Your search keyword '"Greiter-Wilke, Andrea"' showing total 33 results

1. Cardiovascular safety assessments in the cynomolgus monkey: Unmasking potential background arrhythmias in general toxicity studies.

Author

Greiter-Wilke, Andrea, Baird, Ted, O'Donohue, Kyle, and Koerner, Annette

Subjects

*CARDIOVASCULAR agents, *MEDICATION safety, *KRA, *ARRHYTHMIA, *DRUG toxicity, *THERAPEUTICS

Abstract

Introduction We describe experience with an unexpectedly high background incidence of atrioventricular block (AVB) observed in Mauritian cynomolgus monkeys (MCM) during preclinical safety assessment for bitopertin, a glycine-transporter-1 inhibitor. Methods Preclinical ECGs were reviewed to assess potential effects on cardiac conductivity, specifically AVB. Results Bitopertin administration in Chinese/Vietnamese monkeys (CVM; n = 46) or MCM (n = 64, from all relevant studies) revealed dose-dependent hypoactivity with a lack of expected increases in heart rate in response to chair-restraint during ECG recordings. Instances of 2° AVB were detected post-dose in two repeat-dose studies in MCM. AVB was generally restricted to animals showing a lower than expected increase in heart rate during restraint compared to placebo conditions (111–161 to 220–250 bpm). A subsequent study in MCM prescreened for AVB found pre-existing 2° AVB in 15.4% of animals. After exclusion of these animals, no incidences of AVB were identified over 36 weeks of bitopertin treatment. No evidence of AVB was observed in CVM in a 14-day study with continuous ECG recordings or in any clinical studies to date. Discussion Bitopertin-treatment was not associated with a direct effect on AV conduction in AVB naive MCM. Pre-test detection of AVB in MCM was likely due to the unmasking of pre-existing AVB through a slowed heart rate. The background incidence of AVB in the current MCM cohort was much higher than has been previously reported. These data suggest that ECG prescreening of unrestrained, nonstressed animals is recommended for the accurate assessment of possible treatment-related increases in AVB, especially in MCM. [ABSTRACT FROM AUTHOR]

Published

2016

2. Nonclinical cardiovascular safety assessment of thioridazine: Impact of autonomic tone, body temperature, and choice of species.

Author

Greiter-Wilke, Andrea, Roberts, Sonia, Heinig, Katja, Waiz, David, Jenni, Roland, and Holzgrefe, Henry

Subjects

*BODY temperature, *KRA, *AUTONOMIC nervous system, *SPECIES, *BEAGLE (Dog breed), *BLOOD pressure

Abstract

Pending updates to ICH S7B/E14 guidelines will enable the substitution of human TQT studies with support from concomitant negative hERG and non-rodent CV studies. This retrospective analysis compared the effects of thioridazine (THD) (5–20 mg/kg) on heart rate (HR), blood pressure (BP), body temperature (Tc), and QT in the dog (n = 6), cynomolgus monkey (n = 4), and Goettingen minipig (n = 4) with data from previously completed studies employing crossover designs. As QT measurements are confounded by HR and Tc changes, QT effects were individually corrected for changes in HR (QTca) and Tc (QTcaT). THD-induced hemodynamic changes seen in humans were most accurately reflected in the monkey and, to a lesser extent, the dog, but not in the minipig. The minipig was most sensitive to THD QTc effects. When QTca was adjusted for THD-associated Tc decreases in minipigs and monkeys, the minipig revealed a lessened but pronounced QTcaT increase (48 ms). In the monkey, a persistent QTca increase was reduced to only a transient (0.5–3 h) QTcaT increase (20 ms). The dog's lack of THD QTca effects triggered co-administration of atenolol (AT) to attenuate THD-induced HR increases in the dog and monkey. THD + AT revealed peak QTcaT increases of 32 ms in the dog and 40 ms in the monkey, suggesting potential autonomic nervous system (ANS) interference in detecting repolarization changes. These results highlight critical species-specific differences in the outcome of parallel safety investigations. Species selection for nonclinical safety studies should consider the potential impact of Tc and ANS effects to avoid false-negative or overly positive outcomes. [ABSTRACT FROM AUTHOR]

Published

2022

3. CiPA-like Cardiovascular In Silico Modeling—Two Case Reports.

Author

Greiter-Wilke, Andrea, Davies, Mark, Sturm, Stefan, Roberts, Sonia, and Polonchuk, Liudmila

Subjects

*ION channel models, *TELEMETRY

Published

2017

4. Cardiovascular effects of RTR2996, a single stranded oligonucleotide, in the minipig.

Author

Roberts, Sonia, Greiter-Wilke, Andrea, Waiz, David, Jenni, Roland, Weile, Christian, Zihlmann, Marco, Tessier, Yann, Braendli-Baiocco, Annamaria, and Festag, Matthias

Subjects

*COMPLEMENT activation, *COMPLEMENT receptors, *BLOOD pressure, *OLIGONUCLEOTIDES, *NUCLEIC acids

Published

2019

5. Evaluation of a CNS compound in two species: Differential pharmacological responses in dogs and minipigs

Author

Greiter-Wilke, Andrea, Baird, Theodore J., Mohr, Susanne, Stewart, Lucinda, Sarmiento, Rosa Maria Rodriguez, and Sanders, Martin

Published

2012

6. Atrioventricular block in the Mauritian cynomolgus monkey—A not so uncommon arrhythmia?

Author

Greiter-Wilke, Andrea, O'Donohue, Kyle, Körner, Annette, and Baird, Ted

Subjects

*ATRIOVENTRICULAR node, *KRA, *ARRHYTHMIA, *PHARMACEUTICAL research, *DRUG toxicity, *DRUG dosage, *ELECTROCARDIOGRAPHY

Published

2015

7. Sensitivity of telemetry to predict QT interval prolongation in dog toxicity studies: Assessment of effects of moxifloxacin by invasive and non-invasive methods

Author

Festag, Matthias, Greiter-Wilke, Andrea, Schmitt, Georg, Holzgrefe, Henry, Breidenbach, Alexander, and Weiser, Thomas

Published

2009

8. Application of the probabilistic method for QT rate-correction in telemetered beagles: Effects of moxifloxacin

Author

Greiter-Wilke, Andrea, Jenni, R., Waiz, D., Breidenbach, A., and Holzgrefe, H.

Published

2008

9. Renal studies in safety pharmacology and toxicology: A survey conducted in the top 15 pharmaceutical companies.

Author

Benjamin, Amanda, Gallacher, David J., Greiter-Wilke, Andrea, Guillon, Jean-Michel, Kasai, Cheiko, Ledieu, David, Levesque, Paul, Prelle, Katja, Ratcliffe, Sian, Sannajust, Frederick, and Valentin, Jean-Pierre

Subjects

*MEDICATION safety, *DRUG toxicity, *KIDNEY physiology, *PHARMACEUTICAL industry, *PHARMACOLOGY

Abstract

Introduction With the recent development of more sensitive biomarkers to assess kidney injury preclinically, a survey was designed i) to investigate what strategies are used to investigate renal toxicity in both ICH S7A compliant Safety Pharmacology (SP) studies after a single dose of a compound and within repeat-dose toxicity studies by large pharmaceutical companies today; ii) to understand whether renal SP studies have impact or utility in drug development and/or if it may be more appropriate to assess renal effects after multiple doses of compounds; iii) to ascertain how much mechanistic work is performed by the top 15 largest pharmaceutical companies (as determined by R&D revenue size); iv) to gain an insight into the impact of the validation of DIKI biomarkers and their introduction in the safety evaluation paradigm; and v) to understand the impact of renal/urinary safety study data on progression of projects. Methods Two short anonymous surveys were submitted to SP leaders of the top 15 pharmaceutical companies, as defined by 2012 R&D portfolio size. Fourteen multiple choice questions were designed to explore the strategies used to investigate renal effects in both ICH S7A compliant SP studies and within toxicology studies. Results A 67% and 60% response rate was obtained in the first and second surveys, respectively. Nine out of ten respondent companies conduct renal excretory measurements (eg. urine analysis) in toxicology studies whereas only five out of ten conduct specific renal SP studies; and all of those 5 also conduct the renal excretory measurements in toxicology studies. These companies measure and/or calculate a variety of parameters as part of these studies, and also on a case by case basis include regulatory qualified and non-qualified DIKI biomarkers. Finally, only one company has used renal/urinary functional data alone to stop a project, whereas the majority of respondents combine renal data with other target organ assessments to form an integrated decision-making set. Conclusion These short surveys highlighted areas of similarity: a) urinary measurements are most commonly taken on repeat-dose toxicity studies, and b) renal SP studies are less often utilised. The two major differences are a) lack of consistent use of DIKI biomarkers in urinary safety studies and b) the way large pharmaceutical companies assess renal function. Finally, suggestions were made to improve the safety assessment methods for determining the safety of compounds with potential renal liability. [ABSTRACT FROM AUTHOR]

Published

2015

10. Assessment of corrected JT-peak (JTpc) and Tpeak-to-Tend (TpTec) as proarrhythmia biomarkers in non-human primates: Outcome from a HESI consortium.

Author

Boulay, Emmanuel, Authier, Simon, Bartko, Theresa, Greiter-Wilke, Andrea, Leishman, Derek, Li, Dingzhou, Nichols, Jill V., Pierson, Jennifer, Rossman, Eric I., Valentin, Jean-Pierre, Vicente, Jose, Walisser, Jacqueline, Troncy, Eric, and Wisialowski, Todd A.

Subjects

*KRA, *ION channels, *QUINIDINE, *PROARRHYTHMIA, *PHARMACODYNAMICS

Abstract

Corrected QT interval (QTc)is an established biomarker for drug-induced Torsade de Pointe (TdP), but with concerns for a false positive signal. Clinically, JTpc and TpTec have emerged as ECG sub-intervals to differentiate predominant hERG vs. mixed ion channel blocking drugs that prolong QTc. In a multicentric, prospective, controlled study, different proarrhythmic drug effects on QTc, JTpc and TpTec were characterized with cynomolgus monkeys using telemetry in a Lead II configuration for internal and external telemetry.Drugs and vehicle were administered orally (PO) to group size of 4 to 8 animals, in 4 laboratories. In monkeys, dofetilide (0.03–0.3 mg/kg) was associated with exposure dependent QTc and JTpc increase, but no significant TpTec effect. Similarly, quinidine (2–50 mg/kg) increased QTc and JTpc but did not change TpTec. Mexiletine (1–15 mg/kg) and verapamil (50 mg/kg) did not induce any significant effect on QTc, JTpc or TpTec. Clinically, predominant hERG blockers (dofetilide and quinidine) prolong QTc, JTpc and TpTec and are associated with increased risk for TdP. Results from this study demonstrate that ECG changes after dofetilide and quinidine administration to telemetered monkeys differ from the clinical response, lacking the expected effects on TpTec. Potential explanations for the lack of translation include physio-pharmacology species differences or ECG recording and analysis methodology variations. Mixed ion channel blockers verapamil and mexiletine administered to monkeys showed no significant QTc, JTpc or TpTec prolongation as expected based on the similar clinical response for these agents. [ABSTRACT FROM AUTHOR]

Published

2024

11. Feasibility studies to investigate the use of jacketed telemetry in the Göttingen minipig for the assessment of ECG and respiration.

Author

Waiz, David, Roberts, Sonia, Greiter-Wilke, Andrea, and Jenni, Roland

Subjects

*TELEMETRY, *FEASIBILITY studies, *ELECTROCARDIOGRAPHY, *RESPIRATORY measurements, *RESPIRATION

Published

2019

12. Feasibility studies to investigate the use of jacketed telemetry in the Göttingen minipig for the assessment of ECG and respiration.

Author

Waiz, David, Roberts, Sonia, Greiter-Wilke, Andrea, and Jenni, Roland

Subjects

*TELEMETRY, *SWINE, *ELECTROCARDIOGRAPHY, *RESPIRATION, *MEDICAL screening, *ANIMAL health

Published

2018

13. Best practice considerations for nonclinical in vivo cardiovascular telemetry studies in non-rodent species: Delivering high quality QTc data to support ICH E14/S7B Q&As.

Author

Rossman, Eric I., Wisialowski, Todd A., Vargas, Hugo M., Valentin, Jean-Pierre, Rolf, Michael G., Roche, Brian M., Riley, Steve, Pugsley, Michael K., Nichols, Jill, Li, Dingzhou, Leishman, Derek J., Kleiman, Robert B., Greiter-Wilke, Andrea, Gintant, Gary A., Engwall, Michael J., Delaunois, Annie, and Authier, Simon

Subjects

*CONTRACT research organizations, *TELEMETRY, *BEST practices, *DATA quality, *DRUG development

Abstract

The ICH E14/S7B Questions and Answers (Q&As) guideline introduces the concept of a "double negative" nonclinical scenario (negative hERG assay and negative in vivo QTc study) to demonstrate that a drug does not produce a clinically relevant QT prolongation (i.e., no QT liability). This nonclinical "double negative" data package, along with negative Phase 1 clinical QTc data, may be sufficient to substitute for a clinical Thorough QT (TQT) study in some specific cases. While standalone GLP in vivo cardiovascular studies in non-rodent species are standard practice during nonclinical drug development for small molecule programs, a variety of approaches to the design, conduct, analysis and interpretation are utilized across pharmaceutical companies and contract research organizations (CROs) that may, in some cases, negatively impact the stringent sensitivity needed to fulfill the new Q&As. Subject matter experts from both Pharma and CROs have collaborated to recommend best practices for more robust nonclinical cardiovascular telemetry studies in non-rodent species, with input from clinical and regulatory experts. The aim was to increase consistency and harmonization across the industry and to ensure delivery of high quality nonclinical QTc data to meet the proposed sensitivities defined within the revised ICH E14/S7B Q&As guideline (Q&As 5.1 and 6.1). The detailed best practice recommendations presented here cover the design and execution of the safety pharmacology cardiovascular study, including optimal methods for acquiring, analyzing, reporting, and interpreting the resulting QTc and pharmacokinetic data to allow for direct comparison to clinical exposures and assessment of safety margin for QTc prolongation. [ABSTRACT FROM AUTHOR]

Published

2023

14. The Safety Pharmacology Society salary survey.

Author

Pugsley, Michael K., Authier, Simon, Brabham, Tiffini, Soloviev, Maxim, Markgraf, Carrie G., Correll, Krystle, Traebert, Martin, Greiter-Wilke, Andrea, Valentin, Jean-Pierre, Vargas, Hugo, Botchway, Alfred, Leishman, Derek J., and Curtis, Michael J.

Subjects

*WAGE surveys, *PHARMACOLOGY, *CERTIFICATION, *MEDICATION safety, *PHARMACOLOGISTS, *STATISTICAL correlation

Abstract

Introduction Safety pharmacology is a growing discipline with scientists broadly distributed across international geographical regions. This electronic salary survey is the first to be distributed amongst the entire Safety Pharmacology Society (SPS) membership. An electronic survey was sent to all members of the Society. Categorical survey questions assessed membership employment types, annual incomes, and professional certifications, along with other associated career attributes. Methods This survey was distributed to the SPS membership that is comprised of safety pharmacologists, toxicologists and pharmacologists working globally in the pharmaceutical industry, at contract research organizations (CRO), regulatory agencies, and academia or within the technology provider industry. The survey was open for responses from December 2015 to March 2016. Results The survey response rate was 28% (129/453). North America (68%) was the region with the largest number of respondents followed by Europe (28%). A preponderance of respondents (77%) had 12 years of industry experience or more. 52% of responders earned annually between $40,000 and $120,000. As expected, salary was generally positively correlated with the number of years of experience in the industry or the educational background but there was no correlation between salary and the number of employee's directly supervised. The median salary was higher for male vs female respondents, but so was median age, indicative of no gender ‘salary gap’. Discussion Our 2016 SPS salary survey results showcased significant diversity regarding factors that can influence salary compensation within this discipline. These data provided insights into the complex global job market trends. They also revealed the level of scientific specialization embedded within the organization, presently uniquely positioned to support the dynamic career paths of current and future safety pharmacologists. [ABSTRACT FROM AUTHOR]

Published

2017

15. The incidence of spontaneous arrhythmias in telemetered beagle dogs, Göttingen Minipigs and Cynomolgus non-human primates: A HESI consortium retrospective analysis.

Author

Boulay, Emmanuel, Miraucourt, Loïs S., Pugsley, Michael K., Abernathy, Matthew M., Chui, Ray, Dalton, Jill, Demers, Marjorie, Dybdal, Noel, Gazaille, Elissa, Greiter-Wilke, Andrea, Hoffmann, Peter, Huang, Hai, LaDuke, Carrie, Norton, Kevin, Pierson, Jennifer B., Reeves, Isabelle, Roche, Brian, Rossman, Eric I., Schultze, Albert E., and Tang, Hai-Ming

Subjects

*BEAGLE (Dog breed), *ARRHYTHMIA, *FEMALE dogs, *BLOOD diseases, *PRIMATES, *VENTRICULAR fibrillation

Abstract

Characterization of the incidence of spontaneous arrhythmias to identify possible drug-related effects is often an important part of the analysis in safety pharmacology studies using telemetry. A retrospective analysis in non-clinical species with and without telemetry transmitters was conducted. Electrocardiograms (24 h) from male and female beagle dogs (n = 131), Göttingen minipigs (n = 108) and cynomolgus non-human primates (NHP; n = 78) were analyzed. Ventricular tachycardia (VT) was observed in 3% of the dogs but was absent in minipigs and NHPs. Ventricular fibrillation (VF) was not observed in the 3 species. Ventricular premature beats (VPBs) were more frequent during daytime and atrioventricular blocks (AVBs) were more frequent at night in all species. A limited number of animals exhibited a high arrhythmia frequency and there was no correlation between animals with higher frequency of an arrhythmia type and the frequency of other arrythmias in the same animals. Clinical chemistry or hematology parameters were not different with or without telemetry devices. NHP with a transmural left ventricular pressure (LVP) catheter exhibited a greater incidence of VPBs and PJCs compared to telemetry animals without LVP. All species were similar with regards to the frequency of ventricular ectopic beats (26–46%) while the dog seemed to have more frequent junctional complexes and AVB compared to NHP and minipigs. Arrhythmia screening may be considered during pre-study evaluations, to exclude animals with abnormally high arrhythmia incidence. [ABSTRACT FROM AUTHOR]

Published

2023

16. Improving the in Vivo QTc assay: The value of implementing best practices to support an integrated nonclinical-clinical QTc risk assessment and TQT substitute.

Author

Vargas, Hugo M., Rossman, Eric I., Wisialowski, Todd A., Nichols, Jill, Pugsley, Michael K., Roche, Brian, Gintant, Gary A., Greiter-Wilke, Andrea, Kleiman, Robert B., Valentin, Jean-Pierre, and Leishman, Derek J.

Subjects

*RISK assessment, *BEST practices, *SIGNAL detection, *DRUG labeling, *IN vivo studies, *DRUG side effects

Abstract

Recent updates and modifications to the clinical ICH E14 and nonclinical ICH S7B guidelines, which both relate to the evaluation of drug-induced delayed repolarization risk, provide an opportunity for nonclinical in vivo electrocardiographic (ECG) data to directly influence clinical strategies, interpretation, regulatory decision-making and product labeling. This opportunity can be leveraged with more robust nonclinical in vivo QTc datasets based upon consensus standardized protocols and experimental best practices that reduce variability and optimize QTc signal detection, i.e. , demonstrate assay sensitivity. The immediate opportunity for such nonclinical studies is when adequate clinical exposures (e.g. , supratherapeutic) cannot be safely achieved, or other factors limit the robustness of the clinical QTc evaluation, e.g. , the ICH E14 Q5.1 and Q6.1 scenarios. This position paper discusses the regulatory historical evolution and processes leading to this opportunity and details the expectations of future nonclinical in vivo QTc studies of new drug candidates. The conduct of in vivo QTc assays that are consistently designed, executed and analyzed will lead to confident interpretation, and increase their value for clinical QTc risk assessment. Lastly, this paper provides the rationale and basis for our companion article which describes technical details on in vivo QTc best practices and recommendations to achieve the goals of the new ICH E14/S7B Q&As, see Rossman et al., 2023 (this journal). [ABSTRACT FROM AUTHOR]

Published

2023

17. Human ex-vivo action potential model for pro-arrhythmia risk assessment.

Author

Page, Guy, Ratchada, Phachareeya, Miron, Yannick, Steiner, Guido, Ghetti, Andre, Miller, Paul E., Reynolds, Jack A., Wang, Ken, Greiter-Wilke, Andrea, Polonchuk, Liudmila, Traebert, Martin, Gintant, Gary A., and Abi-Gerges, Najah

Subjects

*ACTION potentials, *ARRHYTHMIA, *DRUG development, *ORGAN donors, *DOFETILIDE, *THERAPEUTICS, *DISEASE risk factors

Abstract

While current S7B/E14 guidelines have succeeded in protecting patients from QT-prolonging drugs, the absence of a predictive paradigm identifying pro-arrhythmic risks has limited the development of valuable drug programs. We investigated if a human ex-vivo action potential (AP)-based model could provide a more predictive approach for assessing pro-arrhythmic risk in man. Human ventricular trabeculae from ethically consented organ donors were used to evaluate the effects of dofetilide, d,l-sotalol, quinidine, paracetamol and verapamil on AP duration (APD) and recognized pro-arrhythmia predictors (short-term variability of APD at 90% repolarization (STV(APD90)), triangulation (ADP90-APD30) and incidence of early afterdepolarizations at 1 and 2 Hz to quantitatively identify the pro-arrhythmic risk. Each drug was blinded and tested separately with 3 concentrations in triplicate trabeculae from 5 hearts, with one vehicle time control per heart. Electrophysiological stability of the model was not affected by sequential applications of vehicle (0.1% dimethyl sulfoxide). Paracetamol and verapamil did not significantly alter anyone of the AP parameters and were classified as devoid of pro-arrhythmic risk. Dofetilide, d,l-sotalol and quinidine exhibited an increase in the manifestation of pro-arrhythmia markers. The model provided quantitative and actionable activity flags and the relatively low total variability in tissue response allowed for the identification of pro-arrhythmic signals. Power analysis indicated that a total of 6 trabeculae derived from 2 hearts are sufficient to identify drug-induced pro-arrhythmia. Thus, the human ex-vivo AP-based model provides an integrative translational assay assisting in shaping clinical development plans that could be used in conjunction with the new CiPA-proposed approach. [ABSTRACT FROM AUTHOR]

Published

2016

18. Applying the audiogenic seizure model to evaluate the interaction with anticonvulsant treatment.

Author

Dinklo, Theo, Aegler, Monika, and Greiter-Wilke, Andrea

Subjects

*SPASMS, *ANTICONVULSANTS, *EMERGENCY medicine, *BENZODIAZEPINES, *DRUG interactions, *CLINICAL trials

Published

2015

19. Translational PK/PD modeling for cardiovascular safety assessment of drug candidates: Methods and examples in drug development.

Author

Caruso, Antonello, Frances, Nicolas, Meille, Christophe, Greiter-Wilke, Andrea, Hillebrecht, Alexander, and Lavé, Thierry

Subjects

*PHARMACOKINETICS, *PHARMACODYNAMICS, *CARDIOVASCULAR system physiology, *DRUG toxicity, *DRUG development, *MEDICAL protocols

Abstract

Introduction Cardiovascular toxicity is a significant cause of candidate failure in drug development. Pharmacokinetic/pharmacodynamic (PK/PD) modeling may reduce attrition by improving the understanding of the relationship between drug exposure and changes in cardiovascular endpoints. Diverse examples are discussed that elucidate how modeling can facilitate the interpretation of cardiovascular safety data in animals and enable quantitative translation of preclinical findings to man. Methods Twelve compounds under development in diverse therapeutic areas were tested in cardiovascular safety studies in the telemetered beagle dog and cynomolgus monkey. Drug-induced changes observed in different cardiovascular endpoints (QRS complex and QTc interval of the ECG, heart rate, blood pressure, and myocardial contractility) were described by means of PK/PD modeling. A range of direct and indirect effect models were employed to characterize the plasma concentration-cardiovascular effect relationship for each compound. Results For every drug candidate the proposed PK/PD models appropriately described the cardiovascular effects observed in dog and monkey. Two of the compounds subsequently reached clinical development and cardiovascular data were generated in first-in-human clinical trials. For one drug candidate, a threshold model was used to describe QTc prolongation in the monkey and man. Blood pressure changes induced by the second compound were linked to plasma exposure in dog and human via an indirect response model. In both cases it was found that translational modeling accurately predicted the human response observed during clinical development. Discussion In this article, a range of PK/PD models are discussed that successfully described cardiovascular safety findings in the preclinical setting. Where clinical data were available, it was found that translational modeling enabled the accurate prediction of outcomes in man and facilitated the description of the therapeutic index. PK/PD modeling is thus demonstrated as a powerful tool to aid in the quantitative cardiovascular safety assessment of drug candidates and the optimization of early clinical study protocols. [ABSTRACT FROM AUTHOR]

Published

2014

20. Preclinical QT safety assessment: Cross-species comparisons and human translation from an industry consortium.

Author

Holzgrefe, Henry, Ferber, Georg, Champeroux, Pascal, Gill, Michael, Honda, Masaki, Greiter-Wilke, Andrea, Baird, Theodore, Meyer, Olivier, and Saulnier, Muriel

Subjects

*MEDICATION safety, *CROSS-species amplification, *DRUG therapy for heart diseases, *MEDICAL needs assessment, *COMPARATIVE studies, *ANIMAL models in research

Abstract

Abstract: Introduction: In vivo models have been required to demonstrate relative cardiac safety, but model sensitivity has not been systematically investigated. Cross-species and human translation of repolarization delay, assessed as QT/QTc prolongation, has not been compared employing common methodologies across multiple species and sites. Therefore, the accurate translation of repolarization results within and between preclinical species, and to man, remains problematic. Methods: Six pharmaceutical companies entered into an informal consortium designed to collect high-resolution telemetered data in multiple species (dog; n=34, cynomolgus; n=37, minipig; n=12, marmoset; n=14, guinea pig; n=5, and man; n=57). All animals received vehicle and varying doses of moxifloxacin (3–100mg/kg, p.o.) with telemetered ECGs (≥500Hz) obtained for 20–24h post-dose. Individual probabilistic QT–RR relationships were derived for each subject. The rate-correction efficacies of the individual (QTca) and generic correction formulae (Bazett, Fridericia, and Van de Water) were objectively assessed as the mean squared slopes of the QTc–RR relationships. Normalized moxifloxacin QTca responses (Veh Δ%/μM) were derived for 1h centered on the moxifloxacin Tmax. Results: All QT–RR ranges demonstrated probabilistic uncertainty; slopes varied distinctly by species where dog and human exhibited the lowest QT rate-dependence, which was much steeper in the cynomolgus and guinea pig. Incorporating probabilistic uncertainty, the normalized QTca-moxifloxacin responses were similarly conserved across all species, including man. Discussion: The current results provide the first unambiguous evidence that all preclinical in vivo repolarization assays, when accurately modeled and evaluated, yield results that are consistent with the conservation of moxifloxacin-induced QT prolongation across all common preclinical species. Furthermore, these outcomes are directly transferable across all species including man. The consortium results indicate that the implementation of standardized QTc data presentation, QTc reference cycle lengths, and rate-correction coefficients can markedly improve the concordance of preclinical and clinical outcomes in most preclinical species. [Copyright &y& Elsevier]

Published

2014

21. Current nonclinical in vivo safety pharmacology testing enables safe entry to first-in-human clinical trials: The IQ consortium nonclinical to clinical translational database.

Author

Ackley, David, Abernathy, Matthew, Chaves, Alysia, Damiano, Bruce, Delaunois, Annie, Foley, Michael, Greiter-Wilke, Andrea, Guillon, Jean-Michel, Maher, Jonathan, Monticello, Tom, Pannirselvam, Malar, Renninger, Jon, and Vargas, Hugo

Subjects

*PHARMACOLOGY, *CLINICAL trials, *INTELLIGENCE levels, *CONSORTIA, *DATABASES

Published

2019

22. Rodent respiratory findings with mGlu5 positive allosteric modulator RG7342, translation to non-rodent and man.

Author

Dinklo, Theo, Waiz, David, Roberts, Sonia, Sturm, Stefan, Jenni, Roland, Aegler, Monika, and Greiter-Wilke, Andrea

Subjects

*RODENTS, *PLETHYSMOGRAPHY, *KRA, *MURIDAE, *TRANSLATIONS

Published

2019

23. Cardiovascular effects of verapamil in the Göttingen minipig.

Author

Roberts, Sonia, Jenni, Roland, Waiz, David, and Greiter-Wilke, Andrea

Subjects

*CALCIUM antagonists, *CALCIUM channels, *ION channels, *PULMONARY artery, *HEART beat, *BLOOD pressure

Published

2019

24. JTp and Tpe as Biomarkers of proarrhythmic risk in nonclinical models: Historical data evaluation by the HESI consortium.

Author

Gendron-Parra, Nicolas, Abernathy, Matthew M., Boulay, Emmanuel, Chui, Ray, Friedrichs, Gregory S., Greiter-Wilke, Andrea, Guillon, Jean-michel, Leishman, Derek J., Nichols, Jill, Pierson, Jennifer, Skinner, Matt, Pugsley, Michael K., Valentin, Jean-Pierre, Vargas, Hugo M., and Authier, Simon

Subjects

*BIOMARKERS, *BIOLOGICAL tags, *CONSORTIA, *DATA modeling, *BEAGLE (Dog breed)

Published

2019

25. Drug safety Africa: An overview of safety pharmacology & toxicology in South Africa.

Author

Guth, Brian D., Grobler, Anne F., Frazier, Kendall S., Greiter-Wilke, Andrea, Herzyk, Danuta, Hough, Tertius A., Khan, Asrar Ali, Markert, Michael, Smith, James D., Svenson, Karen L., Wells, Sara, and Pugsley, Michael K.

Subjects

*CLINICAL toxicology, *TOXICOLOGICAL chemistry, *TOXICOLOGY, *PHARMACOLOGY, *FOOD toxicology, *BIOMOLECULES, *CENTRAL nervous system, *GASTROINTESTINAL system

Abstract

This meeting report is based on presentations given at the first Drug Safety Africa Meeting in Potchefstroom, South Africa from November 20–22, 2018 at the North-West University campus. There were 134 attendees (including 26 speakers and 34 students) from the pharmaceutical industry, academia, regulatory agencies as well as 6 exhibitors. These meeting proceedings are designed to inform the content that was presented in terms of Safety Pharmacology (SP) and Toxicology methods and models that are used by the pharmaceutical industry to characterize the safety profile of novel small chemical or biological molecules. The first part of this report includes an overview of the core battery studies defined by cardiovascular, central nervous system (CNS) and respiratory studies. Approaches to evaluating drug effects on the renal and gastrointestinal systems and murine phenotyping were also discussed. Subsequently, toxicological approaches were presented including standard strategies and options for early identification and characterization of risks associated with a novel therapeutic, the types of toxicology studies conducted and relevance to risk assessment supporting first-in-human (FIH) clinical trials and target organ toxicity. Biopharmaceutical development and principles of immunotoxicology were discussed as well as emerging technologies. An additional poster session was held that included 18 posters on advanced studies and topics by South African researchers, postgraduate students and postdoctoral fellows. [ABSTRACT FROM AUTHOR]

Published

2019

26. Cardiovascular effects of verapamil in the Göttingen minipig.

Author

Roberts, Sonia, Jenni, Roland, Waiz, David, and Greiter-Wilke, Andrea

Subjects

*CARDIOVASCULAR system, *VERAPAMIL, *DRUG interactions, *ANIMAL models in research, *SWINE, *ANIMAL health

Published

2018

27. JTp and Tpe as Biomarkers of proarrhythmic risk in nonclinical models: Historical data evaluation by the HESI consortium.

Author

Gendron-Parra, Nicolas, Abernathy, Matthew M., Boulay, Emmanuel, Chui, Ray, Friedrichs, Gregory S., Greiter-Wilke, Andrea, Guillon, Jean-michel, Leishman, Derek J., Nichols, Jill, Pierson, Jennifer, Skinner, Matt, Pugsley, Michael K., Valentin, Jean-Pierre, Vargas, Hugo M., and Authier, Simon

Subjects

*ARRHYTHMIA, *BIOMARKERS, *PHARMACOLOGY, *CLINICAL trials, *ELECTROCARDIOGRAPHY

Published

2018

28. Using a new implantable telemetry device to examine the effects of L-NAME on cardiovascular parameters in the Göttingen minipig.

Author

Roberts, Sonia, Jenni, Roland, Waiz, David, Ferrari, Luca, Erdin, Ruedi, Bucheli, Franz, Pettinger, Steve, and Greiter-Wilke, Andrea

Subjects

*BIOTELEMETRY, *ARTIFICIAL implants, *CARDIOVASCULAR diseases, *PARAMETER estimation, *LABORATORY swine

Published

2015

29. Assessing Cardiotoxicity In Vitro: A Comparison of Complexity.

Author

Roberts, Sonia, Bertinetti-Lapatki, Cristina, Polonchuk, Liudmila, and Greiter-Wilke, Andrea

Subjects

*CARDIOTOXICITY, *ION channels

Published

2017

30. An Overview of the Safety Pharmacology Society (SPS) Strategic Plan (2016-2018).

Author

Pugsley, Michael K., Authier, Simon, Koerner, John, Redfern, Will S., Markgraf, Carrie G., Brabham, Tiffini, Correll, Krystle, Soloviev, Maxim, Botchway, Alfred, Engwall, Michael, Traebert, Martin, Valentin, Jean-Pierre, Mow, Tomas, Greiter-Wilke, Andrea, Prior, Helen, Vargas, Hugo M., and Leishman, Derek J.

Subjects

*PHARMACOLOGY, *PHARMACOLOGY education, *SOCIETIES

Published

2017

31. The electromechanical window (EMw): A heart-rate independent biomarker for delayed repolarization of the heart.

Author

Waiz, David, Roberts, Sonia, Jenni, Roland, and Greiter-Wilke, Andrea

Subjects

*ELECTROMECHANICAL effects, *BIOMARKERS, *HEART beat, *TELEMETER (Physiological apparatus), *MOXIFLOXACIN

Published

2016

32. Human ex-vivo action potential model for pro-arrhythmia risk assessment.

Author

Page, Guy, Ratchada, Phachareeya, Miron, Yannick, Ghetti, Andrea, Miller, Paul, Reynolds, Jack, Steiner, Guido, Greiter-Wilke, Andrea, Polonchuk, Liudmila, Traebert, Martin, Gintant, Gary A., and Abi-Gerges, Najah

Subjects

*ACTION potentials, *PROARRHYTHMIA, *HEALTH programs, *ORGAN donors, *ION channels, *DISEASE risk factors

Published

2016

33. Assessment of the relationship between core body temperature and QT/QTc in the minipig using Dihydrocapsaicin

Author

Tang, Hai Ming, Sanders, Martin, Baird, Theodore, and Greiter-Wilke, Andrea

Published

2012