhinitis/sinusitis (mainly involving the lower half of the nose and most prominently affecting the respiratory epithelium) was the most important finding. The respiratory tract findings were consistent with irritation. The irritant nature of the formulation was confirmed in a BCOP-test. It was concluded that a part of the irritant formulation entered into the nose/airways via aspiration during gavage-dosing. This was considered to be related to the high viscosity of the vehicle (PEG400). The problem was further prevented by adapting the gavage procedure and by reducing the volume and/or concentration of the formulation. Compound B (also a solution in PEG 400) resulted in high mortality at the high dose in the 3m mouse study, from the 1st week onwards. At necropsy, the preterminally dead/sacrificed animals showed gastrointestinal dilatation with test formulation being present in the stomach. Acute, necrotizing rhinitis/sinusitis was the cause of death for the majority of these mice. Only a minority of these animals showed lesions in other parts of the respiratory tract. The test article and PEG 400 (to a lesser extent) were demonstrated to delay gastric emptying in a separate pharmacology study. This effect, together with the high viscosity of the vehicle and the irritant nature of the compound formulation resulted in entry of the formulation in the respiratory tract (probably due to regurgitation/aspiration) with subsequent inflammatory/necrotizing changes. For the majority of mice, the cause of death would not have been evident without evaluation of the nose. In conclusion, evaluation of the nose can be valuable to determine the cause of death in rodents. [Copyright &y& Elsevier]

Published
2009
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27. Spiro-Azetidine Oxindoles as Long-Acting Injectables for Pre-Exposure Prophylaxis against Respiratory Syncytial Virus Infections.

Author

Kesteleyn B, Herschke F, Darville N, Stoops B, Jacobs T, Jacoby E, Shaffer P, Lammens L, Van Rompaey D, Matcha K, Martinez Lamenca C, Coesemans E, Hache G, Pieters S, Lecomte M, Hu L, Demin S, Milligan C, Abeywickrema P, De Bruyn S, Van Den Berg J, Ysebaert N, De Zwart L, Nájera I, Rigaux P, Roymans D, and Jonckers THM

Subjects
Humans, Animals, Pre-Exposure Prophylaxis methods, Injections, Intramuscular, Indoles chemistry, Indoles administration & dosage, Indoles pharmacology, Injections, Subcutaneous, Respiratory Syncytial Virus, Human drug effects, Virus Internalization drug effects, Respiratory Syncytial Virus Infections prevention & control, Respiratory Syncytial Virus Infections drug therapy, Oxindoles chemistry, Oxindoles pharmacology, Spiro Compounds chemistry, Spiro Compounds pharmacology, Spiro Compounds pharmacokinetics, Spiro Compounds administration & dosage, Antiviral Agents pharmacology, Antiviral Agents chemistry, Antiviral Agents administration & dosage, Azetidines chemistry, Azetidines pharmacology, Azetidines administration & dosage, Azetidines pharmacokinetics
Abstract

Respiratory syncytial virus (RSV) is a major cause of hospitalization in infants, the elderly, and immune-compromised patients. While a half-life extended monoclonal antibody and 2 vaccines have recently been approved for infants and the elderly, respectively, options to prevent disease in immune-compromised patients are still needed. Here, we describe spiro-azetidine oxindoles as small molecule RSV entry inhibitors displaying favorable potency, developability attributes, and long-acting PK when injected as an aqueous suspension, suggesting their potential to prevent complications following RSV infection over a period of 3 to 6 months with 1 or 2 long-acting intramuscular (IM) or subcutaneous (SC) injections in these immune-compromised patients.

Published
2024
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28. Homeostasis, injury, and recovery dynamics at multiple scales in a self-organizing mouse intestinal crypt.

Author

Gall L, Duckworth C, Jardi F, Lammens L, Parker A, Bianco A, Kimko H, Pritchard DM, and Pin C

Subjects
Mice, Animals, Cell Proliferation physiology, Cell Differentiation physiology, Homeostasis physiology, Intestines, Intestinal Mucosa metabolism
Abstract

The maintenance of the functional integrity of the intestinal epithelium requires a tight coordination between cell production, migration, and shedding along the crypt-villus axis. Dysregulation of these processes may result in loss of the intestinal barrier and disease. With the aim of generating a more complete and integrated understanding of how the epithelium maintains homeostasis and recovers after injury, we have built a multi-scale agent-based model (ABM) of the mouse intestinal epithelium. We demonstrate that stable, self-organizing behaviour in the crypt emerges from the dynamic interaction of multiple signalling pathways, such as Wnt, Notch, BMP, ZNRF3/RNF43, and YAP-Hippo pathways, which regulate proliferation and differentiation, respond to environmental mechanical cues, form feedback mechanisms, and modulate the dynamics of the cell cycle protein network. The model recapitulates the crypt phenotype reported after persistent stem cell ablation and after the inhibition of the CDK1 cycle protein. Moreover, we simulated 5-fluorouracil (5-FU)-induced toxicity at multiple scales starting from DNA and RNA damage, which disrupts the cell cycle, cell signalling, proliferation, differentiation, and migration and leads to loss of barrier integrity. During recovery, our in silico crypt regenerates its structure in a self-organizing, dynamic fashion driven by dedifferentiation and enhanced by negative feedback loops. Thus, the model enables the simulation of xenobiotic-, in particular chemotherapy-, induced mechanisms of intestinal toxicity and epithelial recovery. Overall, we present a systems model able to simulate the disruption of molecular events and its impact across multiple levels of epithelial organization and demonstrate its application to epithelial research and drug development., Competing Interests: LG, AB, HK, CP Employee and shareholder of AstraZeneca Plc, CD, AP, DP No competing interests declared, FJ Employee of Johnson & Johnson, LL Employee and shareholder of Johnson & Johnson, (© 2023, Gall et al.)

Published
2023
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29. A dynamic model of the intestinal epithelium integrates multiple sources of preclinical data and enables clinical translation of drug-induced toxicity.

Author

Gall L, Jardi F, Lammens L, Piñero J, Souza TM, Rodrigues D, Jennen DGJ, de Kok TM, Coyle L, Chung SW, Ferreira S, Jo H, Beattie KA, Kelly C, Duckworth CA, Pritchard DM, and Pin C

Subjects
Mice, Humans, Animals, Fluorouracil toxicity, Fluorouracil metabolism, Intestinal Mucosa metabolism, Diarrhea chemically induced, Doxorubicin toxicity, Citrulline, Drug-Related Side Effects and Adverse Reactions
Abstract

We have built a quantitative systems toxicology modeling framework focused on the early prediction of oncotherapeutic-induced clinical intestinal adverse effects. The model describes stem and progenitor cell dynamics in the small intestinal epithelium and integrates heterogeneous epithelial-related processes, such as transcriptional profiles, citrulline kinetics, and probability of diarrhea. We fitted a mouse-specific version of the model to quantify doxorubicin and 5-fluorouracil (5-FU)-induced toxicity, which included pharmacokinetics and 5-FU metabolism and assumed that both drugs led to cell cycle arrest and apoptosis in stem cells and proliferative progenitors. The model successfully recapitulated observations in mice regarding dose-dependent disruption of proliferation which could lead to villus shortening, decrease of circulating citrulline, increased diarrhea risk, and transcriptional induction of the p53 pathway. Using a human-specific epithelial model, we translated the cytotoxic activity of doxorubicin and 5-FU quantified in mice into human intestinal injury and predicted with accuracy clinical diarrhea incidence. However, for gefitinib, a specific-molecularly targeted therapy, the mice failed to reproduce epithelial toxicity at exposures much higher than those associated with clinical diarrhea. This indicates that, regardless of the translational modeling approach, preclinical experimental settings have to be suitable to quantify drug-induced clinical toxicity with precision at the structural scale of the model. Our work demonstrates the usefulness of translational models at early stages of the drug development pipeline to predict clinical toxicity and highlights the importance of understanding cross-settings differences in toxicity when building these approaches., (© 2023 The Authors. CPT: Pharmacometrics & Systems Pharmacology published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published
2023
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30. Safety, Tolerability, and Pharmacokinetics of JNJ-1802, a Pan-serotype Dengue Direct Antiviral Small Molecule, in a Phase 1, Double-Blind, Randomized, Dose-Escalation Study in Healthy Volunteers.

Author

Ackaert O, Vanhoutte F, Verpoorten N, Buelens A, Lachau-Durand S, Lammens L, Hoetelmans R, Van Loock M, and Herrera-Taracena G

Subjects
Humans, Area Under Curve, Dose-Response Relationship, Drug, Double-Blind Method, Healthy Volunteers, Serogroup, Adolescent, Young Adult, Adult, Middle Aged, Antiviral Agents pharmacokinetics, Dengue drug therapy
Abstract

Background: Dengue is a growing global health threat with no specific antiviral drugs available for treatment or prophylaxis. This first-in-human, double-blind, randomized, placebo-controlled study aimed to examine the safety, tolerability, and pharmacokinetics of increasing single and multiple oral doses of JNJ-1802, a pan-serotype dengue antiviral small molecule., Methods: Eligible healthy participants (18-55 years of age) were randomized to receive oral JNJ-1802 in fasted conditions as (1) single doses (50-1200 mg; n = 29) or placebo (n = 10); or (2) once-daily doses (50-560 mg for 10 consecutive days or 400 mg for 31 days; n = 38) or placebo (n = 9). Safety and tolerability were evaluated throughout the study. Plasma and urine samples were collected at predetermined time points to characterize pharmacokinetics., Results: JNJ-1802 was generally safe and well-tolerated. One grade 3 adverse event (depression) was reported but not considered drug-related by the investigator. Two grade 2 events of rash occurred (multiple-dose part) that were considered very likely related to JNJ-1802 by the investigator and resolved. No clinically relevant changes were observed in laboratory tests, electrocardiograms, or vital signs.JNJ-1802 exposure after single or multiple doses increased dose-proportionally from 50 to 150 mg and less than dose-proportionally for higher doses. The terminal elimination half-life was 6.3-9.2 days and the accumulation factor was 4.3-7.3 after 10 days and 14.6 after 31 days with low amounts of unchanged drug in urine (<0.001% of the 400 mg dose)., Conclusions: Pharmacokinetics and safety results of JNJ-1802 support further clinical development for the treatment and prevention of dengue infection., Competing Interests: Potential conflicts of interest. O. A., S. L.-D., L. L., R. H., G. H.-T., M. V. L., and A. B. are all full-time employees of Janssen and potential stockholders of Johnson & Johnson. F. V. potentially owns shares from Johnson & Johnson as part of his past employee remuneration. M. V. L., O. A., and G. H.-T. have been named inventors in pending patent applications (M. V. L. and G. H.-T.: Janssen Pharmaceuticals and Katholieke Universiteit Leuven). N. V. reports no potential conflicts. All authors have submitted the ICMJE Form for Disclosure of Potential Conflicts of Interest. Conflicts that the editors consider relevant to the content of the manuscript have been disclosed., (© The Author(s) 2023. Published by Oxford University Press on behalf of Infectious Diseases Society of America.)

Published
2023
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31. Impact of heavy metal exposure on biological control of a deadly amphibian pathogen by zooplankton.

Author

Deknock A, Pasmans F, van Leeuwenberg R, Van Praet S, De Troyer N, Goessens T, Lammens L, Bruneel S, Lens L, Martel A, Croubels S, and Goethals P

Subjects
Amphibians, Animals, Ecosystem, Zooplankton, Chytridiomycota, Metals, Heavy toxicity
Abstract

Despite devastating effects on global biodiversity, efficient mitigation strategies against amphibian chytridiomycosis are lacking. Since the free-living pathogenic zoospores of Batrachochytrium dendrobatidis (Bd), the infective stage of this disease, can serve as a nutritious food source for components of zooplankton communities, these groups may act as biological control agents by eliminating zoospores from the aquatic environment. Such pathogen-predator interaction is, however, embedded in the aquatic food web structure and is therefore affected by abiotic factors interfering with these networks. Heavy metals, released from both natural and anthropogenic sources, are widespread contaminants of aquatic ecosystems and may interfere with planktonic communities and thus pathogen elimination rates. We investigated the interaction between zooplankton communities and chytridiomycosis infections in a Flemish agricultural region. Moreover, we also investigated the impact of heavy metal contamination, that was previously investigated in the region and presented in recent work, on zooplankton assemblages and chytridiomycosis infections. Finally, we tested the effect of sublethal concentrations of copper and zinc on Bd removal rates by Daphnia magna in a laboratory assay. Although zinc, copper, nickel and chromium were widely abundant pollutants, heavy metals were no driving force for zooplankton assemblages at our study locations. Moreover, our field survey did not reveal indirect effects of zooplankton assemblages on chytridiomycosis infections. However, sampling occasions testing negative for Bd showed a higher degree of copper contamination compared to positive sampling occasions, indicating a potential inhibitory effect of copper on Bd prevalence. Finally, whereas D. magna significantly reduced zoospore densities in its environment, sublethal concentrations of copper and zinc showed no interference with pathogen removal in the laboratory assay. Our results provide perspectives for further research on such a biological control strategy against chytridiomycosis by optimizing environmental conditions for pathogen predation., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published
2022
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32. JNJ-67569762, A 2-Aminotetrahydropyridine-Based Selective BACE1 Inhibitor Targeting the S3 Pocket: From Discovery to Clinical Candidate.

Author

Rombouts FJR, Kusakabe KI, Alexander R, Austin N, Borghys H, De Cleyn M, Dhuyvetter D, Gijsen HJM, Hrupka B, Jacobs T, Jerhaoui S, Lammens L, Leclercq L, Tsubone K, Ueno T, Morimoto K, Einaru S, Sumiyoshi H, Van den Bergh A, Vos A, Surkyn M, Teisman A, and Moechars D

Subjects
Amyloid Precursor Protein Secretases metabolism, Aspartic Acid Endopeptidases metabolism, Crystallography, X-Ray, Dose-Response Relationship, Drug, Humans, Models, Molecular, Molecular Structure, Pyrrolidines chemical synthesis, Pyrrolidines chemistry, Structure-Activity Relationship, Amyloid Precursor Protein Secretases antagonists & inhibitors, Aspartic Acid Endopeptidases antagonists & inhibitors, Drug Discovery, Pyrrolidines pharmacology
Abstract

The discovery of a novel 2-aminotetrahydropyridine class of BACE1 inhibitors is described. Their pK a and lipophilicity were modulated by a pending sulfonyl group, while good permeability and brain penetration were achieved via intramolecular hydrogen bonding. BACE1 selectivity over BACE2 was achieved in the S3 pocket by a novel bicyclic ring system. An optimization addressing reactive metabolite formation, cardiovascular safety, and CNS toxicity is described, leading to the clinical candidate JNJ-67569762 ( 12 ), which gave robust dose-dependent BACE1-mediated amyloid β lowering without showing BACE2-dependent hair depigmentation in preclinical models. We show that 12 has a favorable projected human dose and PK and hence presented us with an opportunity to test a highly selective BACE1 inhibitor in humans. However, 12 was found to have a QT effect upon repeat dosing in dogs and its development was halted in favor of other selective leads, which will be reported in the future.

Published
2021
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33. Application of Disinfectants for Environmental Control of a Lethal Amphibian Pathogen.

Author

Lammens L, Martel A, and Pasmans F

Abstract

Chytridiomycosis is an emerging infectious disease threatening amphibian populations worldwide. While environmental disinfection is important in mitigating the disease, successful elimination of Batrachochytrium dendrobatidis (Bd) without excessively harming ecosystems is challenging. We selected peracetic acid (PAA) as the most potent of six commercially available products regarding their ability to inhibit growth of a highly virulent Bd strain. PAA killed Bd after 5 min of exposure to approximately 94.7 mg/L. We examined the toxicity of PAA against three invertebrate species and Discoglossus pictus tadpoles. 93% of invertebrates, but none of the tadpoles survived 5 min of exposure to 94.7 mg/L. Tadpoles showed no adverse effects after 5 min exposure to concentrations of approximately 37.9 mg/L or lower. Addition of PAA to aquatic microcosms decreased pH, while dissolved oxygen (DO) initially increased. Degradation of PAA reversed the pH drop, but caused a massive drop in DO, which could be remedied by aeration. As proof of concept, microcosms that were aerated and treated with 94.7 mg/L PAA sustained survival of tadpoles starting 48 h after treatment. Disinfecting aquatic environments using PAA could contribute to mitigating chytridiomycosis, while preserving at least some invertebrate diversity, but requires temporary removal of resident amphibians.

Published
2021
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34. Preclinical toxicity and pharmacokinetics of a new orally bioavailable flubendazole formulation and the impact for clinical trials and risk/benefit to patients.

Author

Lachau-Durand S, Lammens L, van der Leede BJ, Van Gompel J, Bailey G, Engelen M, and Lampo A

Subjects
Administration, Oral, Animals, Antinematodal Agents administration & dosage, Dogs, Drug Evaluation, Preclinical, Female, Gerbillinae, Male, Mebendazole administration & dosage, Mebendazole adverse effects, Mebendazole pharmacokinetics, Rats, Sprague-Dawley, Antinematodal Agents adverse effects, Antinematodal Agents pharmacokinetics, Mebendazole analogs & derivatives, Mutagenicity Tests
Abstract

Background: Flubendazole, originally developed to treat infections with intestinal nematodes, has been shown to be efficacious in animal models of filarial infections. For treatment of filarial nematodes, systemic exposure is needed. For this purpose, an orally bioavailable amorphous solid dispersion (ASD) formulation of flubendazole was developed. As this formulation results in improved systemic absorption, the pharmacokinetic and toxicological profile of the flubendazole ASD formulation have been assessed to ensure human safety before clinical trials could be initiated., Methods & Findings: Safety pharmacology, toxicity and genotoxicity studies have been conducted with the flubendazole ASD formulation. In animals, flubendazole has good oral bioavailability from an ASD formulation ranging from 15% in dogs, 27% in rats to more than 100% in jirds. In in vivo toxicity studies with the ASD formulation, high systemic exposure to flubendazole and its main metabolites was reached. Flubendazole, up to high peak plasma concentrations, does not induce Cmax related effects in CNS or cardiovascular system. In repeated dose toxicity studies in rats and dogs, flubendazole-induced changes were observed in haematological, lymphoid and gastrointestinal systems and in testes. In dogs, the liver was an additional target organ. Upon treatment cessation, at least partial recovery was observed for these changes in dogs. In rats, the No Observed Adverse Effect Level (NOAEL) was 5 mg (as base)/kg body weight/day (mg eq./kg/day) in males and 2.5 mg eq./kg/day in females. In dogs, the NOAEL was lower than 20 mg eq./kg/day. Regarding genotoxicity, flubendazole was negative in the Ames test, but positive in the in vivo micronucleus test., Conclusions: Based on these results, in combination with previously described genotoxicity and reproductive toxicity data and the outcome of the preclinical efficacy studies, it was concluded that no flubendazole treatment regimen can be selected that would provide efficacy in humans at safe exposure., Competing Interests: I have read the journal's policy and the authors of this manuscript have the following competing interests: ownership of stocks or shares of Johnson & Johnson. All authors are employees of Johnson & Johnson.

Published
2019
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35. Translational safety biomarkers of colonic barrier integrity in the rat.

Author

Erkens T, Bueters R, van Heerden M, Cuyckens F, Vreeken R, Goeminne N, and Lammens L

Subjects
Animals, Biomarkers blood, Biomarkers urine, Colon metabolism, Colon pathology, Feces chemistry, Intestinal Mucosa metabolism, Intestinal Mucosa pathology, Male, Permeability, Rats, Sprague-Dawley, Translational Research, Biomedical, Biomarkers analysis, Colon drug effects, Decanoic Acids toxicity, Ibuprofen toxicity, Intestinal Mucosa drug effects
Abstract

The intestinal barrier controls intestinal permeability, and its disruption has been associated with multiple diseases. Therefore, preclinical safety biomarkers monitoring barrier integrity are essential during the development of drugs targeting the intestines, particularly if starting treatment early after onset of disease. Classical toxicology endpoints are not sensitive enough and therefore our objective was to identify non-invasive markers enabling early in vivo detection of colonic barrier perturbation. Male Sprague-Dawley rats were dosed intracolonically via the rectum, using sodium caprate or ibuprofen as tool compounds to alter barrier integrity. Several potentially translational biomarkers and probe molecules related to permeability, inflammation or tissue damage were evaluated, using various analytical platforms, including immunoassays, targeted metabolomics and highly sensitive ultra-performance liquid chromatography-tandem mass spectrometry. Several markers were identified that allow early in vivo detection of colonic barrier integrity changes, before histopathological evidence of tissue damage. The most promising permeability markers identified were plasma fluorescein isothiocyanate-dextran 4000 and a lactulose/mannitol/sucralose mixture in urine. These markers showed maximum increases over 100-fold or approximately 10-50-fold, respectively. Intracolonic administration of the above probe molecules outperformed oral administration and inflammatory or other biomarkers, such as α 2 -macroglobulin, calprotectin, cytokines, prostaglandins and a panel of metabolic molecules to identify early and subtle changes in barrier integrity. However, optimal timing of probe administration and sample collection is important for all markers evaluated. Inclusion of these probe molecules in preclinical toxicity studies might aid in risk assessment and the design of a clinical biomarker plan, as several of these markers have translational potential., (Copyright © 2018 John Wiley & Sons, Ltd.)

Published
2018
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36. Grommet and adenoid pain evaluation (GRAPE) study.

Author

F L, J B, E M, K B, G L, J I, F I, W L, N L, F J, M J, and P L

Subjects
Child, Child, Preschool, Female, Humans, Infant, Male, Pain Measurement methods, Pain, Postoperative diagnosis, Acetaminophen therapeutic use, Adenoidectomy adverse effects, Adenoids surgery, Analgesics, Non-Narcotic therapeutic use, Middle Ear Ventilation adverse effects, Pain, Postoperative drug therapy
Abstract

In the GRAPE study an analysis is made of postoperative pain sensation in children between 6 months and 6 years after adenotomy and placement of ear grommets. Intraoperative treatment with paracetamol versus placebo shows no statistically significant difference in pain between both groups indicating that this type of surgery causes little discomfort and does not require specific intraoperative analgesic treatment., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published
2018
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37. Legacy data sharing to improve drug safety assessment: the eTOX project.

Author

Sanz F, Pognan F, Steger-Hartmann T, Díaz C, Cases M, Pastor M, Marc P, Wichard J, Briggs K, Watson DK, Kleinöder T, Yang C, Amberg A, Beaumont M, Brookes AJ, Brunak S, Cronin MTD, Ecker GF, Escher S, Greene N, Guzmán A, Hersey A, Jacques P, Lammens L, Mestres J, Muster W, Northeved H, Pinches M, Saiz J, Sajot N, Valencia A, van der Lei J, Vermeulen NPE, Vock E, Wolber G, and Zamora I

Subjects
Humans, Risk Assessment methods, Drug Evaluation, Preclinical methods, Drug Industry methods, Drug-Related Side Effects and Adverse Reactions, Information Dissemination
Abstract

The sharing of legacy preclinical safety data among pharmaceutical companies and its integration with other information sources offers unprecedented opportunities to improve the early assessment of drug safety. Here, we discuss the experience of the eTOX project, which was established through the Innovative Medicines Initiative to explore this possibility.

Published
2017
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38. Bilateral Symmetrical Idiopathic Necrotizing Encephalopathy: A New Syndrome in Sprague-Dawley Rats.

Author

De Jonghe S, Abbott D, Vinken P, Moesen E, Feyen B, Lammens L, Vynckier A, and De Lahunta A

Subjects
Animals, Brain drug effects, Brain pathology, Female, Male, Rats, Rats, Sprague-Dawley, Toxicity Tests, Brain Diseases veterinary, Brain Infarction veterinary, Necrosis veterinary
Abstract

This article describes the occurrence of a bilaterally symmetrical encephalopathy in Sprague-Dawley rats, which occurred over the period 2005 to 2012 in our laboratory in both untreated control rats and rats treated with different pharmacologically active compounds. The acute brain lesions consisted of degeneration/necrosis in the ventral areas of the brain mostly with little inflammatory response; in the more rare chronic cases there were numerous lipid-laden macrophages. The areas most consistently affected were the crus cerebri, the ventral midbrain, the pyramids, and the internal capsule. Other areas less frequently affected were the mammillary bodies, the fimbria, the olfactory tubercles, the optic tracts, and the ventral hippocampus. All available data, including clinical signs, gross pathology, clinical pathology, diet, breeding, and housing were collected and are presented. Our investigations did not elucidate the pathogenesis of the lesions, although the infarction-type changes are suggestive of a vascular etiology. To our knowledge, this particular lesion with its consistent distribution pattern has not been reported in the rat literature and its publication is therefore important to the toxicological pathology community, because an unbalanced group distribution in a toxicology study could potentially confound the safety assessment of a compound., (© 2015 by The Author(s).)

Published
2015
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39. Juvenile animal testing of hydroxypropyl-β-cyclodextrin in support of pediatric drug development.

Author

De Schaepdrijver L, Mariën D, Rhimi C, Voets M, van Heerden M, and Lammens L

Subjects
2-Hydroxypropyl-beta-cyclodextrin, Administration, Oral, Age Factors, Animals, Excipients administration & dosage, Excipients pharmacokinetics, Humans, Infant, Infant, Newborn, Injections, Intravenous, Kidney growth & development, Kidney metabolism, Metabolic Clearance Rate, Models, Animal, Rats, Sprague-Dawley, Renal Elimination, Risk Assessment, Species Specificity, beta-Cyclodextrins administration & dosage, beta-Cyclodextrins pharmacokinetics, Excipients toxicity, Toxicity Tests methods, beta-Cyclodextrins toxicity
Abstract

Hydroxypropyl-β-cyclodextrin (HP-β-CD) is being explored as excipient for administration of poorly soluble NCE's in pediatrics. In support of pharmaceutical development, non-clinical studies were performed to investigate whether oral and intravenous administration of HP-β-CD showed a different response in juvenile rats versus adult rats. Juvenile rats received HP-β-CD via the intravenous route at dose levels of 50, 200 and 400mg/kg/day from postnatal day 16 to 44, or via oral gavage at 500, 1000 and 2000mg/kg/day from postnatal day 4 to 46. In addition to in vivo parameters, toxicokinetics and post-mortem evaluations were conducted. The main findings were related to the renal excretion of intact HP-β-CD and were regarded as non-adverse transient adaptive responses. The pathogenesis of the osmotic nephrosis-like changes are discussed. With increasing age a more effective renal clearance of HP-β-CD is present in line with the postnatal functional maturation of the kidney. In addition, following oral administration an increase in soft stools was seen which was related to osmotic water retention in the large intestine. The findings in the juvenile studies are very similar to those observed in previously performed adult rat studies at similar dose levels, same routes and similar or longer dose duration. No novel toxicity was seen in the juvenile studies., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published
2015
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40. Evaluation of miR-122 and other biomarkers in distinct acute liver injury in rats.

Author

Starckx S, Batheja A, Verheyen GR, Jonghe SD, Steemans K, Dijck BV, Singer M, Bogdan N, Snoeys J, Vinken P, Sasaki JC, Gompel JV, Guzzie-Peck P, Lampo A, and Lammens L

Subjects
Acetaminophen toxicity, Animals, Biomarkers blood, Chemical and Drug Induced Liver Injury genetics, Chemical and Drug Induced Liver Injury pathology, Isocyanates toxicity, Liver chemistry, Liver pathology, Male, Naphthalenes toxicity, Propanols toxicity, Rats, Rats, Sprague-Dawley, Toxicity Tests, Acute, Chemical and Drug Induced Liver Injury blood, MicroRNAs blood
Abstract

The detection of drug-induced hepatotoxicity remains an important safety issue in drug development. A liver-specific microRNA species, microRNA-122 (miR-122), has recently shown potential for predicting liver injury in addition to the standard hepatic injury biomarkers. The objective of this study was to measure miR-122 together with several other liver markers in distinct settings of acute liver toxicity in rats to determine the value of miR-122 as a biomarker for liver injury in this species. Rats were exposed to 3 well-established liver toxicants (acetaminophen, allyl alcohol, and α-naphthyl isothiocyanate), a liver-enzyme inducer (phenobarbital), or a cardiotoxicant (doxorubicin). There was a clear increase in plasma miR-122 following administration of acetaminophen, allyl alcohol, and α-naphthyl isothiocyanate. The response of miR-122 paralleled that of other markers and was consistent with liver injury as indicated by histopathological evaluation. Furthermore, the changes in miR-122 were detected earlier than standard liver injury markers and exhibited a wide dynamic range. In contrast, miR-122 responses to phenobarbital and doxorubicin were low. Based on these findings, miR-122 shows significant promise and may provide added value for assessing liver toxicity in drug development.

Published
2013
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41. Mechanistic investigations on the etiology of Risperdal(®) Consta(®)-induced bone changes in female Wistar Hannover rats.

Author

de Waal EJ, Roosen W, Vinken P, Vandenberghe J, Sterkens P, and Lammens L

Subjects
Absorptiometry, Photon, Alkaline Phosphatase blood, Animals, Antipsychotic Agents toxicity, Bone Diseases blood, Bone Diseases pathology, Calcitonin blood, Collagen Type I blood, Female, Femur drug effects, Femur pathology, Follicle Stimulating Hormone blood, Luteinizing Hormone blood, Osteocalcin blood, Parathyroid Hormone blood, Peptides blood, Prolactin blood, Random Allocation, Rats, Rats, Wistar, Risperidone toxicity, Thyroid Hormones blood, Tibia drug effects, Tibia pathology, Tomography, X-Ray Computed, Antipsychotic Agents pharmacology, Bone Density drug effects, Bone Diseases chemically induced, Risperidone pharmacology
Abstract

RISPERDAL(®) CONSTA(®) is a long-acting, intramuscular formulation of risperidone microspheres for the biweekly treatment of schizophrenia and other psychiatric disorders. In a 24-month carcinogenicity study male and female Wistar Hannover rats received RISPERDAL(®) CONSTA(®) by intramuscular injection at dosages of 5 or 40 mg/kg once every 2 weeks. Bone changes described as "osteodystrophy" were observed by routine microscopic examination at 40 mg/kg in the sternum of female rats after 12 months, and in the sternum and stifle joint of both male and female rats after 24 months of treatment, respectively. To investigate the etiology of these bone changes, a 12-month mechanistic study was conducted in female Wistar Hannover rats at dosages of 5, 20 and 40 mg/kg once every 2 weeks. In addition to routine parameters, this study included bone markers, hormone measurements, and peripheral quantitative computed tomography (pQCT) and dual-energy X-ray absorptiometry (DXA) bone density measurements. It revealed a treatment-related reduction in metaphyseal trabecular bone density of the femur and tibia at 20 and 40 mg/kg, which was evident in the tibia from Week 13 of treatment onwards. There was no convincing evidence for any of the modes of action known to underlie trabecular bone loss in rats including renal, nutritional, or hepatic osteodystrophy, estrogen deficiency, hyperthyroidism or glucocorticoid excess. It is hypothetized that prolonged hyperprolactinemia accompanied by an increase in parathyroid hormone-related protein (PTHrP) levels and a slight hypoestrogenic state could have caused the reduced trabecular bone density in RISPERDAL(®) CONSTA(®)-treated rats. The relevance of this finding in terms of human risk is unknown., (Copyright © 2012 Elsevier Ireland Ltd. All rights reserved.)

Published
2012
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42. Phospholipidosis in rats treated with amiodarone: serum biochemistry and whole genome micro-array analysis supporting the lipid traffic jam hypothesis and the subsequent rise of the biomarker BMP.

Author

Mesens N, Desmidt M, Verheyen GR, Starckx S, Damsch S, De Vries R, Verhemeldonck M, Van Gompel J, Lampo A, and Lammens L

Subjects
Animals, Biomarkers blood, Biomarkers urine, Cholesterol blood, Gene Expression Regulation, Glycerophospholipids blood, Glycerophospholipids metabolism, Lipidoses blood, Lipidoses urine, Liver pathology, Lung pathology, Lymphocytes drug effects, Lymphocytes pathology, Male, Metabolic Networks and Pathways drug effects, Oligonucleotide Array Sequence Analysis, Organ Size drug effects, Phospholipids blood, Rats, Rats, Sprague-Dawley, Spleen pathology, Toxicogenetics, Amiodarone toxicity, Lipid Metabolism drug effects, Lipidoses chemically induced, Lysophospholipids blood, Lysophospholipids urine
Abstract

To provide mechanistic insight in the induction of phospholipidosis and the appearance of the proposed biomarker di-docosahexaenoyl (C22:6)-bis(monoacylglycerol) phosphate (BMP), rats were treated with 150 mg/kg amiodarone for 12 consecutive days and analyzed at three different time points (day 4, 9, and 12). Biochemical analysis of the serum revealed a significant increase in cholesterol and phospholipids at the three time points. Bio-analysis on the serum and urine detected a time-dependent increase in BMP, as high as 10-fold compared to vehicle-treated animals on day 12. Paralleling these increases, micro-array analysis on the liver of treated rats identified cholesterol biosynthesis and glycerophospholipid metabolism as highly modulated pathways. This modulation indicates that during phospholipidosis-induction interactions take place between the cationic amphiphilic drug and phospholipids at the level of BMP-rich internal membranes of endosomes, impeding cholesterol sorting and leading to an accumulation of internal membranes, converting into multilamellar bodies. This process shows analogy to Niemann-Pick disease type C (NPC). Whereas the NPC-induced lipid traffic jam is situated at the cholesterol sorting proteins NPC1 and NPC2, the amiodarone-induced traffic jam is thought to be located at the BMP level, demonstrating its role in the mechanism of phospholipidosis-induction and its significance for use as a biomarker.

Published
2012
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43. Ethnic differences in diabetes-related mortality in the Brussels-Capital Region (2001-05): the role of socioeconomic position.

Author

Vandenheede H, Lammens L, Deboosere P, Gadeyne S, and De Spiegelaere M

Subjects
Adult, Africa, Northern ethnology, Aged, Belgium ethnology, Censuses, Educational Status, Female, Housing, Humans, Male, Middle Aged, Registries, Social Class, Diabetes Mellitus mortality, Ethnicity statistics & numerical data
Abstract

Objectives: To examine if and to what extent ethnic differences in diabetes-related mortality are associated with differences in education and housing status., Methods: The data consist of a cohort study linking the 2001 census to emigration and mortality data for the period 2001-05. The study population comprises all Belgian and North African inhabitants of the Brussels-Capital Region (BCR) aged 25-74. Age-standardized mortality rates (ASMRs) (direct standardization) and mortality rate ratios (MRRS) (Poisson regression) are computed., Results: North Africans have a higher diabetes-related mortality compared to Belgians. The ASMRs for North African and Belgian women are 54.8 (95% confidence interval (CI) 31.5-78.2) and 23.8 (95% CI 20.3-27.3), respectively. These differences in diabetes-related mortality largely disappear when differences in education are taken into account. The MRRs for North African versus Belgian origin drop from 1.62 (95% CI 1.11-2.37) to 1.19 (95% CI 0.73-1.93) in men and from 3.35 (95% CI 2.08-5.41) to 1.88 (95% CI 0.95-3.69) in women., Conclusions: Differences in education play an important part in the excess diabetes-related mortality among North Africans in the BCR.

Published
2011
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44. Zebrafish developmental toxicity assay: A fishy solution to reproductive toxicity screening, or just a red herring?

Author

Van den Bulck K, Hill A, Mesens N, Diekman H, De Schaepdrijver L, and Lammens L

Subjects
Animals, Body Burden, Congenital Abnormalities etiology, Dose-Response Relationship, Drug, Embryo, Nonmammalian abnormalities, Endpoint Determination, False Positive Reactions, Teratogens pharmacokinetics, Zebrafish abnormalities, Embryo, Nonmammalian drug effects, Embryonic Development drug effects, Teratogens toxicity, Toxicity Tests methods, Toxicity Tests standards, Toxicity Tests statistics & numerical data, Zebrafish embryology
Abstract

The zebrafish embryotoxicity/teratogenicity assay is described as a useful alternative screening model to evaluate the effect of drugs on embryofoetal development. Fertilized eggs were exposed to different concentrations of 15 compounds with teratogenic (8) and non-teratogenic (7) potential until 96h post-fertilization when 28 morphological endpoints and the level of compound uptake was assessed. The majority of drugs testing positive in mammals was also positive in zebrafish (75% sensitivity), while a relative high number of false positives were noted (43% specificity). Compound uptake determination appears useful for clarifying classifications as teratogenic or potential overdose although assay sensitivity could be improved to 71% if the exposure threshold, previously suggested as ∼50ng/larvae, is reconsidered. The zebrafish assay shows some potential, though limited in its current form, as a screening tool for developmental toxicity within Janssen drug development. Further assay refinement with respect to endpoints and body burden threshold is required., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published
2011
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45. Unexpected nasal changes in rats related to reflux after gavage dosing.

Author

Damsch S, Eichenbaum G, Looszova A, Lammens L, Feyen B, Van den Bulck K, Knight E, Kelley M, and Tonelli A

Subjects
Administration, Oral, Animals, Dose-Response Relationship, Drug, Gastric Emptying, Gastroesophageal Reflux metabolism, Male, Organ Size, Rats, Rats, Sprague-Dawley, Toxicity Tests, Dyspnea pathology, Enteral Nutrition adverse effects, Gastroesophageal Reflux pathology, Nasal Cavity pathology
Abstract

In a three-week oral gavage toxicity study in rats, a high incidence of respiratory symptoms and high mortality was noted in compound-dosed rats only. Because of audible respiration, an effect in the upper respiratory tract was suspected and the nasal cavity was included for examination. Histology revealed extensive necrosis and purulent inflammation within the nasal passages, indicative of direct irritation. Since posterior nasal regions were most affected, with food material present within the inflammatory exudates, reflux and retrograde aspiration of irritant material (possibly stomach contents with test formulation) into the nasal cavity were suspected. Lowering the dose volume and fasting the rats prior to gavage dosing substantially reduced the respiratory effects and mortality. The current article focuses on the histological changes in the nasal cavity indicative of gavage-related reflux and provides guidance on differentiation between technical gavage error and gavage-related reflux.

Published
2011
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46. Gavage-related reflux in rats: identification, pathogenesis, and toxicological implications (review).

Author

Damsch S, Eichenbaum G, Tonelli A, Lammens L, Van den Bulck K, Feyen B, Vandenberghe J, Megens A, Knight E, and Kelley M

Subjects
Administration, Oral, Animals, Dyspnea, Gastric Acid metabolism, Gastric Emptying, Gastroesophageal Reflux metabolism, Rats, Risk Factors, Enteral Nutrition adverse effects, Gastroesophageal Reflux pathology, Nasal Cavity pathology
Abstract

After oral gavage dosing of rats, reflux may occur, resulting in serious respiratory effects and mortality. Published information on gavage-related reflux is limited, as it has not yet been a focus of research. Nevertheless, it represents a recurrent challenge in daily toxicology practice of oral gavage dosing. The absence of clear guidance and criteria for the identification and management of reflux-induced effects can limit the ability to properly interpret toxicity study results. The review presented herein includes an overview of experimental data from gavage studies in rats, in which reflux was observed, and provides a comprehensive analysis of the literature on reflux in general and the different potential pathways contributing to gavage-related reflux in rats. The article aims to increase the awareness and understanding of the pathogenesis of gavage-related reflux and provides guidance on identification of potential risk factors, as well as interpretation of histological changes and their toxicological relevance. Furthermore, differentiation of reflux-induced effects from direct compound-related toxicity and from gavage errors is addressed in particular, and the importance of nasal histology is discussed.

Published
2011
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47. Real life juvenile toxicity case studies: the good, the bad and the ugly.

Author

De Schaepdrijver L, Rouan MC, Raoof A, Bailey GP, De Zwart L, Monbaliu J, Coogan TP, Lammens L, and Coussement W

Subjects
Age Factors, Animals, Animals, Laboratory, Child, Dogs, Humans, Mice, Pharmaceutical Preparations metabolism, Rats, United States, United States Food and Drug Administration, Drug Evaluation, Preclinical methods, Drug-Related Side Effects and Adverse Reactions, Pediatrics methods, Research Design legislation & jurisprudence, Toxicity Tests methods
Abstract

With the growing experience in the conduct of juvenile toxicity studies for multiple classes of compound, the 'case-by-case' approach has become under much more pressure. Instead, a general screen or 'standard design' is now commonly expected by regulatory authorities with more routine inclusion of neurological and reproductive assessments. Minor modifications or additions can be made to the design to address specific questions according to the class of drug or intended clinical use. This drift from a 'case-by-case' approach to a 'standard design' approach is present within certain reviewing divisions of the FDA, often requesting by default a rodent and non-rodent juvenile animal study. However, juvenile animal studies should be designed thoughtfully to fulfil a purpose based on scientific rationale, with each endpoint carefully considered in terms of practicality and interpretability of data generated. Only when using the appropriate strategy and design may juvenile studies add value by (1) identifying potential safety or pharmacokinetic issues for drugs intended for paediatric use, (2) suggesting additional clinical endpoints and (3) adding new information to the product label. As the knowledge from juvenile animal studies in various species grows, a better understanding of the significance/relevance of findings will be achieved.

Published
2008
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48. Hemorrhagic cardiomyopathy in male mice treated with an NNRTI: the role of vitamin K.

Author

De Jonghe S, Verbeeck J, Vinken P, Lammens L, Starckx S, Lachau-Durand S, Bouche MP, Willems B, and Coussement W

Subjects
Administration, Oral, Animals, Area Under Curve, Blood Coagulation drug effects, Cardiomyopathies prevention & control, Diet, Female, Heart drug effects, Hemorrhagic Disorders prevention & control, Male, Mice, Nitriles, Partial Thromboplastin Time, Prothrombin Time, Pyrimidines, Troponin T blood, Vitamin K Deficiency prevention & control, Cardiomyopathies etiology, Hemorrhagic Disorders etiology, Pyridazines toxicity, Reverse Transcriptase Inhibitors toxicity, Vitamin K therapeutic use, Vitamin K Deficiency etiology
Abstract

Dietary dosing of the non-nucleoside reverse transcriptase inhibitor (NNRTI) TMC125, under development for treatment of HIV-1, resulted in a syndrome in male mice in a previous experiment that was termed hemorrhagic cardiomyopathy. In literature, this syndrome, which was described in rodent species only, was linked to vitamin K deficiency. Two mechanistic studies were conducted, one with dietary administration and a second with gavage. The syndrome was reproduced in only 1 male mouse after continuous dietary dosing, and TMC125 was demonstrated to affect coagulation parameters (prothrombin time [PT], activated partial thromboplastin time [APTT], clotting factors II, VII and XI), particularly in males. This was counteracted by vitamin K supplementation, supporting the hypothesis that the effects were mediated via a vitamin K deficiency. It is therefore concluded that the observed cardiac changes were not caused by a direct cardiotoxic effect but occurred after a state of disabled clotting ability with subsequent effects on mouse cardiac muscle. Therefore, clotting times can be used as adequate safety biomarkers in clinical trials. To date, no changes have been observed at therapeutic doses of TMC125, following human monitoring of PT and APTT. One other NNRTI, Efavirenz (Sustiva), has been reported to cause prolongation of coagulation times in rats and monkeys.

Published
2008
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49. Optimising the design of preliminary toxicity studies for pharmaceutical safety testing in the dog.

Author

Smith D, Combes R, Depelchin O, Jacobsen SD, Hack R, Luft J, Lammens L, von Landenberg F, Phillips B, Pfister R, Rabemampianina Y, Sparrow S, Stark C, and Stephan-Gueldner M

Subjects
Animals, Pharmaceutical Preparations classification, Toxicity Tests standards, Animal Testing Alternatives, Animal Welfare, Dogs, Drug Evaluation, Preclinical methods, Drug-Related Side Effects and Adverse Reactions, Toxicity Tests methods
Abstract

A working party, comprising two animal welfare organisations and some 12 pharmaceutical companies in Europe, was established to minimise the use of the dog in safety testing. As first step, the participants defined the major objectives of preliminary dose-range finding/MTD toxicity studies in non-rodents, defined the principles and requirements for this study type and agreed on a proposal for an optimised study design, based on collective experience of conducting such studies in industry, involving an evaluation of 100 individual study data sets. The suggested study design is explained and described, and reflects current best practice in the pharmaceutical industry in Europe. The implementation of such an optimised design is believed to result in a reduction in the overall numbers of animals used for this purpose, without jeopardising the scientific rationale and usefulness of the studies for informing the conduct of later regulatory studies.

Published
2005
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