Your search keyword '"Ingrid M C Kamerling"' showing total 47 results

1. Immunogenicity and reactogenicity of intradermal mRNA-1273 SARS-CoV-2 vaccination: a non-inferiority, randomized-controlled trial

Author

Manon L. M. Prins, Geert V. T. Roozen, Cilia. R. Pothast, Wesley Huisman, Rob van Binnendijk, Gerco den Hartog, Vincent P. Kuiper, Corine Prins, Jacqueline J. Janse, Olivia. A. C. Lamers, Jan Pieter R. Koopman, Annelieke C. Kruithof, Ingrid M. C. Kamerling, Romy C. Dijkland, Alicia. C. de Kroon, Shohreh Azimi, Mariet C. W. Feltkamp, Marjan Kuijer, Simon P. Jochems, Mirjam H. M. Heemskerk, Frits R. Rosendaal, Meta Roestenberg, Leo G. Visser, and Anna H. E. Roukens

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Fractional dosing can be a cost-effective vaccination strategy to accelerate individual and herd immunity in a pandemic. We assessed the immunogenicity and safety of primary intradermal (ID) vaccination, with a 1/5th dose compared with the standard intramuscular (IM) dose of mRNA-1273 in SARS-CoV-2 naïve persons. We conducted an open-label, non-inferiority, randomized controlled trial in the Netherlands between June and December 2021. One hundred and fifty healthy and SARS-CoV-2 naïve participants, aged 18–30 years, were randomized (1:1:1) to receive either two doses of 20 µg mRNA-1273 ID with a standard needle (SN) or the Bella-mu® needle (BM), or two doses of 100 µg IM, 28 days apart. The primary outcome was non-inferiority in seroconversion rates at day 43 (D43), defined as a neutralizing antibody concentration threshold of 465 IU/mL, the lowest response in the IM group. The non-inferiority margin was set at −15%. Neutralizing antibody concentrations at D43 were 1789 (95% CI: 1488–2150) in the IM and 1263 (951–1676) and 1295 (1020–1645) in the ID-SN and ID-BM groups, respectively. The absolute difference in seroconversion proportion between fractional and standard-dose groups was −13.95% (−24.31 to −3.60) for the ID-SN and −13.04% (−22.78 to −3.31) for the ID-BM group and exceeded the predefined non-inferiority margin. Although ID vaccination with 1/5th dose of mRNA-1273 did not meet the predefined non-inferior criteria, the neutralizing antibody concentrations in these groups are far above the proposed proxy for protection against severe disease (100 IU/mL), justifying this strategy in times of vaccine scarcity to accelerate mass protection against severe disease.

Published

2024

2. Accelerating vaccine trial conduct in a pandemic with a hot spot‐based inclusion strategy using trial and epidemic simulation

Author

Johan L. van derPlas, Michiel J. vanEsdonk, Ingrid M. C. Kamerling, and Adam F. Cohen

Subjects

Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270

Abstract

Abstract Clinical development of vaccines in a pandemic situation should be rigorous but expedited to tackle the pandemic threat as fast as possible. We explored the effects of a novel vaccine trial strategy that actively identifies and enrolls subjects in local areas with high infection rates. In addition, we assessed the practical requirements needed for such a strategy. Clinical trial simulations were used to assess the effects of utilizing these so‐called “hot spot strategy” compared to a traditional vaccine field trial. We used preset parameters of a pandemic outbreak and incorporated realistic aspects of conducting a trial in a pandemic setting. Our simulations demonstrated that incorporating a hot spot strategy shortened the duration of the vaccine trial considerably, even if only one hot spot was identified during the clinical trial. The active hot spot strategy described in this paper has clear advantages compared to a “wait‐and‐see” approach that is used in traditional vaccine efficacy trials. Completion of a clinical trial can be expedited by adapting to resurgences and outbreaks that will occur in a population during a pandemic. However, this approach requires a speed of response that is unusual for a traditional phase III clinical trial. Therefore, several recommendations are made to help accomplish rapid clinical trial setup in areas identified as local outbreaks. The described model and hot spot vaccination strategy can be adjusted to disease‐specific transmission characteristics and could therefore be applied to any future pandemic threat.

Published

2021

3. An exploratory first‐in‐man study to investigate the pharmacokinetics and safety of liposomal dexamethasone at a 2‐ and 1‐week interval in patients with metastatic castration resistant prostate cancer

Author

Josephina P. M. Vrouwe, Ingrid M. C. Kamerling, Michiel J. vanEsdonk, Josbert M. Metselaar, Frederik E. Stuurman, Gabri van derPluijm, Jacobus Burggraaf, and Susanne Osanto

Subjects

dexamethasone, liposomes, metastatic castration resistant prostate cancer, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Dexamethasone has antitumor activity in metastatic castration resistant prostate cancer (mCRPC). We aimed to investigate intravenous liposome‐encapsulated dexamethasone disodium phosphate (liposomal dexamethasone) administration in mCRPC patients. In this exploratory first‐in‐man study, patients in part A received a starting dose of 10 mg followed by five doses of 20 mg liposomal dexamethasone at 2‐week intervals. Upon review of part A safety, patients in part B received 10 weekly doses of 18.5 mg. Primary outcomes were safety and pharmacokinetic profile, secondary outcome was antitumor efficacy. Nine mCRPC patients (5 part A, 4 part B) were enrolled. All patients experienced grade 1–2 toxicity, one (part B) patient experienced grade 3 toxicity (permanent bladder catheter‐related urosepsis). No infusion‐related adverse events occurred. One patient had upsloping glucose levels ≤9.1 mmol/L. Trough plasma concentrations of liposomal‐ and free dexamethasone were below the lower limit of quantification (LLOQ) in part A, and above LLOQ in three patients in part B (t1/2 ~50 h for liposomal dexamethasone), trough concentrations of liposomal‐ and free dexamethasone increased toward the end of the study. In seven of nine patients (78%) patients, stable disease was observed in bone and/or CT scans at follow‐up, and in one (part B) of these seven patients a >50% PSA biochemical response was observed. Bi‐ and once weekly administrations of IV liposomal dexamethasone were well‐tolerated. Weekly dosing enabled trough concentrations of liposomal‐ and free dexamethasone >LLOQ. The data presented support further clinical investigation in well‐powered studies. Clinical trial registration: ISRCTN 10011715.

Published

2021

4. A novel sustained‐release cysteamine bitartrate formulation for the treatment of cystinosis: Pharmacokinetics and safety in healthy male volunteers

Author

Cécile L. Berends, Lisa Pagan, Michiel J. vanEsdonk, Naomi B. Klarenbeek, Kirsten R. Bergmann, Matthijs Moerland, Vincent van derWel, Saco J. deVisser, Hans Büller, Frans deLoos, Wouter S. deVries, Hans Waals, Leo G. J. deLeede, Jacobus Burggraaf, and Ingrid M. C. Kamerling

Subjects

compliance, cystagon, cysteamine, cystinosis, sustained‐release, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract The strict intake regimen of cysteamine bitartrate formulations, associated with side effects, is a concern for the treatment compliance in cystinosis therapy. Therefore, there is a need for a cysteamine formulation with an improved pharmacokinetic profile. This study investigated the pharmacokinetics, safety and tolerability of a new sustained‐release cysteamine dosage form, PO‐001, in healthy volunteers. This was a randomized, investigator‐blinded, three‐way cross‐over study to compare single doses (600 mg) of PO‐001 with Cystagon® (immediate‐release) and Procysbi® (delayed‐release). Collected blood samples were analyzed for plasma cysteamine concentrations and pharmacokinetic parameters were estimated by noncompartmental analysis. In addition, plasma cysteamine concentrations were analyzed using a population pharmacokinetic approach using NONMEM®. Pharmacokinetics showed clear sustained‐release characteristics of PO‐001 over time with a lower Cmax and longer Tmax compared to Cystagon® and Procysbi®. All treatment‐emergent adverse events were of mild severity, with the exception of two subjects who reported moderate severity gastrointestinal problems including vomiting and diarrhea, which were related to Cystagon® intake. Population PK simulations showed a favourable PK profile based on Cmax and Ctrough concentrations at steady state. In conclusion, a single dose of 600 mg PO‐001 was well tolerated with no findings of clinical concern. This new cysteamine bitartrate formulation showed pharmacokinetics of a sustained‐release formulation, which may be beneficial for the treatment of cystinosis patients. This study supports advancing this type of sustained‐release formulation into a subsequent study to confirm reduced dosing frequency with efficient control of white blood cells (WBCs) cystine levels. Netherlands Trial Registry (NTR) (NL67638.056.18).

Published

2021

5. Viral clearance, pharmacokinetics and tolerability of ensovibep in patients with mild to moderate COVID‐19: A phase 2a, open‐label, single‐dose escalation study

Author

Manon L. M. Prins, Johan L. van der Plas, Maurits F. J. M. Vissers, Cécile L. Berends, Gaby Tresch, Marianne Soergel, Elena Fernández, Nikita van den Berge, Daniël Duijsings, Christof Zitt, Vaia Stavropoulou, Maya Zimmermann, Roxana F. Drake, Jacobus Burggraaf, Geert H. Groeneveld, and Ingrid M. C. Kamerling

Subjects

Pharmacology, Pharmacology (medical)

Abstract

To assess viral clearance, pharmacokinetics, tolerability and symptom evolution following ensovibep administration in symptomatic COVID-19 outpatients.In this open-label, first-in-patient study a single dose of either 225 mg (n = 6) or 600 mg (n = 6) of ensovibep was administered intravenously in outpatients with mild-to-moderate COVID-19 symptoms. Pharmacokinetic profiles were determined (90-day period). Pharmacodynamic assessments consisted of viral load (qPCR and cultures) and symptom questionnaires. Immunogenicity against ensovibep and SARS-CoV-2-neutralizing activity were determined. Safety and tolerability were assessed throughout a 13-week follow-up.Both doses showed similar pharmacokinetics (first-order) with mean half-lives of 14 (SD 5.0) and 13 days (SD 5.7) for the 225- and 600-mg groups, respectively. Pharmacologically relevant serum concentrations were maintained in all subjects for at least 2 weeks postdose, regardless of possible immunogenicity against ensovibep. Viral load changes from baseline at day 15 were 5.1 (SD 0.86) and 5.3 (SD 2.2) logSingle-dose intravenous administration of 225 or 600 mg of ensovibep appeared safe and well tolerated in patients with mild-to-moderate COVID-19. Ensovibep showed favourable pharmacokinetics in patients and the pharmacodynamic results warrant further research in a larger phase 2/3 randomized-controlled trail.

Published

2022

6. Corrigendum: Controlled Human Infections As a Tool to Reduce Uncertainty in Clinical Vaccine Development

Author

Meta Roestenberg, Ingrid M. C. Kamerling, and Saco J. de Visser

Subjects

vaccine, malaria, product development (PD) process, clinical development, low-income access, Medicine (General), R5-920

Published

2019

7. Immunosuppression by hydroxychloroquine: mechanistic proof in in vitro experiments but limited systemic activity in a randomized placebo-controlled clinical pharmacology study

Author

Aliede E. in ‘t Veld, Hendrika W. Grievink, Johan L. van der Plas, Boukje C. Eveleens Maarse, Sebastiaan J. W. van Kraaij, Tess D. Woutman, Mascha Schoonakker, Naomi B. Klarenbeek, Marieke L. de Kam, Ingrid M. C. Kamerling, Manon A. A. Jansen, and Matthijs Moerland

Subjects

Immunology

Abstract

Based on its wide range of immunosuppressive properties, hydroxychloroquine (HCQ) is used for the treatment of several autoimmune diseases. Limited literature is available on the relationship between HCQ concentration and its immunosuppressive effect. To gain insight in this relationship, we performed in vitro experiments in human PBMCs and explored the effect of HCQ on T and B cell proliferation and Toll-like receptor (TLR)3/TLR7/TLR9/RIG-I-induced cytokine production. In a placebo-controlled clinical study, these same endpoints were evaluated in healthy volunteers that were treated with a cumulative dose of 2400 mg HCQ over 5 days. In vitro, HCQ inhibited TLR responses with IC50s > 100 ng/mL and reaching 100% inhibition. In the clinical study, maximal HCQ plasma concentrations ranged from 75 to 200 ng/mL. No ex vivo HCQ effects were found on RIG-I-mediated cytokine release, but there was significant suppression of TLR7 responses and mild suppression of TLR3 and TLR9 responses. Moreover, HCQ treatment did not affect B cell and T cell proliferation. These investigations show that HCQ has clear immunosuppressive effects on human PBMCs, but the effective concentrations exceed the circulating HCQ concentrations under conventional clinical use. Of note, based on HCQ’s physicochemical properties, tissue drug concentrations may be higher, potentially resulting in significant local immunosuppression. This trial is registered in the International Clinical Trials Registry Platform (ICTRP) under study number NL8726.

Published

2023

8. Controlled Human Infections As a Tool to Reduce Uncertainty in Clinical Vaccine Development

Author

Meta Roestenberg, Ingrid M. C. Kamerling, and Saco J. de Visser

Subjects

vaccine, malaria, product development (PD) process, clinical development, low-income access, Medicine (General), R5-920

Abstract

Vaccines can be extremely cost-effective public health measures. Unfortunately the research and development (R&D) of novel vaccines is suffering from rising costs and declining success rates. Because many vaccines target low- and middle income markets (LMIC), output needs to be maintained at a constrained budget. In addition, scientific neglect and political uncertainty around reimbursement decisions make it an unattractive arena for private investors. The vaccine development pipeline for LMIC thus is in need for a different, sustainable, and cost-effective development model. In conventional vaccine development, objectives for every clinical development phase have been predefined. However, given the scarcity of resources, the most efficient clinical development path should identify vaccine candidates with the highest potential impact as soon as possible. We argue for a custom-made question-based development path based on the scientific questions, success probabilities and investments required. One question can be addressed by several studies and one study can provide partial answers to multiple questions. An example of a question-based approach is the implementation of a controlled human malaria infection model (CHMI). Malaria vaccine R&D faces major scientific challenges and has limited resources. Therefore, early preliminary efficacy data needs to be obtained in order to reallocate resources as efficiently as possible and reduce clinical development costs. To meet this demand, novel malaria vaccines are tested for efficacy in so-called CHMI trials in which small groups of healthy volunteers are vaccinated and subsequently infected with malaria. Early evaluation studies of critical questions, such as CHMI, are highly rewarding, since they prevent expenditures on projects that are unlikely to succeed. Each set of estimated probabilities and costs (combined with market value) will have its own optimal priority sequence of questions to address. Algorithms can be designed to determine the optimal order in which questions should be addressed. Experimental infections of healthy volunteers is an example of how a question-based approach to vaccine development can be implemented and has the potential to change the arena of clinical vaccine development.

Published

2018

9. First‐in‐human trial to assess the safety, tolerability, pharmacokinetics and pharmacodynamics of STR‐324, a dual enkephalinase inhibitor for pain management

Author

Geert Jan Groeneveld, Erica S. Klaassen, Ingrid M C Kamerling, Emilie M. J. van Brummelen, Vanessa Ville, Annie-Claude Benichou, Cécile L. Berends, Kirsten R. Bergmann, Laurence M Moss, and Victor Juarez-Perez

Subjects

Male, dual enkephalinase inhibitor, Cmax, Pharmacology, Placebo, Double-Blind Method, first-in-human, Pharmacokinetics, Humans, Enkephalinase inhibitor, Medicine, Pharmacology (medical), Dosing, Dose-Response Relationship, Drug, business.industry, opioids, Crossover study, Healthy Volunteers, DENKI, pain management, phase 1, Tolerability, Area Under Curve, Pharmacodynamics, Neprilysin, business

Abstract

Aim Dual enkephalinase inhibitors (DENKIs) are involved in the regulation of nociception via opioid receptors. The novel compound STR-324 belongs to the DENKI pharmacological class. This first-in-human study evaluated the safety, tolerability, pharmacokinetics and pharmacodynamics of STR-324 in healthy male participants. Methods This was a randomised, double-blind, placebo-controlled ascending dosing study in two parts: in part 1, 30 participants received 0.004-11.475 mg h(-1) of STR-324 or placebo (ratio 4:1) by 4 h intravenous infusion in a two-group, partial crossover design with four treatment periods separated by 1 month wash-out, and in part 2, 48 participants divided into three groups received either the active drug (1.25-11.25 mg h(-1)) or placebo (ratio 3:1) by 48 h intravenous infusion. Safety and tolerability parameters, pharmacokinetics and pharmacodynamic effects on neurocognitive and neurophysiological tasks and on a nociceptive test battery were evaluated. Results No clinically relevant changes in safety parameters were observed. All treatment-emergent adverse events were mild and transient. The pharmacokinetics of STR-324 could not be determined due to most concentrations being below quantifiable limits. STR-324 metabolite concentrations were measurable, showing dose proportionality of C-max and AUC(inf) with an estimated t(1/2) of 0.2-0.5 h. Significant changes in pharmacodynamic parameters were observed, but these were not consistent or dose-dependent. Conclusion STR-324 displayed favourable safety and tolerability profiles at all doses up to 11.475 mg h(-1). Although pharmacokinetic characterisation of STR-324 was limited, dose proportionality could be assumed based on major metabolite data assayed as proxy. No clear effects on nociceptive thresholds or other pharmacodynamic measures were observed. Trial registry: EudraCT (2014-002402-21) and toetsingonline.nl (63085).

Published

2021

10. Accelerating vaccine trial conduct in a pandemic with a hot spot‐based inclusion strategy using trial and epidemic simulation

Author

Ingrid M. C. Kamerling, Adam F. Cohen, Johan L. van der Plas, and Michiel J van Esdonk

Subjects

Time Factors, Computer science, Population, Vaccine Efficacy, RM1-950, Article, General Biochemistry, Genetics and Molecular Biology, Pandemic, Humans, General Pharmacology, Toxicology and Pharmaceutics, education, Pandemics, Hot spot (computer programming), Clinical Trials as Topic, education.field_of_study, SARS-CoV-2, Research, General Neuroscience, Vaccine trial, COVID-19, General Medicine, Vaccine efficacy, Vaccination, Clinical trial, Risk analysis (engineering), Field trial, Therapeutics. Pharmacology, Public aspects of medicine, RA1-1270

Abstract

Clinical development of vaccines in a pandemic situation should be rigorous but expedited to tackle the pandemic threat as fast as possible. We explored the effects of a novel vaccine trial strategy that actively identifies and enrolls subjects in local areas with high infection rates. In addition, we assessed the practical requirements needed for such a strategy. Clinical trial simulations were used to assess the effects of utilizing these so‐called “hot spot strategy” compared to a traditional vaccine field trial. We used preset parameters of a pandemic outbreak and incorporated realistic aspects of conducting a trial in a pandemic setting. Our simulations demonstrated that incorporating a hot spot strategy shortened the duration of the vaccine trial considerably, even if only one hot spot was identified during the clinical trial. The active hot spot strategy described in this paper has clear advantages compared to a “wait‐and‐see” approach that is used in traditional vaccine efficacy trials. Completion of a clinical trial can be expedited by adapting to resurgences and outbreaks that will occur in a population during a pandemic. However, this approach requires a speed of response that is unusual for a traditional phase III clinical trial. Therefore, several recommendations are made to help accomplish rapid clinical trial setup in areas identified as local outbreaks. The described model and hot spot vaccination strategy can be adjusted to disease‐specific transmission characteristics and could therefore be applied to any future pandemic threat.

Published

2021

11. The Oral Pheneticillin Absorption Test: An Accurate Method to Identify Patients with Inadequate Oral Pheneticillin Absorption

Author

Anneke C. Dijkmans, Dinemarie M. Kweekel, Jaap T. van Dissel, Michiel J. van Esdonk, Ingrid M. C. Kamerling, and Jacobus Burggraaf

Subjects

penicillin, oral, pheneticillin, streptococcal, Therapeutics. Pharmacology, RM1-950

Abstract

Severe streptococcal infections are commonly treated with intravenous followed by oral penicillin (pheneticillin) therapy. However, switching from iv to oral therapy is complicated by the variability in oral pheneticillin absorption. We employed an Oral Absorption Test (OAT) for pheneticillin to identify patients in whom oral pheneticillin absorption is poor. Out of 84 patients 30 patients (36%) were identified as insufficient absorbers. Treatment failure due to pheneticillin malabsorption can be avoided by performing an OAT, and these patients should be treated by another antibiotic, which is known to be absorbed well.

Published

2019

12. Dose-Finding Study of a CEA-Targeting Agent, SGM-101, for Intraoperative Fluorescence Imaging of Colorectal Cancer

Author

Shadhvi S. Bhairosingh, Koen C.M.J. Peeters, Dennis P. Schaap, Kim S. de Valk, Charlotte E.S. Hoogstins, Denise E. Hilling, Bérénice Framery, Fabian A. Holman, Leonora S.F. Boogerd, Miranda Kusters, Maxime J M van der Valk, Françoise Cailler, Marion M. Deken, Jacobus Burggraaf, Ruben P J Meijer, Harm J. T. Rutten, Ingrid M C Kamerling, Alexander L. Vahrmeijer, Surgery, CCA - Imaging and biomarkers, and CCA - Cancer Treatment and quality of life

Subjects

Male, medicine.medical_specialty, Fluorescence-lifetime imaging microscopy, Colorectal cancer, medicine.medical_treatment, 03 medical and health sciences, 0302 clinical medicine, Carcinoembryonic antigen, Surgical oncology, Translational Research, medicine, Humans, Neoadjuvant therapy, Aged, Chemotherapy, biology, business.industry, Optical Imaging, Middle Aged, medicine.disease, Carcinoembryonic Antigen, Radiation therapy, Clinical trial, Oncology, 030220 oncology & carcinogenesis, biology.protein, Female, 030211 gastroenterology & hepatology, Surgery, Radiology, Neoplasm Recurrence, Local, Colorectal Neoplasms, business

Abstract

BackgroundCarcinoembryonic antigen is overexpressed in colorectal cancer (CRC), making it an optimal target for fluorescence imaging. A phase I/II study was designed to determine the optimal imaging dose of SGM-101 for intraoperative fluorescence imaging of primary and recurrent CRC.MethodsPatients were included and received a single dose of SGM-101 at least 24 h before surgery. Patients who received routine anticancer therapy (i.e., radiotherapy or chemotherapy) also were eligible. A dedicated near-infrared imaging system was used for real-time fluorescence imaging during surgery. Safety assessments were performed and SGM-101 efficacy was evaluated per dose level to determine the most optimal imaging dose.ResultsThirty-seven patients with CRC were included in the analysis. Fluorescence was visible in all primary and recurrent tumors. In seven patients, no fluorescence was seen; all were confirmed as pathological complete responses after neoadjuvant therapy. Two tumors showed false-positive fluorescence. In the 37 patients, a total of 97 lesions were excised. The highest mean intraoperative tumor-to-background ratio (TBR) of 1.9 (p = 0.019) was seen in the 10-mg dose. This dose showed a sensitivity of 96%, specificity of 63%, and negative predictive value of 94%. Nine patients (24%) had a surgical plan alteration based on fluorescence, with additional malignant lesions detected in six patients.ConclusionsThe optimal imaging dose was established at 10 mg 4 days before surgery. The results accentuate the potential of SGM-101 and designated a promising base for the multinational phase III study, which enrolled the first patients in June 2019.

Published

2021

13. Pharmacokinetics of fosfomycin in patients with prophylactic treatment for recurrent Escherichia coli urinary tract infection

Author

Anneke C. Dijkmans, Erik B Wilms, Cees van Nieuwkoop, Ingrid M. C. Kamerling, Jasper Stevens, Jacobus Burggraaf, S G Kuiper, and Groningen Kidney Center (GKC)

Subjects

Microbiology (medical), medicine.medical_specialty, FEMALE-PATIENTS, Urinary system, Urine, Fosfomycin, PROFILE, Gastroenterology, Pharmacokinetics, Tandem Mass Spectrometry, Escherichia coli urinary tract infection, Internal medicine, Escherichia coli, ABSORPTION, Humans, Medicine, Pharmacology (medical), In patient, Prospective Studies, Dosing, Pharmacology, PLASMA, business.industry, TROMETAMOL, biochemical phenomena, metabolism, and nutrition, PHARMACODYNAMICS, Anti-Bacterial Agents, LC-MS/MS METHOD, Infectious Diseases, Pharmacodynamics, Urinary Tract Infections, Quality of Life, PENETRATION, business, Chromatography, Liquid, medicine.drug

Abstract

Objectives To evaluate the pharmacokinetics and clinical effectiveness of IV and oral fosfomycin treatment in patients with recurrent urinary tract infection (rUTI) with Escherichia coli. Patients and methods Patients with rUTI treated with 3 g of oral fosfomycin every 72 h for at least 14 days were included in a prospective open-label single-centre study. Serum samples were taken after oral and IV administration of fosfomycin. Urine was collected for 24 h on 3 consecutive days. Fosfomycin concentrations in serum and urine were analysed using validated LC–MS/MS. Pharmacokinetics were evaluated using a population model. EudraCT number 2018-000616-25. Results Twelve patients were included, of whom nine were also administered IV fosfomycin. Data were best described by a two-compartment model with linear elimination and a transit-absorption compartment. Median values for absolute bioavailability and serum half-life were 18% and 2.13 h, respectively. Geometric mean urine concentrations on Days 1, 2 and 3 were above an MIC of 8 mg/L after both oral and IV administration. Quality of life reported on a scale of 1–10 increased from 5.1 to 7.4 (P = 0.001). The average score of UTI symptoms decreased after fosfomycin dosing (by 3.1 points, 95% CI = −0.7 to 7.0, P = 0.10). Conclusions Oral fosfomycin at 3 g every 72 h provides plasma and urine concentrations of fosfomycin above the MIC for E. coli. This pharmacokinetic model can be used to develop optimal dosing regimens of fosfomycin in patients with UTI.

Published

2020

14. Administration of an adeno-associated viral vector expressing interferon-beta in patients with inflammatory hand arthritis, results of a phase I/II study

Author

G. Ruiterkamp, R.G.H.H. Nelissen, J.P.M. Vrouwe, J.J.M. Meulenberg, Monique Reijnierse, L. Bevaart, Ingrid M. C. Kamerling, Jacobus Burggraaf, T.W.J. Huizinga, R.J. Lamers, N.B. Klarenbeek, Margreet Kloppenburg, and A. Navas-Cañete

Subjects

medicine.medical_specialty, Hand Joints, Genetic enhancement, Genetic Vectors, Biomedical Engineering, Arthritis, Gastroenterology, Viral vector, Cohort Studies, Gene therapy, Rheumatology, Internal medicine, Osteoarthritis, medicine, Humans, Orthopedics and Sports Medicine, Vector (molecular biology), Rheumatoid arthritis, Adverse effect, Aged, biology, business.industry, IFN-beta, Genetic Therapy, Interferon-beta, Dependovirus, Middle Aged, medicine.disease, Tolerability, biology.protein, AAV5, Female, Antibody, business

Abstract

Objective: Inflammatory hand arthritis (IHA) results in impaired function. Local gene therapy with ART-I02, a recombinant adeno-associated virus (AAV) serotype 5 vector expressing interferon (IFN)-beta, under the transcriptional control of nuclear factor kappa-B responsive promoter, was preclinically shown to have favorable effects. This study aimed to investigate the safety and tolerability of local gene therapy with ART-I02 in patients with IHA.Methods: In this first-in-human, dose-escalating, cohort study, 12 IHA patients were to receive a single intra-articular (IA) injection of ART-I02 ranging 0.3 x 10(12)-1.2 x 10(13) genome copies in an affected hand joint. Adverse events (AEs), routine safety laboratory and the clinical course of disease were periodically evaluated. Baseline- and follow-up contrast enhanced magnetic resonance images (MRIs), shedding of viral vectors in bodily fluids, and AAV5 and IFN-beta immune responses were evaluated. A data review committee provided safety recommendations.Results: Four patients were enrolled. Long-lasting local AEs were observed in 3 patients upon IA injection of ART-I02. The AEs were moderate in severity and could be treated conservative. Given the duration of the AEs and their possible or probable relation to ART-I02, no additional patients were enrolled. No systemic treatment emergent AEs were observed. The MRIs reflected the AEs by (peri)arthritis. No T-cell response against AAV5 or IFN-beta, nor IFN-beta antibodies could be detected. Neutralizing antibody titers against AAV5 raised post-dose.Conclusion: Single IA doses of 0.6 x 10(12) or 1.2 x 10(12) ART-I02 vector genomes were administered without systemic side effects or serious AEs. However, local tolerability was insufficient for continuation. (C) 2021 Published by Elsevier Ltd on behalf of Osteoarthritis Research Society International.

Published

2022

15. An exploratory first-in-man study to investigate the pharmacokinetics and safety of liposomal dexamethasone at a 2- and 1-week interval in patients with metastatic castration resistant prostate cancer

Author

Josephina P.M. Vrouwe, Michiel J van Esdonk, Gabri van der Pluijm, Susanne Osanto, Josbert M. Metselaar, Jacobus Burggraaf, Ingrid M C Kamerling, and Frederik E. Stuurman

Subjects

Male, liposomes, medicine.medical_specialty, Urology, Bone Neoplasms, dexamethasone, RM1-950, Adenocarcinoma, Prostate cancer, Drug Delivery Systems, Pharmacokinetics, Medicine, Humans, Dosing, General Pharmacology, Toxicology and Pharmaceutics, Adverse effect, Dexamethasone, Aged, First-in-man study, business.industry, metastatic castration resistant prostate cancer, Original Articles, Middle Aged, medicine.disease, Clinical trial, Prostatic Neoplasms, Castration-Resistant, Neurology, Toxicity, Original Article, Therapeutics. Pharmacology, business, medicine.drug

Abstract

Dexamethasone has antitumor activity in metastatic castration resistant prostate cancer (mCRPC). We aimed to investigate intravenous liposome‐encapsulated dexamethasone disodium phosphate (liposomal dexamethasone) administration in mCRPC patients. In this exploratory first‐in‐man study, patients in part A received a starting dose of 10 mg followed by five doses of 20 mg liposomal dexamethasone at 2‐week intervals. Upon review of part A safety, patients in part B received 10 weekly doses of 18.5 mg. Primary outcomes were safety and pharmacokinetic profile, secondary outcome was antitumor efficacy. Nine mCRPC patients (5 part A, 4 part B) were enrolled. All patients experienced grade 1–2 toxicity, one (part B) patient experienced grade 3 toxicity (permanent bladder catheter‐related urosepsis). No infusion‐related adverse events occurred. One patient had upsloping glucose levels ≤9.1 mmol/L. Trough plasma concentrations of liposomal‐ and free dexamethasone were below the lower limit of quantification (LLOQ) in part A, and above LLOQ in three patients in part B (t 1/2 ~50 h for liposomal dexamethasone), trough concentrations of liposomal‐ and free dexamethasone increased toward the end of the study. In seven of nine patients (78%) patients, stable disease was observed in bone and/or CT scans at follow‐up, and in one (part B) of these seven patients a >50% PSA biochemical response was observed. Bi‐ and once weekly administrations of IV liposomal dexamethasone were well‐tolerated. Weekly dosing enabled trough concentrations of liposomal‐ and free dexamethasone >LLOQ. The data presented support further clinical investigation in well‐powered studies. Clinical trial registration: ISRCTN 10011715., This trial is the first to report pharmacokinetic profile, safety and efficacy outcomes using weekly and bi‐weekly IV administered liposomal dexamethasone in mCRPC. Liposomal dexamethasone was well toleratedDutch Healthcare Institute. Systemic corticosteroids. Farmacotherapeutisch kompas. Consulted 2020. DD and considerably prolonged plasma half‐life of dexamethasone. Additional study is needed to determine targeting and patient outcomes with this regimen.

Published

2021

16. Prevalent levels of RSV serum neutralizing antibodies in healthy adults outside the RSV-season

Author

Pauline Verdijk, Meta Roestenberg, Ingrid M C Kamerling, Emilie M. J. van Brummelen, Johan L. van der Plas, Rienk E. Jeeninga, and Jacobus Burggraaf

Subjects

Adult, viruses, 030231 tropical medicine, Immunology, Short Report, Respiratory Syncytial Virus Infections, Respiratory syncytial virus, Antibodies, Viral, Virus, 03 medical and health sciences, 0302 clinical medicine, Healthy volunteers, Respiratory Syncytial Virus Vaccines, Immunology and Allergy, Medicine, Humans, neutralizing antibodies, 030212 general & internal medicine, Respiratory system, Pharmacology, biology, business.industry, Immunogenicity, vaccines, Antibodies, Neutralizing, Clinical research, healthy volunteers, Respiratory Syncytial Virus, Human, biology.protein, Seasons, Antibody, live-attenuated, business, controlled human infection model, Research Article

Abstract

One of the main challenges in early clinical research with respiratory syncytial virus (RSV) live-attenuated vaccines (LAVs) is to assess immunogenicity in healthy adults. Healthy adults will have preexisting levels of serum neutralizing antibodies that could prematurely neutralize the LAV and underestimate the potential effect of the vaccine on the immune system. Data on prevalence and distribution of virus neutralizing titers (VNTs) in healthy adults is limited and there is no absolute threshold for protection against RSV-infection that can serve as an eligibility criterion in early phase trials. We assessed the RSV-specific serum VNT in healthy adults outside the Dutch RSV-Season in two clinical studies performed in 2017 (exploratory study, n = 100) and 2018 (first-in-human LAV-study, n = 190) using the same neutralizing assay. Our findings show that the prevalence and distribution of serum VNT was overall consistent in the two clinical studies. Log2 VNTs were normally distributed, distributions of VNTs were similar and there was no statistical difference in mean log2 VNT for both studies (p = .3). Serum VNTs were comparable during the 6 months of screening in the FIH LAV-study. Our findings will help to determine a cutoff serum VNT to be used as an eligibility criterion in future early phase clinical trials.

Published

2019

17. Effect of Food on the Pharmacokinetics of 2 Formulations of DRL-17822, a Novel Selective Cholesteryl Ester Transfer Protein (CETP) Inhibitor, in Healthy Males

Author

Rajinder Kumar, Rajesh Gandhi, Ingrid M C Kamerling, Marieke L. de Kam, Anirudh Gautam, Bijay Kumar Padhi, Jasper Stevens, Kulkarni Swati, Rajeev Singh Raghuvanshi, Shanavas Alikunju, Jacobus Burggraaf, and Annelieke C. Kruithof

Subjects

Adult, Male, cholesteryl ester transfer protein (CETP) inhibition, Adolescent, Drug Compounding, Pharmaceutical Science, Administration, Oral, Tetrazoles, 030226 pharmacology & pharmacy, 03 medical and health sciences, Food-Drug Interactions, Young Adult, 0302 clinical medicine, Pharmacokinetics, Cholesterylester transfer protein, food effect, Medicine, Humans, Pharmacology (medical), Food science, CETP inhibitor, Triglycerides, amorphous solid dispersion formulation, Cross-Over Studies, biology, business.industry, Cholesterol, HDL, Cholesterol, LDL, Middle Aged, DRL-17822, Crossover study, Dietary Fats, Healthy Volunteers, Amorphous solid, Cholesterol Ester Transfer Proteins, Nanocrystal, 030220 oncology & carcinogenesis, Area Under Curve, biology.protein, Quinolines, nanocrystal formulation, Dispersion (chemistry), business, pharmacokinetics, Lipoprotein

Abstract

DRL-17822 is a novel selective cholesteryl ester transfer protein inhibitor that showed an increased exposure, including an increase of >20-fold of maximum concentration and area under the plasma concentration-time curve from time zero to the time of the last quantifiable concentration, following a high-fat breakfast using a nanocrystal formulation. To reduce this effect of food, we generated an amorphous solid dispersion formulation. In this study, we compared the food effect of both formulations of DRL-17822 in a 2-part randomized, open-label, 4-way crossover study involving healthy adult males 18-45 years of age. In both parts of the study, 12 subjects received both formulations of DRL-17822 in both the fasted and fed states; a low-fat breakfast was provided in the first part and a high-fat breakfast in the second part. Compared to the nanocrystal formulation, the amorphous solid dispersion formulation substantially increased DRL-17822 exposure in the fasted state, including increased maximum concentration, area under the plasma concentration-time curve from time zero to the time of the last quantifiable concentration, and area under plasma concentration-time curve from time zero to infinity. Following a high-fat breakfast, DRL-17822 exposure was increased to a lesser extent in the amorphous solid dispersion formulation compared to the nanocrystal formulation (P < .001). Moreover, compared to the nanocrystal formulation the amorphous solid dispersion formulation caused a more pronounced increase in high-density lipoprotein in the fasted state. Consuming breakfast increased the effect of DRL-17822 on high-density lipoprotein. Taken together, our results indicate that by improving its formulation, DRL-17822 has a favorable exposure profile and therefore a more predictable food effect profile.

Published

2019

18. A novel sustained‐release cysteamine bitartrate formulation for the treatment of cystinosis: Pharmacokinetics and safety in healthy male volunteers

Author

Leo G. J. de Leede, Wouter S. de Vries, N.B. Klarenbeek, Hans Waals, Kirsten R. Bergmann, Saco J. de Visser, Vincent van der Wel, Ingrid M. C. Kamerling, Michiel J van Esdonk, Frans de Loos, Jacobus Burggraaf, Lisa Pagan, Matthijs Moerland, Hans Büller, and Cécile L. Berends

Subjects

cystagon, Adult, Male, Cysteamine Bitartrate, Cysteamine, Population, Cystinosis, RM1-950, Pharmacology, 030226 pharmacology & pharmacy, compliance, Dosage form, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Pharmacokinetics, medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, education, Adverse effect, Cystine Depleting Agents, Netherlands, education.field_of_study, Cross-Over Studies, business.industry, Original Articles, medicine.disease, Healthy Volunteers, Neurology, Tolerability, chemistry, sustained‐release, 030220 oncology & carcinogenesis, Area Under Curve, Delayed-Action Preparations, Original Article, Therapeutics. Pharmacology, business

Abstract

The strict intake regimen of cysteamine bitartrate formulations, associated with side effects, is a concern for the treatment compliance in cystinosis therapy. Therefore, there is a need for a cysteamine formulation with an improved pharmacokinetic profile. This study investigated the pharmacokinetics, safety and tolerability of a new sustained‐release cysteamine dosage form, PO‐001, in healthy volunteers. This was a randomized, investigator‐blinded, three‐way cross‐over study to compare single doses (600 mg) of PO‐001 with Cystagon® (immediate‐release) and Procysbi® (delayed‐release). Collected blood samples were analyzed for plasma cysteamine concentrations and pharmacokinetic parameters were estimated by noncompartmental analysis. In addition, plasma cysteamine concentrations were analyzed using a population pharmacokinetic approach using NONMEM®. Pharmacokinetics showed clear sustained‐release characteristics of PO‐001 over time with a lower C max and longer T max compared to Cystagon® and Procysbi®. All treatment‐emergent adverse events were of mild severity, with the exception of two subjects who reported moderate severity gastrointestinal problems including vomiting and diarrhea, which were related to Cystagon® intake. Population PK simulations showed a favourable PK profile based on C max and C trough concentrations at steady state. In conclusion, a single dose of 600 mg PO‐001 was well tolerated with no findings of clinical concern. This new cysteamine bitartrate formulation showed pharmacokinetics of a sustained‐release formulation, which may be beneficial for the treatment of cystinosis patients. This study supports advancing this type of sustained‐release formulation into a subsequent study to confirm reduced dosing frequency with efficient control of white blood cells (WBCs) cystine levels. Netherlands Trial Registry (NTR) (NL67638.056.18)., PO‐001 showed clear sustained‐release characteristics with a favourable pharmacokinetic profile based on the t max, and both C max and C trough concentrations PO‐001 could be an advanced treatment for cystinosis patients.

Published

2021

19. Safety, tolerability and pharmacokinetic characterisation of DACRA KBP-042 in healthy male subjects

Author

Raj Kumar, Karen Broekhuizen, Ingrid M C Kamerling, Marlous R. Dillingh, Jacobus Burggraaf, Wadim M I de Boon, Marieke de Kam, Asger Reinstrup Bihlet, Kim Henriksen, Morten A. Karsdal, and Claus Christiansen

Subjects

Agonist, Calcitonin, Male, medicine.drug_class, Nausea, Amylin, Pharmacology, Placebo, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Pharmacokinetics, Weight loss, medicine, Humans, Pharmacology (medical), 030212 general & internal medicine, Calcitonin receptor, Amylin Receptor Agonists, Dose-Response Relationship, Drug, business.industry, Receptors, Calcitonin, Tolerability, Vomiting, medicine.symptom, business

Abstract

There is a need for anti-diabetic agents successfully targeting insulin sensitivity and treating obesity control at the same time. The aim of this first-in-human study was 1) to evaluate safety and tolerability; 2) to evaluate pharmacokinetics and 3) to assess indications of receptor engagement of single ascending doses of KBP-042, a Dual Amylin and Calcitonin Receptor Agonists (DACRA) that has shown promising preclinical data, with superior activity in terms of typical amylin-induced responses including reduction of food intake, weight loss and gluco-regulatory capacities. A randomised double-blind placebo-controlled single ascending dose study was performed with six dose levels of KBP-042 (5, 7.5, 10, 20, 20 evening and 40µg) in healthy male adults. KBP-042 or placebo was administered as a single dose after an overnight fast, followed by a standardized lunch after four hours. KBP-042 was associated with dose-dependent complaints of nausea and vomiting, with a lack of tolerability at doses of 20µg and above. Doses of 5 to 40 μg KBP-042 were behaved according to a linear pharmacokinetic profile. Indications of target receptor engagement were observed at the level of glucose control and lowering of bone resorption, compared to placebo. The results of this study showed that doses up to 40 μg were safe, although tolerability was not present at the highest doses. The study confirmed target receptor engagement at the studied doses.

Published

2021

20. Assessment of Risks Associated With Severe Acute Respiratory Syndrome Coronavirus 2 Experimental Human Infection Studies

Author

Ingrid M C Kamerling, Meta Roestenberg, Frits R. Rosendaal, Vincent P. Kuiper, and Leonardus Gerardus Visser

Subjects

Microbiology (medical), medicine.medical_specialty, Isolation (health care), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Secondary infection, 030204 cardiovascular system & hematology, medicine.disease_cause, Viewpoints Article, Disease Outbreaks, 03 medical and health sciences, 0302 clinical medicine, Medicine, Humans, 030212 general & internal medicine, Intensive care medicine, Risk management, Coronavirus, human challenge model, business.industry, SARS-CoV-2, Outbreak, COVID-19, risk assessment, Residual risk, Infectious Diseases, AcademicSubjects/MED00290, business, Risk assessment, controlled human infection model

Abstract

Controlled human infection (CHI) models for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) have been proposed as a tool to accelerate the development of vaccines and drugs. Such models carry inherent risks. Participants may develop severe disease or complications after deliberate infection. Prolonged isolation may negatively impact their well-being. Through secondary infection of study personnel or participant household contacts, the experimental virus strain may cause a community outbreak. We identified risks associated with such a SARS-CoV-2 CHI model and assessed their likelihood and impact and propose strategies that mitigate these risks. In this report, we show that risks can be minimized with proper risk mitigation strategies; the residual risk, however, should be weighed carefully against the scientific and social values of such a CHI model.

Published

2020

21. The optimal imaging window for dysplastic colorectal polyp detection using c-met-targeted fluorescence molecular endoscopy

Author

Marieke L. de Kam, Arend Karrenbeld, Jessie Westerhof, Iris Schmidt, Jan J. Koornstra, Ingrid M C Kamerling, Wouter B. Nagengast, F. J. Voskuil, James C. H. Hardwick, Steven J de Jongh, Dominic J. Robinson, Josephina P.M. Vrouwe, Jacobus Burggraaf, Otorhinolaryngology and Head and Neck Surgery, and Guided Treatment in Optimal Selected Cancer Patients (GUTS)

Subjects

Adenoma, Male, medicine.medical_specialty, Colorectal cancer, Population, Colonic Polyps, colorectal cancer, Colorectal adenoma, Gastroenterology, Fluorescence spectroscopy, 03 medical and health sciences, 0302 clinical medicine, In vivo, Internal medicine, EMI-137 targeting c-Met, Fluorescence microscope, medicine, Humans, Radiology, Nuclear Medicine and imaging, fluorescence molecular endoscopy, education, 030304 developmental biology, Aged, colorectal polyp detection, 0303 health sciences, education.field_of_study, business.industry, Colonoscopy, Middle Aged, Proto-Oncogene Proteins c-met, medicine.disease, optimal imaging window, Spectrometry, Fluorescence, Colorectal Polyp, 030211 gastroenterology & hepatology, Histopathology, Female, business, Colorectal Neoplasms, HT29 Cells

Abstract

Fluorescence molecular endoscopy (FME) is an emerging technique that has the potential to improve the 22% colorectal polyp detection miss-rate. We determined the optimal dose-to-imaging interval and safety of FME using EMI-137, a c-Met-targeted fluorescent peptide, in a population at high risk for colorectal cancer. Methods: We performed in vivo FME and quantification of fluorescence by multidiameter single-fiber reflectance/single-fiber fluorescence spectroscopy in 15 patients with a dysplastic colorectal adenoma. EMI-137 was intravenously administered (0.13 mg/kg) at a 1-, 2- or 3-h dose-to-imaging interval (n = 3 patients per cohort). Two cohorts were expanded to 6 patients on the basis of target-to-background ratios. Fluorescence was correlated to histopathology and c-Met expression. EMI-137 binding specificity was assessed by fluorescence microscopy and in vitro experiments. Results: FME using EMI-137 appeared to be safe and well tolerated. All dose-to-imaging intervals showed significantly higher fluorescence in the colorectal lesions than in surrounding tissue, with a target-to-background ratio of 1.53, 1.66, and 1.74 for the 1-, 2-, and 3-h cohorts, respectively, and a mean intrinsic fluorescence of 0.035 vs. 0.023 mm-1 (P < 0.0003), 0.034 vs. 0.021 mm-1 (P < 0.0001), and 0.033 vs. 0.019 mm-1 (P < 0.0001), respectively. Fluorescence correlated with histopathology on a macroscopic and microscopic level, with significant c-Met overexpression in dysplastic mucosa. In vitro, a dose-dependent specific binding was confirmed. Conclusion: FME using EMI-137 appeared to be safe and feasible within a 1- to 3-h dose-to-imaging interval. No clinically significant differences were observed among the cohorts, although a 1-h dose-to-imaging interval was preferred from a clinical perspective. Future studies will investigate EMI-137 for improved colorectal polyp detection during screening colonoscopies.

Published

2020

22. How to expedite early-phase SARS-CoV-2 vaccine trials in pandemic setting- a practical perspective

Author

Meta Roestenberg, Adam F. Cohen, Johan L. van der Plas, and Ingrid M C Kamerling

Subjects

Pharmacology, 2019-20 coronavirus outbreak, Clinical Trials as Topic, COVID-19 Vaccines, Coronavirus disease 2019 (COVID-19), business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Perspective (graphical), Editorials, COVID-19, Virology, Editorial, Pandemic, Medicine, Humans, Pharmacology (medical), Early phase, business, Pandemics

Published

2020

23. The effect of food and formulation on the population pharmacokinetics of cholesteryl ester transferase protein inhibitor DRL-17822 in healthy male volunteers

Author

Annelieke C. Kruithof, Shanavas Alikunju, Anirudh Gautam, Jasper Stevens, Sebastiaan C. Goulooze, Ingrid M. C. Kamerling, Jacobus Burggraaf, and Groningen Kidney Center (GKC)

Subjects

Male, HDL, Short Report, Administration, Oral, Biological Availability, Tetrazoles, Absorption (skin), Pharmaceutical formulation, 030226 pharmacology & pharmacy, food/drug interaction, 03 medical and health sciences, chemistry.chemical_compound, Food-Drug Interactions, 0302 clinical medicine, Pharmacokinetics, population pharmacokinetics, Transferases, Transferase, Humans, Pharmacology (medical), 030212 general & internal medicine, CETP inhibitor, Pharmacology, drug interaction, Chromatography, Cross-Over Studies, Chemistry, cardiovascular, food, digestive, oral, and skin physiology, Drug interaction, Healthy Volunteers, Bioavailability, cholesteryl ester transferase protein inhibitor, Pharmaceutical Preparations, Cholesteryl ester, Quinolines, Cholesterol Esters

Abstract

We aimed to characterise the population pharmacokinetics of cholesteryl ester transferase protein inhibitor DRL-17822 in healthy males and explore the effect of food and formulation on the oral absorption of DRL-17822 in 4 phase I studies. DRL-17822 was dosed orally (2-1000 mg) in 2 different drug formulations (nanocrystal formulation and amorphous solid dispersion formulation) after either an overnight fast, or a low-fat, continental or high-fat breakfast. A 2-compartment model with 6 transit absorption compartments best characterised the data. Additionally, a strong interaction of food and formulation on bioavailability was observed and parsimoniously characterised in the model by binning combinations of food state and formulation with similar bio-availabilities. The final model adequately characterised the pharmacokinetic data of DRL-17822 in healthy males including the complex interaction of food and drug formulation. The amorphous solid dispersion formulation has a lower food effect on bioavailability compared with the nanocrystal formulation.

Published

2019

24. The Oral Pheneticillin Absorption Test: An Accurate Method to Identify Patients with Inadequate Oral Pheneticillin Absorption

Author

Jaap T. van Dissel, Jacobus Burggraaf, D. M. Kweekel, Ingrid M C Kamerling, Michiel J van Esdonk, and Anneke C. Dijkmans

Subjects

0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Malabsorption, medicine.drug_class, 030106 microbiology, Antibiotics, Absorption (skin), Biochemistry, Microbiology, Gastroenterology, Treatment failure, 03 medical and health sciences, oral, streptococcal, Internal medicine, medicine, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, Oral therapy, pheneticillin, business.industry, Brief Report, lcsh:RM1-950, food and beverages, medicine.disease, Pheneticillin, Penicillin, stomatognathic diseases, 030104 developmental biology, Infectious Diseases, lcsh:Therapeutics. Pharmacology, penicillin, business, STREPTOCOCCAL INFECTIONS, medicine.drug

Abstract

Severe streptococcal infections are commonly treated with intravenous followed by oral penicillin (pheneticillin) therapy. However, switching from iv to oral therapy is complicated by the variability in oral pheneticillin absorption. We employed an Oral Absorption Test (OAT) for pheneticillin to identify patients in whom oral pheneticillin absorption is poor. Out of 84 patients 30 patients (36%) were identified as insufficient absorbers. Treatment failure due to pheneticillin malabsorption can be avoided by performing an OAT, and these patients should be treated by another antibiotic, which is known to be absorbed well.

Published

2019

25. Corrigendum: Controlled Human Infections As a Tool to Reduce Uncertainty in Clinical Vaccine Development

Author

Saco J. de Visser, Ingrid M. C. Kamerling, and Meta Roestenberg

Subjects

medicine.medical_specialty, clinical development, media_common.quotation_subject, 030231 tropical medicine, malaria, Review, low-income access, Scarcity, 03 medical and health sciences, 0302 clinical medicine, Order (exchange), vaccine, Medicine, 030212 general & internal medicine, Market value, Set (psychology), Intensive care medicine, Reimbursement, media_common, lcsh:R5-920, Malaria vaccine, business.industry, Public health, Correction, General Medicine, medicine.disease, product development (PD) process, Risk analysis (engineering), lcsh:Medicine (General), business, Malaria

Abstract

Vaccines can be extremely cost-effective public health measures. Unfortunately the research and development (R&D) of novel vaccines is suffering from rising costs and declining success rates. Because many vaccines target low- and middle income markets (LMIC), output needs to be maintained at a constrained budget. In addition, scientific neglect and political uncertainty around reimbursement decisions make it an unattractive arena for private investors. The vaccine development pipeline for LMIC thus is in need for a different, sustainable, and cost-effective development model. In conventional vaccine development, objectives for every clinical development phase have been predefined. However, given the scarcity of resources, the most efficient clinical development path should identify vaccine candidates with the highest potential impact as soon as possible. We argue for a custom-made question-based development path based on the scientific questions, success probabilities and investments required. One question can be addressed by several studies and one study can provide partial answers to multiple questions. An example of a question-based approach is the implementation of a controlled human malaria infection model (CHMI). Malaria vaccine R&D faces major scientific challenges and has limited resources. Therefore, early preliminary efficacy data needs to be obtained in order to reallocate resources as efficiently as possible and reduce clinical development costs. To meet this demand, novel malaria vaccines are tested for efficacy in so-called CHMI trials in which small groups of healthy volunteers are vaccinated and subsequently infected with malaria. Early evaluation studies of critical questions, such as CHMI, are highly rewarding, since they prevent expenditures on projects that are unlikely to succeed. Each set of estimated probabilities and costs (combined with market value) will have its own optimal priority sequence of questions to address. Algorithms can be designed to determine the optimal order in which questions should be addressed. Experimental infections of healthy volunteers is an example of how a question-based approach to vaccine development can be implemented and has the potential to change the arena of clinical vaccine development.

Published

2019

26. Levofloxacin-Induced QTc Prolongation Depends on the Time of Drug Administration

Author

W. Birkhoff, Jacobus Burggraaf, Ingrid M. C. Kamerling, Jasper Stevens, Meindert Danhof, V. Gotta, Johanna H. Meijer, and Laura Kervezee

Subjects

QTC PROLONGATION, business.industry, Confounding, 030204 cardiovascular system & hematology, 030226 pharmacology & pharmacy, QT interval, Crossover study, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Levofloxacin, Modeling and Simulation, Anesthesia, Heart rate, medicine, Pharmacology (medical), Dosing, business, medicine.drug

Abstract

Understanding the factors influencing a drug's potential to prolong the QTc interval on an electrocardiogram is essential for the correct evaluation of its safety profile. To explore the effect of dosing time on drug-induced QTc prolongation, a randomized, crossover, clinical trial was conducted in which 12 healthy male subjects received levofloxacin at 02:00, 06:00, 10:00, 14:00, 18:00, and 22:00. Using a pharmacokinetic-pharmacodynamic (PK-PD) modeling approach to account for variations in PKs, heart rate, and daily variation in baseline QT, we find that the concentration-QT relationship shows a 24-hour sinusoidal rhythm. Simulations show that the extent of levofloxacin-induced QT prolongation depends on dosing time, with the largest effect at 14:00 (1.73 (95% prediction interval: 1.56-1.90) ms per mg/L) and the smallest effect at 06:00 (-0.04 (-0.19 to 0.12) ms per mg/L). These results suggest that a 24-hour variation in the concentration-QT relationship could be a potentially confounding factor in the assessment of drug-induced QTc prolongation.

Published

2016

27. Colistin methanesulfonate infusion solutions are stable over time and suitable for home administration

Author

Jasper Stevens, Annelies J van Velzen, Daan J Touw, Richard C J M van Rossen, Anneke C. Dijkmans, Titiaan E. Post, Harry G.M. Heijerman, Jacobus Burggraaf, Ingrid M C Kamerling, Erik B Wilms, Groningen Kidney Center (GKC), Nanomedicine & Drug Targeting, Biopharmaceuticals, Discovery, Design and Delivery (BDDD), Groningen Research Institute for Asthma and COPD (GRIAC), Critical care, Anesthesiology, Peri-operative and Emergency medicine (CAPE), and Medicinal Chemistry and Bioanalysis (MCB)

Subjects

0301 basic medicine, PHARMACOKINETICS, Cystic Fibrosis, Home administration, medicine.medical_treatment, 030106 microbiology, Short Report, Infusion bags, Shelf life, 030226 pharmacology & pharmacy, Colistin methanesulfonate (CMS), 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, health services administration, COLISTIMETHATE SODIUM, medicine, General Pharmacology, Toxicology and Pharmaceutics, Saline, health care economics and organizations, Chromatography, STABILITY, Chemistry, Infusion solution, Colistin, CMS, IV administration, Dilution, Elastomeric infusion pums, Anesthesia, Colistimethate Sodium, medicine.drug

Abstract

The stability of colistin methanesulfonate (CMS) was determined in quadruplicate in elastomeric home infusion pumps containing 1, 2 or 3 MU CMS and in infusion bags with 2 MU CMS all in 100 mL normal saline. Infusions were stored at room temperature (20 degrees C-24 degrees C) with or without exposure to natural light or refrigerated (4 degrees C-8 degrees C) and protected from light up to 2 weeks. In the initial solution of 2 MU CMS in 100 mL saline sampled immediately after reconstitution and dilution, 1.5% of CMS was hydrolysed to colistin. When stored at room temperature and exposed to natural light, colistin concentration in elastomeric infusion pumps increased to 2.6% in 8 days and to 2.1% when stored at 4 degrees C. CMS stability increases at lower temperatures and higher concentrations. Based on the current data, chemical stability of CMS infusion solution is sufficient for a shelf life of 7 days refrigerated plus 1 day at room temperature.

Published

2018

28. Fosfomycin as a potential therapy for the treatment of systemic infections

Author

Natalia Veneranda Ortiz Zacarías, Johan W. Mouton, Erik B Wilms, Jacobus Burggraaf, Daan J Touw, Ingrid M C Kamerling, Cees van Nieuwkoop, Anneke C. Dijkmans, Jasper Stevens, Medical Microbiology & Infectious Diseases, Erasmus MC other, Nanomedicine & Drug Targeting, Biopharmaceuticals, Discovery, Design and Delivery (BDDD), Groningen Research Institute for Asthma and COPD (GRIAC), Critical care, Anesthesiology, Peri-operative and Emergency medicine (CAPE), Groningen Kidney Center (GKC), and Medicinal Chemistry and Bioanalysis (MCB)

Subjects

0301 basic medicine, MULTIDRUG-RESISTANT BACTERIA, Administration, Oral, Pharmacology, 0302 clinical medicine, population pharmacokinetics, Drug Resistance, Multiple, Bacterial, Medicine, 030212 general & internal medicine, General Pharmacology, Toxicology and Pharmaceutics, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), fosfomycin, education.field_of_study, Fosfomycin Tromethamine, fosfomycin tromethamine, simulation, Anti-Bacterial Agents, multi‐drug resistant, Treatment Outcome, Neurology, PHOSPHONOMYCIN, Original Article, KLEBSIELLA-PNEUMONIAE, CRITICALLY-ILL PATIENTS, medicine.drug, INTRAVENOUS FOSFOMYCIN, multi-drug resistant, 030106 microbiology, Population, ANTIMICROBIAL SUSCEPTIBILITY, Microbial Sensitivity Tests, Fosfomycin, Models, Biological, Drug Administration Schedule, URINARY-TRACT-INFECTIONS, 03 medical and health sciences, Minimum inhibitory concentration, All institutes and research themes of the Radboud University Medical Center, Pharmacokinetics, Sepsis, Escherichia coli, Humans, Dosing, education, Dose-Response Relationship, Drug, business.industry, TROMETAMOL, ANTIBIOTIC-RESISTANCE, Original Articles, systemic infections, Regimen, lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], Pharmacodynamics, Feasibility Studies, PENETRATION, business

Abstract

Fosfomycin has emerged as a potential therapy for multidrug‐resistant bacterial infections. In most European countries, the oral formulation is only approved as a 3 g single dose for treatment of uncomplicated cystitis. However, for the treatment of complicated systemic infections, this dose regimen is unlikely to reach efficacious serum and tissue concentrations. This study aims to investigate different fosfomycin‐dosing regimens to evaluate its rationale for treatment of systemic infections. Serum concentration‐time profiles of fosfomycin were simulated using a population pharmacokinetic model based on published pharmacokinetic parameter values, their uncertainty, inter‐individual variability and covariates. The model was validated on published data and used to simulate a wide range of dosing regimens for oral and intravenous administration of fosfomycin. Finally, based on the minimum inhibitory concentration for E. coli, surrogate pharmacodynamic indices were calculated for each dosing regimen. This is the first population pharmacokinetic model to describe the oral pharmacokinetics of fosfomycin using data from different literature sources. The model and surrogate pharmacodynamic indices provide quantitative evidence that a dosing regimen of 6–12 g per day divided in 3 doses is required to obtain efficacious exposure and may serve as a first step in the treatment of systemic multi‐drug‐resistant bacterial infections.

Published

2018

29. Colistin

Author

Natalia V. Ortiz-Zacarias, Ingrid M C Kamerling, Erik B Wilms, Henri A. Verbrugh, Cees van Nieuwkoop, Anneke C. Dijkmans, Daan J Touw, W. Birkhoff, and Medical Microbiology & Infectious Diseases

Subjects

INTENSIVE-CARE-UNIT, Gram-negative bacteria, medicine.drug_class, Polymyxin, Antibiotics, Polymyxin Antibiotic, Microbial Sensitivity Tests, Drug resistance, Biology, Pharmacology, medicine.disease_cause, Microbiology, Minimum inhibitory concentration, Drug Resistance, Multiple, Bacterial, COLISTIMETHATE SODIUM, Gram-Negative Bacteria, INTRAVENOUS COLISTIN, medicine, Humans, Pharmacology (medical), Colistin, Pseudomonas aeruginosa, PSEUDOMONAS-AERUGINOSA, Drug Synergism, POPULATION PHARMACOKINETICS, biology.organism_classification, Anti-Bacterial Agents, RESISTANT ACINETOBACTER-BAUMANNII, lipids (amino acids, peptides, and proteins), CONTINUOUS VENOVENOUS HEMODIAFILTRATION, LIQUID-CHROMATOGRAPHY, Drug Monitoring, CRITICALLY-ILL PATIENTS, medicine.drug

Abstract

Colistin (polymyxin E) is a positively charged deca-peptide antibiotic that disrupts the integrity of the outer membrane of the cell wall of gram-negative bacteria by binding to the lipid A moiety of lipopolysaccharides, resulting in cell death. The endotoxic activity of lipopolysaccharides is simultaneously inhibited. Colistin is increasingly being prescribed as rescue treatment for infections with multidrug-resistant bacilli. Nephrotoxicity and, to a lesser degree, neurotoxicity occur often during systemic colistin therapy, and have severely limited its application in the past. However, these side effects are largely reversible and can be managed through close monitoring. The prodrug colistimethate sodium (CMS) is less toxic and is, therefore, the preferred formulation for parenteral administration. Importantly, resistance to colistin seems to emerge often unless it is combined with another antibiotic, but further studies into this phenomenon are necessary. Pharmacokinetic and pharmacodynamic properties have received little attention, partly because of the physicochemical peculiarities of polymyxin antibiotics, especially their propensity to stick to other molecules and surfaces. The ratio between the area under the curve of free colistin and the pathogen's Minimal Inhibitory Concentration (MIC) best predicts microbiological and clinical responses, but more studies are needed in this area. Likewise, further standardization is needed in production and labeling of colistin formulations, and in the way the susceptibility of bacteria to colistin is determined.

Published

2015

30. Fosfomycin: Pharmacological, Clinical and Future Perspectives

Author

Johan W. Mouton, Jasper Stevens, Natalia Veneranda Ortiz Zacarías, Anneke C. Dijkmans, Jacobus Burggraaf, Ingrid M C Kamerling, Daniël J. Touw, Erik B Wilms, Cees van Nieuwkoop, and Medical Microbiology & Infectious Diseases

Subjects

0301 basic medicine, Microbiology (medical), MULTIDRUG-RESISTANT BACTERIA, INFECTIOUS-DISEASES SOCIETY, medicine.drug_class, IN-VITRO ACTIVITY, ANTIMICROBIAL SUSCEPTIBILITY, 030106 microbiology, Antibiotics, Review, Pharmacology, Biology, Fosfomycin, medicine.disease_cause, STREPTOMYCES-WEDMORENSIS, ACINETOBACTER-BAUMANNII, Biochemistry, Microbiology, URINARY-TRACT-INFECTIONS, 03 medical and health sciences, Pharmacokinetics, Oral administration, multidrug resistance, Journal Article, medicine, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, fosfomycin, antimicrobial activity, Pseudomonas aeruginosa, lcsh:RM1-950, PSEUDOMONAS-AERUGINOSA, Fosfomycin Tromethamine, biochemical phenomena, metabolism, and nutrition, Antimicrobial, Multiple drug resistance, lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], lcsh:Therapeutics. Pharmacology, Infectious Diseases, ESCHERICHIA-COLI, CRITICALLY-ILL PATIENTS, pharmacokinetics, medicine.drug

Abstract

Contains fulltext : 182494.pdf (Publisher’s version ) (Open Access) Fosfomycin is a bactericidal, low-molecular weight, broad-spectrum antibiotic, with putative activity against several bacteria, including multidrug-resistant Gram-negative bacteria, by irreversibly inhibiting an early stage in cell wall synthesis. Evidence suggests that fosfomycin has a synergistic effect when used in combination with other antimicrobial agents that act via a different mechanism of action, thereby allowing for reduced dosages and lower toxicity. Fosfomycin does not bind to plasma proteins and is cleared via the kidneys. Due to its extensive tissue penetration, fosfomycin may be indicated for infections of the CNS, soft tissues, bone, lungs, and abscesses. The oral bioavailability of fosfomycin tromethamine is

Published

2017

31. A Phase I Dose-Escalation and Bioequivalence Study of a Trastuzumab Biosimilar in Healthy Male Volunteers

Author

Jacobus Burggraaf, Joannes A. A. Reijers, Liselijn A. B. Wisman, Gerrit Voortman, Eduard P. M. De Cock, Ingrid M C Kamerling, Sandra van Os, and Marieke L. de Kam

Subjects

Adult, Male, medicine.medical_specialty, Pharmacology, Bioequivalence, Antibodies, Monoclonal, Humanized, Placebo, Gastroenterology, Cohort Studies, Young Adult, Double-Blind Method, Pharmacokinetics, Trastuzumab, Internal medicine, Humans, Medicine, Single-Blind Method, Pharmacology (medical), skin and connective tissue diseases, Adverse effect, Biosimilar Pharmaceuticals, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Headache, General Medicine, Crossover study, Healthy Volunteers, Confidence interval, Therapeutic Equivalency, Geometric mean, business, medicine.drug

Abstract

Trastuzumab (Herceptin®) is a humanized monoclonal antibody targeting the human epidermal growth factor receptor 2 (HER2) and is used in the treatment of HER2-overexpressing breast and gastric cancer. FTMB is being developed as a biosimilar of trastuzumab. In this combined dose-escalation and bioequivalence study of parallel design, the pharmacokinetic profile of FTMB was compared with Herceptin®. Healthy male volunteers received single doses of 0.5, 1.5, 3.0 or 6.0 mg/kg FTMB, or placebo, in consecutive dose-escalation cohorts to assess the safety profile. Thereafter, the 6 mg/kg cohort was expanded to establish bioequivalence between FTMB (Test) and Herceptin® (Reference) based on an acceptance interval of 80.0–125.0 %. In total, 118 subjects were enrolled in the study. The mean area under the concentration–time curve from time zero to infinity (AUC∞) was 1,609 µg·day/mL (Test) and 1,330 µg·day/mL (Reference). The log-transformed geometric mean Test/Reference (T/R) ratio for AUC∞ was 89.6 % (90 % confidence interval [CI] 85.1–94.4), demonstrating bioequivalence. For the secondary endpoint, the maximum concentration observed (C max), the geometric mean T/R ratio was 89.4 % (90 % CI 83.4–95.9). Non-linear, target-mediated pharmacokinetics were also observed. Adverse events other than the documented side effects of Herceptin® (fever, influenza-like illness, and fatigue) did not occur. No signs of cardiotoxicity were observed. This bioequivalence study with a trastuzumab biosimilar in healthy male volunteers demonstrated bioequivalence of FTMB with Herceptin®. FTMB was well tolerated in doses up to 6 mg/kg. Non-linear target elimination was also observed in the pharmacokinetic profile of trastuzumab.

Published

2014

32. Early stage development of the glycine-1 re-uptake inhibitor SCH 900435: central nervous system effects compared with placebo in healthy men

Author

Marieke L. de Kam, Joanna Udo de Haes, Joop M. A. van Gerven, Chris Hogg, Adam F. Cohen, Ingrid M C Kamerling, Marieke Liem-Moolenaar, Graham E. Holder, Pierre Peeters, Huub Jan Kleijn, Edwin Spaans, and Kari L. Franson

Subjects

Pharmacology, medicine.medical_specialty, genetic structures, business.industry, medicine.medical_treatment, Central nervous system, medicine.disease, Placebo, Electrophysiology, Endocrinology, medicine.anatomical_structure, Pharmacokinetics, Schizophrenia, Pharmacodynamics, Visual Disturbance, Internal medicine, medicine, Pharmacology (medical), Antipsychotic, business

Abstract

Aims To report the first three studies with SCH 900435, a selective glycine-1 re-uptake inhibitor in development for treating schizophrenia, using systematic evaluations of pharmacodynamics to understand the observed effects. Methods Three double-blind, placebo-controlled studies (single, visual effect and multiple dose) were performed. In the single and multiple dose study SCH 900435 (0.5–30 mg) was given to healthy males and frequent pharmacokinetic and pharmacodynamic measurements were performed. The visual effects study incorporated visual electrophysiological measures of macular, retinal and intracranial visual pathway function. Results In the single dose study (highest difference, 95% CI, P) increases in smooth pursuit eye movements (8, 12 mg (−6.09, 10.14, −2.04, 0.013), 30 mg), pupil : iris ratio (20 and 30 mg (−0.065, 0.09, −0.04

Published

2013

33. Methods used in clinical development of novel anti-asthma therapies

Author

Ingrid M C Kamerling, Zuzana Diamant, Diderik Boot, and Leif Bjermer

Subjects

Pulmonary and Respiratory Medicine, Drug, medicine.medical_specialty, Exacerbation, media_common.quotation_subject, Anti-Inflammatory Agents, Exacerbation models, Models, Biological, Anti-asthmatic Agent, Bronchoconstrictor Agents, medicine, Humans, Anti-Asthmatic Agents, Intensive care medicine, media_common, Asthma, business.industry, Reproducibility of Results, medicine.disease, respiratory tract diseases, Outcome parameter, Surgery, Clinical trial, Drug development, Early clinical trials, Inflammometry, Bronchial Hyperreactivity, business, Airway, Biomarkers

Abstract

SummaryIn recent years, it has become increasingly important to get as much as possible information on clinical efficacy already in the early phases of drug development. For proof of concept (POC) studies testing novel anti-inflammatory drugs in asthma, there are several validated exacerbation models, inducing various aspects of the airway inflammation and airway responsiveness. The choice of the appropriate asthma model depends on the drug's targets within the inflammatory process.For adequate assessment of the drug's anti-inflammatory potential, it is crucial to choose adequate (surrogate) biomarkers. Ideally, these should include measures of airway response, central and peripheral airway inflammation and airway hyperresponsiveness. Overall, there are validated non-invasive sampling techniques for the measurement of inflammatory markers in asthma that can be applied as outcome parameters in early clinical trials. If adequately implemented, these measurements can provide early indication of proof of pharmacological and potential therapeutic efficacy—even in first administration to humans.

Published

2008

34. Detection of colorectal polyps in humans using an intravenously administered fluorescent peptide targeted against c-Met

Author

James C. H. Hardwick, Philip W. Voorneveld, Marieke L. de Kam, Hans Morreau, Andrew Healey, Roger Bjerke, Andrea J Kales, Ragnar Bendiksen, Paul Gordon, Geir Torheim, Siver Andreas Moestue, Grethe Tang Dalsgaard, Marit Swaerd-Nordmo, Bard Indrevoll, Fijs W. B. van Leeuwen, Ingrid M C Kamerling, Jacobus Burggraaf, Lenneke Schrier, Liv-Ingrid Odegardstuen, Tessa Buckle, Alexandra M. J. Langers, Siavash Yazdanfar, and Madhuri V Warren

Subjects

Male, Pathology, medicine.medical_specialty, C-Met, Colorectal cancer, Molecular Sequence Data, Intestinal polyp, Colonoscopy, Peptide, Peptides, Cyclic, General Biochemistry, Genetics and Molecular Biology, Fluorescence, chemistry.chemical_compound, Mice, Cell Line, Tumor, otorhinolaryngologic diseases, medicine, Animals, Humans, Amino Acid Sequence, chemistry.chemical_classification, Mice, Inbred BALB C, medicine.diagnostic_test, business.industry, Intestinal Polyps, General Medicine, Proto-Oncogene Proteins c-met, medicine.disease, digestive system diseases, Macaca fascicularis, chemistry, Biomarker (medicine), Female, Molecular imaging, business, Colorectal Neoplasms

Abstract

Colon cancer prevention currently relies on colonoscopy using white light to detect and remove polyps, but small and flat polyps are difficult to detect and frequently missed when using this technique. Fluorescence colonoscopy combined with a fluorescent probe specific for a polyp biomarker may improve polyp detection. Here we describe GE-137, a water-soluble probe consisting of a 26-amino acid cyclic peptide that binds the human tyrosine kinase c-Met conjugated to a fluorescent cyanine dye. Intravenous administration of GE-137 leads to its accumulation specifically in c-Met-expressing tumors in mice, and it is safe and well tolerated in humans. Fluorescence colonoscopy in patients receiving intravenous GE-137 enabled visualization of all neoplastic polyps that were visible with white light (38), as well as an additional nine polyps that were not visible with white light. This first-in-human pilot study shows that molecular imaging using an intravenous fluorescent agent specific for c-Met is feasible and safe, and that it may enable the detection of polyps missed by other techniques.

Published

2015

35. Reproducibility of biomarkers in induced sputum and in serum from chronic smokers

Author

Marieke de Kam, Cesar Calderon, Zuzana Diamant, Jacobus Burggraaf, Rob Zuiker, J. Diderik Boot, Nicoletta Morelli, Ingrid M C Kamerling, Adam F. Cohen, Pulmonary medicine, and Other Research

Subjects

Pulmonary and Respiratory Medicine, Serum, EXHALED NITRIC-OXIDE, Adult, Male, AIRWAY INFLAMMATION, Neutrophils, Induced sputum, OBSTRUCTIVE PULMONARY-DISEASE, MARKERS, Medicine, SURFACTANT PROTEIN D, COPD, Humans, Pharmacology (medical), Interleukin 8, Pulmonary surfactant associated protein D, Asthma, Reproducibility, Serum Amyloid A Protein, business.industry, Macrophages, Biochemistry (medical), Interleukin-8, Smoking, Airway inflammation, Sputum, Reproducibility of Results, Middle Aged, medicine.disease, Pulmonary Surfactant-Associated Protein D, respiratory tract diseases, EXACERBATIONS, Immunology, Exhaled nitric oxide, ASTHMA, Female, medicine.symptom, business, CELL COUNTS, Biomarkers, Chronic smokers

Abstract

Rationale: Soluble inflammatory markers obtained from non-invasive airway sampling such as induced sputum may be useful biomarkers for targeted pharmaceutical interventions. However, before these soluble markers can be used as potential targets, their variability and reproducibility need to be established in distinct study populations.Objective: This study aimed to assess the reproducibility of biomarkers obtained from induced sputum and serum in chronic smokers and non-smokers. Method: Sputum and serum samples were obtained from 16 healthy non-smokers and 16 asymptomatic chronic smokers (for both groups: 8M/8F, 30-52 years, FEV1 >= 80% pred.; >= 10 pack years for the smokers) on 2 separate visits 4-10 days apart. Soluble markers in serum and sputum were analysed by ELISA. The differences between smokers vs non-smokers were analysed with a t-test and variability was assessed on log-transformed data by a mixed model ANOVA.Results: Analysable sputum samples could be obtained from all 32 subjects. In both study populations neutrophils and macrophages were the predominant cell types. Serum Pulmonary Surfactant Associated Protein D had favourable reproducibility criteria for reliability ratio (0.99), intra-subject coefficient of variation (11.2%) and the Bland Altman limits of agreement. Furthermore, chronic smokers, compared to non-smokers, had significantly higher sputum concentrations of IL-8 (1094.6 pg/mL vs 460.8 pg/mL, p = 0.006)), and higher serum concentrations of Pulmonary Surfactant Associated Protein D (110.9 pg/mL vs 64.7 pg/mL, p = 0.019), and lower concentrations of Serum Amyloid A (1352.4 pg/mL vs 2297.5 pg/mL, p = 0.022).Conclusion: Serum Pulmonary Surfactant Associated Protein D proved to be a biomarker that fulfilled the criteria for reproducibility in both study groups. (C) 2015 Elsevier Ltd. All rights reserved.

Published

2015

36. Kinetics of TH2 biomarkers in sputum of asthmatics following inhaled allergen

Author

Veronica M. Rivas, Nicoletta Morelli, Ingrid M C Kamerling, Michael Tanen, Rob Zuiker, J. Diderik Boot, Robin Mogg, Marcella Ruddy, Kristien Van Dyck, Inge De Lepeleire, and Zuzana Diamant

Subjects

Pulmonary and Respiratory Medicine, allergen bronchial provocation test, asthma, sputum, Th2 inflammation, fluticasone, medicine.disease_cause, Placebo, Allergen, Medicine, Original Research Article, Asthma, Fluticasone, business.industry, Eosinophil, respiratory system, medicine.disease, Crossover study, respiratory tract diseases, TH2 inflammation, medicine.anatomical_structure, Pharmacodynamics, Immunology, Sputum, medicine.symptom, business, medicine.drug

Abstract

Background : Allergen-induced late airway response offers important pharmacodynamic targets, including T helper 2 (TH2) biomarkers. However, detection of inflammatory markers has been limited in dithiothreitol-processed sputum. Objectives : To test whether allergen-induced TH2 inflammatory markers can be reproducibly quantified by sensitive detection techniques in ultracentrifuged sputum and the effect of fluticasone (FP) on these endpoints. Methods : Thirteen allergic asthmatics with dual allergen-induced airway responses, documented during a single-blind placebo run-in period, participated in a double-blind, two-period crossover study. Each period consisted of three consecutive days, separated by ≥3 weeks. Following randomization, subjects inhaled FP (500 µg bid, five doses total) or placebo. On Day 2 in each study period, allergen challenge was performed and airway response measured by forced expiratory volume in 1 sec (FEV1) until 7 h post-challenge. Sputum was induced 24 h pre-allergen and 7 and 24 h post-allergen. Sputum samples were split into two portions: TH2 biomarkers were quantified by Meso Scale multiplex platform following ultracentrifugation, and cell differentials were counted on Giemsa–May-Grunwald-stained cytospins. Allergen-induced changes in inflammatory endpoints were compared between FP and placebo using a mixed model ANCOVA. Results : Inhaled allergen induced dual airway responses in all subjects during both placebo periods with reproducible late asthmatic response (LAR) and increased sputum inflammatory biomarkers (IL-2, IL-4, IL-13, and eotaxin-1) and eosinophil counts. FP effectively blunted both the LAR and the inflammatory biomarkers. Conclusions : Combining novel, sensitive quantification methods with ultracentrifugation allows reproducible quantification of sputum biomarkers following allergen challenge, reversed by FP. This approach allows non-invasive identification of pharmacodynamic targets for anti-asthma therapies. Keywords : allergen bronchial provocation test; asthma; sputum; TH2 inflammation; fluticasone (Published: 26 May 2015) Citation: European Clinical Respiratory Journal 2015, 2: 28319 - http://dx.doi.org/10.3402/ecrj.v2.28319

Published

2015

37. Gallbladder volume as a biomarker for the motilin effect in healthy volunteers and patients with functional dyspepsia

Author

J. Burggraaf, Ad A.M. Masclee, Ingrid M C Kamerling, M. L. de Kam, A. D. Van Haarst, and Adam F. Cohen

Subjects

education.field_of_study, medicine.medical_specialty, Hepatology, business.industry, Gallbladder, digestive, oral, and skin physiology, Population, Gastroenterology, Placebo, Crossover study, law.invention, Motilin, medicine.anatomical_structure, Randomized controlled trial, law, Internal medicine, Biomarker (medicine), Medicine, Pharmacology (medical), Analysis of variance, education, business, hormones, hormone substitutes, and hormone antagonists

Abstract

Summary Aim : To investigate a motilin effect on gallbladder volume in healthy volunteers and patients with functional dyspepsia. Methods : Forty-three healthy volunteers and 10 patients with functional dyspepsia received motilin (4 pmol.min/kg) or placebo in four separate double-blind, randomized, placebo-controlled, cross-over studies. The gallbladder volume was measured by ultrasonography. Analysis of variance of the combined data of these studies was performed to investigate a motilin effect on gallbladder volume and potential differences between patients and healthy volunteers. Results : The baseline gallbladder volume was similar for placebo and motilin treatment, as well as for patients and healthy volunteers. Motilin, compared with placebo, significantly decreased the gallbladder volume in healthy volunteers (P = 0.003) and patients (P

Published

2004

38. Effects of a nonpeptide motilin receptor antagonist on proximal gastric motor function

Author

Ad A.M. Masclee, Ingrid M C Kamerling, Adam F. Cohen, Aernout D. van Haarst, Marieke L. de Kam, Hartmut Heinzerling, Jacobus Burggraaf, and Rik C. Schoemaker

Subjects

Pharmacology, medicine.medical_specialty, Stomach, Motilin receptor, digestive, oral, and skin physiology, Antagonist, Radioimmunoassay, Distension, Biology, Barostat, Motilin, medicine.anatomical_structure, Endocrinology, Gastrointestinal hormone, Internal medicine, medicine, Pharmacology (medical), hormones, hormone substitutes, and hormone antagonists

Abstract

Aim To assess the effects of the motilin receptor antagonist RWJ-68023 on basal and motilin-stimulated proximal gastric volume. Methods Eighteen healthy male volunteers received RWJ-68023 in two different doses or placebo for 135 min. After 45 min, subjects received a motilin infusion for 90 min. Proximal gastric volume was measured with a barostat at constant pressure and during isobaric distensions. Abdominal symptoms were scored using visual analogue scales. Motilin and RWJ-68023 concentrations were assessed by radioimmunoassay and liquid chromatography-mass spectrometry, respectively. Results Both dosages of RWJ-68023 were safe and well tolerated. The most common adverse events were of gastrointestinal origin. RWJ-68023 did not affect basal proximal gastric volume, but the high-dose RWJ-68023 reduced the contractile effect of motilin on the stomach. This antagonizing effect of RWJ-68023 was only significant (P = 0.014) during the distension procedure. Conclusions The RWJ-68023 doses used in this study were selected to accomplish plasma concentrations that would block the motilin effect entirely. However, the antagonizing effect of RWJ-68023 was partial and only present when the tonic condition of the stomach was modulated by motilin.

Published

2004

39. The effect of motilin on the rectum in healthy volunteers

Author

M. F. Oppenhuizen-Duinker, H. C. Schoemaker, R. Jones, Ad A.M. Masclee, A. D. Van Haarst, Ingrid M C Kamerling, J. Burggraaf, Adam F. Cohen, Hartmut Heinzerling, and Izak Biemond

Subjects

Pharmacology, medicine.medical_specialty, Gastrointestinal agent, business.industry, digestive, oral, and skin physiology, Rectum, Radioimmunoassay, Placebo, Gastroenterology, Crossover study, Barostat, Confidence interval, Motilin, medicine.anatomical_structure, Endocrinology, Internal medicine, medicine, Pharmacology (medical), business, hormones, hormone substitutes, and hormone antagonists

Abstract

Aims The role of motilin in the regulation of upper gastrointestinal (GI) motility is well defined. However, little is known about the effects on the distal GI tract. To investigate the effect of exogenous motilin on rectal function, barostat measurements in the rectum were performed and lower abdominal symptoms were scored. Methods Eight fasted, healthy volunteers were infused intravenously with synthetic motilin or placebo over 90 min in a double-blind, randomized, cross-over design. Rectum volume was measured with a barostat device during constant pressure and during isobaric distensions. Lower abdominal symptoms were scored by visual analogue scales. Plasma motilin concentrations were measured by radioimmunoassay. Results Baseline rectum volumes were similar between treatments: 185 ± 62 mL (motilin) and 136 ± 41 mL (placebo). During the constant pressure procedure, motilin increased rectum volume [area under the effect curve (AUEC)] by 6%[95% confidence interval (CI) −3, 16] of baseline, compared with placebo. During isobaric distensions motilin increased rectum volume (AUEC) by 43 mL (95% CI 0.4, 85; P

Published

2003

40. Motilin effects on the proximal stomach in patients with functional dyspepsia and healthy volunteers

Author

Rik C. Schoemaker, Adam F. Cohen, Izak Biemond, Ad A.M. Masclee, Aernout D. van Haarst, Ingrid M C Kamerling, Richard Jones, Jacobus Burggraaf, and Hartmut Heinzerling

Subjects

Adult, Male, medicine.medical_specialty, Physiology, Gastroenterology, Motilin, Gastrointestinal Agents, Physiology (medical), Internal medicine, Healthy volunteers, medicine, Humans, In patient, Dyspepsia, Proximal stomach, Hepatology, business.industry, Stomach, digestive, oral, and skin physiology, Muscle, Smooth, Nausea, Middle Aged, Barostat, medicine.anatomical_structure, Gastrointestinal hormone, Female, business, hormones, hormone substitutes, and hormone antagonists, Muscle Contraction

Abstract

This study investigates motilin effects on the proximal stomach in patients with functional dyspepsia (FD) and healthy volunteers. Eight healthy volunteers and 12 patients with FD were infused with synthetic motilin or placebo. Proximal gastric volume was measured with a barostat at constant pressure and during isobaric distensions. Abdominal symptoms were scored by visual analog scales. Plasma motilin concentrations were measured by radioimmunoassay. Motilin concentrations and baseline gastric volumes were similar for patients and healthy volunteers. Motilin, compared with placebo, reduced gastric volume by 112 ml [ F(29,195); confidence interval (CI) 95%] in patients and by 96 ml [ F(−7,200); CI 95%] in healthy volunteers. In patients, motilin decreased compliance by 76 ml/mmHg [ F(9,143); CI 95%] compared with placebo, which was similar in volunteers [66 ml/mmHg; F(11,120); CI 95%]. Patients were more nauseous during motilin compared with placebo ( P = 0.04), whereas healthy volunteers did not experience nausea. We conclude that in a fasted condition, FD patients have a similar proximal gastric motor response to motilin as healthy volunteers, but experience an exaggerated sensation of nausea.

Published

2003

41. Dose-related effects of motilin on proximal gastrointestinal motility

Author

Adam F. Cohen, Ad A.M. Masclee, H. C. Schoemaker, Ingrid M. C. Kamerling, Richard Jones, A. D. Van Haarst, Izak Biemond, and J. Burggraaf

Subjects

medicine.medical_specialty, Hepatology, Gastric emptying, business.industry, Stomach, digestive, oral, and skin physiology, Gastroenterology, Peptide hormone, Crossover study, digestive system diseases, Motilin, Contractility, medicine.anatomical_structure, Endocrinology, Gastrointestinal hormone, Internal medicine, Medicine, Pharmacology (medical), business, Antrum, hormones, hormone substitutes, and hormone antagonists

Abstract

Aim: To assess non-invasively the dose–response relations for the effects of exogenous motilin on antrum contraction frequency, gall-bladder volume and gastric myoelectrical activity. Methods: In a double-blind, randomized, placebo-controlled, five-way crossover study, 10 fasted healthy volunteers were infused intravenously with synthetic human motilin (0.5, 1, 2 and 4 pmol.min/kg) or placebo for 60 min. Gall-bladder volume and antrum contractions were assessed by ultrasonography and gastric myoelectrical activity by electrogastrography. Motilin concentrations were measured using a radioimmunoassay. Results: Baseline plasma motilin levels (60 pmol/L) were similar for all treatments. Motilin levels increased upon the start of infusion and rapidly returned to baseline after cessation of the infusion. At motilin doses of 2 and 4 pmol.min/kg, the antrum contraction frequency was significantly augmented, with maximum differences of two contractions per 2-min interval compared to placebo, while no changes in gastric myoelectrical activity were observed. Changes in gall-bladder volume were not significantly different for any of the motilin doses compared to placebo. Conclusions: Motilin increased antrum contraction frequency, whereas no effect on gastric myoelectrical activity was observed. Antrum contraction frequency appears to be a useful biomarker for motilin efficacy, and motilin doses of 2 and 4 pmol.min/kg were equally effective.

Published

2002

42. [Practical guideline for the use of colistin]

Author

Anneke C, Dijkmans, Erik B, Wilms, Ingrid M C, Kamerling, Willem, Birkhoff, Cees, van Nieuwkoop, Henri A, Verbrugh, and Daan J, Touw

Subjects

Gastrointestinal Tract, Cystic Fibrosis, Colistin, Drug Resistance, Multiple, Bacterial, Practice Guidelines as Topic, Pseudomonas aeruginosa, Humans, Drug Therapy, Combination, Pseudomonas Infections, Anti-Bacterial Agents

Abstract

Colistin (polymyxin E) binds to the cell wall of gram-negative bacteria, leading to osmotic destruction of the cell. Since its introduction in 1959, colistin has been little used parenterally due to a high incidence of reversible nephrotoxicity and, to a lesser extent, neurotoxicity. Colistin use remained limited to combating Pseudomonas aeruginosa in cystic fibrosis patients. In addition, oral colistin is part of the recently introduced regime of selective digestive tract decontamination in ICU patients. Intravenous administration of colistin is now increasingly prescribed for the control of multi-resistant microorganisms. Colistin monotherapy, however, rapidly selects resistant subpopulations. Therefore, only combination therapy is advised. The prodrug colistimethate sodium is less toxic and is hydrolyzed in vivo to active colistin; colistin is renally cleared. Clinical practice remains hampered by lack of uniformity and standardization of names, dosage units, dosing recommendations and methods of concentration and susceptibility testing.

Published

2014

43. Efficacy and safety of RPL554, a dual PDE3 and PDE4 inhibitor, in healthy volunteers and in patients with asthma or chronic obstructive pulmonary disease: findings from four clinical trials

Author

Ingrid M C Kamerling, Dave Singh, Domenico Spina, Mario Cazzola, Clive P. Page, Zuzana Diamant, Rob Zuiker, Nicoletta Morelli, Marieke L. de Kam, Lui Franciosi, Luigino Calzetta, Michael J A Walker, Jacobus Burggraaf, Adam F. Cohen, and Katharine H. Banner

Subjects

Male, Settore MED/10 - Malattie dell'Apparato Respiratorio, Phosphodiesterase 3 Inhibitors, Gastroenterology, Pulmonary Disease, Chronic Obstructive, ALLERGEN, Forced Expiratory Volume, Clinical endpoint, Single-Blind Method, Prospective Studies, Prospective cohort study, ANTIASTHMA DRUGS, COPD, Middle Aged, Healthy Volunteers, PHOSPHODIESTERASE-4 INHIBITOR, LUNG-FUNCTION, Treatment Outcome, Inhalation, SELECTIVE PHOSPHODIESTERASE-3, Anesthesia, Administration, Female, medicine.symptom, medicine.drug, Pulmonary and Respiratory Medicine, Adult, medicine.medical_specialty, Chronic Obstructive, Pyrimidinones, ROFLUMILAST, Placebo, Pulmonary Disease, Young Adult, Internal medicine, Isoquinolines, Humans, Aged, Asthma, Nebulizers and Vaporizers, Phosphodiesterase 4 Inhibitors, Follow-Up Studies, Administration, Inhalation, medicine, Adverse effect, business.industry, AIRWAY RESPONSIVENESS, medicine.disease, Sputum, Methacholine, CHALLENGE, business, RESPONSES

Abstract

Many patients with asthma or chronic obstructive pulmonary disease (COPD) routinely receive a combination of an inhaled bronchodilator and anti-inflammatory glucocorticosteroid, but those with severe disease often respond poorly to these classes of drug. We assessed the efficacy and safety of a novel inhaled dual phosphodiesterase 3 (PDE3) and PDE4 inhibitor, RPL554 for its ability to act as a bronchodilator and anti-inflammatory drug.Between February, 2009, and January, 2013, we undertook four proof-of-concept clinical trials in the Netherlands, Italy, and the UK. Nebulised RPL554 was examined in study 1 for safety in 18 healthy men who were randomly assigned (1:1:1) to receive an inhaled dose of RPL554 (0·003 mg/kg or 0·009 mg/kg) or placebo by a computer-generated randomisation table. Subsequently, six non-smoking men with mild allergic asthma received single doses of RPL554 (three received 0·009 mg/kg and three received 0·018 mg/kg) in an open-label, adaptive study, and then ten men with mild allergic asthma were randomly assigned to receive placebo or RPL554 (0·018 mg/kg) by a computer-generated randomisation table for an assessment of safety, bronchodilation, and bronchoprotection. Study 2 examined the reproducibility of the bronchodilator response to a daily dose of nebulised RPL554 (0·018 mg/kg) for 6 consecutive days in a single-blind (patients masked), placebo-controlled study in 12 men with clinically stable asthma. The safety and bronchodilator effect of RPL554 (0·018 mg/kg) was assessed in study 3, an open-label, placebo-controlled crossover trial, in 12 men with mild-to-moderate COPD. In study 4, a placebo-controlled crossover trial, the effect of RPL554 (0·018 mg/kg) on lipopolysaccharide-induced inflammatory cell infiltration in induced sputum was investigated in 21 healthy men. In studies 3 and 4, randomisation was done by computer-generated permutation with a block size of two for study 3 and four for study 4. Unless otherwise stated, participants and clinicians were masked to treatment assignment. Analyses were by intention to treat. All trials were registered with EudraCT, numbers 2008-005048-17, 2011-001698-22, 2010-023573-18, and 2012-000742-34.Safety was a primary endpoint of studies 1 and 3 and a secondary endpoint of studies 2 and 4. Overall, RPL554 was well tolerated, and adverse events were generally mild and of equal frequency between placebo and active treatment groups. Efficacy was a primary endpoint of study 2 and a secondary endpoint of studies 1 and 3. Study 1 measured change in forced expiratory volume in 1 s (FEV1) and provocative concentration of methacholine causing a 20% fall in FEV1 (PC20MCh) in participants with asthma. RPL554 produced rapid bronchodilation in patients with asthma with an FEV1 increase at 1 h of 520 mL (95% CI 320-720; p0·0001), which was a 14% increase from placebo, and increased the PC20MCh by 1·5 doubling doses (95% CI 0·63-2·28; p=0·004) compared with placebo. The primary endpoint of study 2 was maximum FEV1 reached during 6 h after dosing with RPL554 in patients with asthma. RPL554 produced a similar maximum mean increase in FEV1 from placebo on day 1 (555 mL, 95% CI 442-668), day 3 (505 mL, 392-618), and day 6 (485 mL, 371-598; overall p0·0001). A secondary endpoint of study 3 (patients with COPD) was the increase from baseline in FEV1. RPL554 produced bronchodilation with a mean maximum FEV1 increase of 17·2% (SE 5·2). In healthy individuals (study 4), the primary endpoint was percentage change in neutrophil counts in induced sputum 6 h after lipopolysaccharide challenge. RPL554 (0·018 mg/kg) did not significantly reduce the percentage of neutrophils in sputum (80·3% in the RPL554 group vs 84·2% in the placebo group; difference -3·9%, 95% CI -9·4 to 1·6, p=0·15), since RPL554 significantly reduced neutrophils (p=0·002) and total cells (p=0·002) to a similar degree.In four exploratory studies, inhaled RPL554 is an effective and well tolerated bronchodilator, bronchoprotector, and anti-inflammatory drug and further studies will establish the full potential of this new drug for the treatment of patients with COPD or asthma.Verona Pharma.

Published

2013

44. Early stage development of the glycine-1 re-uptake inhibitor SCH 900435: central nervous system effects compared with placebo in healthy men

Author

Marieke, Liem-Moolenaar, Pierre, Peeters, Ingrid M C, Kamerling, Chris, Hogg, Graham, Holder, Huub Jan, Kleijn, Edwin, Spaans, Joanna, Udo De Haes, Marieke L, de Kam, Kari L, Franson, Adam F, Cohen, and Joop M A, van Gerven

Subjects

Adult, Male, Adolescent, Dose-Response Relationship, Drug, Eye Movements, Tetrahydronaphthalenes, Glycine, Brain, Electroencephalography, Middle Aged, Young Adult, Double-Blind Method, Pharmacodynamics, Drug Discovery, Schizophrenia, Humans, Neurotransmitter Uptake Inhibitors, Color Perception, Psychomotor Performance, Antipsychotic Agents

Abstract

To report the first three studies with SCH 900435, a selective glycine-1 re-uptake inhibitor in development for treating schizophrenia, using systematic evaluations of pharmacodynamics to understand the observed effects.Three double-blind, placebo-controlled studies (single, visual effect and multiple dose) were performed. In the single and multiple dose study SCH 900435 (0.5-30 mg) was given to healthy males and frequent pharmacokinetic and pharmacodynamic measurements were performed. The visual effects study incorporated visual electrophysiological measures of macular, retinal and intracranial visual pathway function.In the single dose study (highest difference, 95% CI, P) increases in smooth pursuit eye movements (8, 12 mg (-6.09, 10.14, -2.04, 0.013), 30 mg), pupil : iris ratio (20 and 30 mg (-0.065, 0.09, -0.04,0.0001)), VAS colour perception (30 mg (-9.48, 13.05, -5.91,0.0001)) and changes in spontaneous reports of visual disturbance were found, while FSH (8 mg (0.42, 0.18, 0.66, 0.0015), 12, 20 mg), LH (8-30 mg (1.35, 0.65, 2.05, 0.0003)) and EEG alpha2 activity decreased (12, 20, 30 mg (0.27, 0.14, 0.41, 0.0002)). A subsequent dedicated visual effects study demonstrated that visual effects were transient without underlying electrophysiological changes. This provided enough safety information for starting a multiple ascending dose study, showing less visual symptoms after twice daily dosing and titration, possibly due to tolerance.Several central nervous system (CNS) effects and gonadotropic changes resulted from administration of 8 mg and higher, providing evidence for CNS penetration and pharmacological activity of SCH 900435. Antipsychotic activity in patients, specificity of the reported effects for this drug class and possible tolerance to visual symptoms remain to be established.

Published

2011

45. Effect of garlic powder on C-reactive protein and plasma lipids in overweight and smoking subjects

Author

Jacobus Burggraaf, Rik C. Schoemaker, Martijn B A van Doorn, Verena M. Dirsch, Hans M.G. Princen, Adam F. Cohen, Rolf Gebhardt, Angelika M. Vollmar, P. Meijer, Sonia M. S. Espirito Santo, Ingrid M C Kamerling, and Thomas Haffner

Subjects

GARLIC POWDER, Adult, Male, medicine.medical_specialty, Atorvastatin, Medicine (miscellaneous), Placebo, chemistry.chemical_compound, food, Double-Blind Method, Internal medicine, Blood plasma, medicine, Humans, Pyrroles, Endothelium, Garlic, Triglycerides, Aged, Analysis of Variance, Nutrition and Dietetics, medicine.diagnostic_test, biology, business.industry, Cholesterol, Plant Extracts, Anticholesteremic Agents, C-reactive protein, Cholesterol, HDL, Smoking, Cholesterol, LDL, Middle Aged, Overweight, Lipids, food.food, Endocrinology, C-Reactive Protein, chemistry, Heptanoic Acids, biology.protein, Female, Powders, Lipid profile, business, Body mass index, Biomarkers, medicine.drug

Abstract

Background: Epidemiologic studies suggest that garlic may have beneficial effects on risk factors associated with cardiovascular disease (CVD). However, these findings are not unambiguously supported by randomized placebo-controlled clinical trials. Objective: We sought to investigate the effects of a chemically well-characterized garlic preparation on biomarkers for inflammation, endothelial function, and lipid metabolism in subjects with risk factors for CVD. Design: This was a double-blind, randomized, placebo-controlled trial in 90 overweight [body mass index (in kg/m2) > 24.5] subjects aged 40-75 y who smoked >10 cigarettes/d. The subjects were randomly assigned to 3 parallel treatment groups: garlic powder (2.1 g/d), atorvastatin (40 mg/d), or placebo. Duplicate measurements were performed at baseline and after 1 and 3 mo of treatment. Treatments were compared with analysis of covariance with baseline as the covariate, and differences between the treatments were reported as mean percentage difference and corresponding 97.5% CI. Results: None of the variables showed significant differences between the garlic-treated and the placebo groups. In contrast, compared with the placebo group, atorvastatin treatment resulted in significantly lower plasma concentrations of C-reactive protein (20.2%; 1.7%, 35.3%), total cholesterol (37.2%; 33.1%, 41.1%), LDL cholesterol (52.7%; 47.9%, 57.1%), triacylglycerols (31.9%; 20.8%, 41.5%), and tumor necrosis factor α (TNF-α; 41.9%; 19.0%, 58.3%) and increased the ratio of ex vivo whole blood lipopolysaccharide-stimulated to nonstimulated TNF-α concentrations (109.7%; 37.9%, 218.9%). Conclusion: We conclude that a chemically well-characterized garlic preparation has no significant effect on inflammatory biomarkers, endothelial function, or lipid profile in normolipidemic subjects with risk factors for CVD. © 2006 American Society for Nutrition. Chemicals / CAS: atorvastatin, 134523-00-5, 134523-03-8; C reactive protein, 9007-41-4; Anticholesteremic Agents; atorvastatin, 110862-48-1; Biological Markers; C-Reactive Protein, 9007-41-4; Cholesterol, 57-88-5; Cholesterol, HDL; Cholesterol, LDL; Heptanoic Acids; Lipids; Plant Extracts; Powders; Pyrroles; Triglycerides

Published

2006

46. Effects of a nonpeptide motilin receptor antagonist on proximal gastric motor function

Author

Ingrid M C, Kamerling, Aernout D, van Haarst, Jacobus, Burggraaf, Rik C, Schoemaker, Marieke L, de Kam, Hartmut, Heinzerling, Adam F, Cohen, and Ad A M, Masclee

Subjects

Adult, Male, Motor Neurons, Receptors, Neuropeptide, Adolescent, Double-Blind Method, Pharmacodynamics, Stomach, Sensation, Humans, Middle Aged, Motilin, Receptors, Gastrointestinal Hormone

Abstract

To assess the effects of the motilin receptor antagonist RWJ-68023 on basal and motilin-stimulated proximal gastric volume.Eighteen healthy male volunteers received RWJ-68023 in two different doses or placebo for 135 min. After 45 min, subjects received a motilin infusion for 90 min. Proximal gastric volume was measured with a barostat at constant pressure and during isobaric distensions. Abdominal symptoms were scored using visual analogue scales. Motilin and RWJ-68023 concentrations were assessed by radioimmunoassay and liquid chromatography-mass spectrometry, respectively.Both dosages of RWJ-68023 were safe and well tolerated. The most common adverse events were of gastrointestinal origin. RWJ-68023 did not affect basal proximal gastric volume, but the high-dose RWJ-68023 reduced the contractile effect of motilin on the stomach. This antagonizing effect of RWJ-68023 was only significant (P = 0.014) during the distension procedure.The RWJ-68023 doses used in this study were selected to accomplish plasma concentrations that would block the motilin effect entirely. However, the antagonizing effect of RWJ-68023 was partial and only present when the tonic condition of the stomach was modulated by motilin.

Published

2004

47. Motilin kinetics and effects on proximal stomach in patients with functional dyspepsia (FD) and healthy volunteers

Author

Adam F. Cohen, Rik C. Schoemaker, Ingrid M. C. Kamerling, Ad A.M. Masclee, and A. D. Van Haarst

Subjects

Pharmacology, Abdominal pain, medicine.medical_specialty, Nausea, business.industry, Gallbladder, digestive, oral, and skin physiology, Placebo, Proceedings of the Dutch Society for Clinical Pharmacology and Biopharmacy 19 April 2002, Barostat, Gastroenterology, Confidence interval, Motilin, medicine.anatomical_structure, Endocrinology, Internal medicine, medicine, Pharmacology (medical), medicine.symptom, business, Proximal stomach

Abstract

Motilin is involved in the regulation of upper gastrointestinal (GI) motility and it has been suggested that motilin may play a role in the pathogenesis of poorly understood clinical entities such as FD. The present study was performed in order to further investigate the effects of exogenous motilin on the proximal stomach of healthy volunteers and patients with FD. Eight healthy volunteers and 12 FD patients (Rome II, early satiety) were infused with synthetic motilin (4 pmol kg−1 min−1) or placebo over 90 min in a double-blind, randomized, cross-over study. Proximal gastric volume was measured with a barostat device at a predefined pressure and during isobaric distensions. Abdominal symptoms such as fullness, nausea and abdominal pain were scored by Visual Analogue Scales (VAS). Gallbladder volume was measured by ultrasonography and plasma motilin concentrations were measured with an radioimmuno-assay. Treatment effect within a patient group was estimated with paired Student's t-test, and differences between the two groups were investigated using unpaired Student's t-test. Data are given as mean (± s.d.) and differences are expressed with the corresponding 95% confidence intervals (95% CI). The plasma concentration–time curves for motilin were similar between healthy volunteers and patients. Baseline gastric volumes were similar for both groups; 269 ± 147 ml (healthy volunteers) and 265 ± 98 ml (FD patients). Compared with placebo, motilin reduced proximal gastric volume by 112 ml (95% CI: 29, 195 ml) in FD patients and by 96 ml (95% CI: −7.3, 200) in healthy volunteers (Figure 1). Figure 1 Mean (s.d.) proximal gastric volume (ml) during the constant pressure procedure (MDP + 3 mmHg), corrected for baseline volume in dyspeptic patients (n = 12) during motilin (▪) and placebo (□) and in healthy volunteers (n = 8) during motilin ... In the FD-patients, motilin decreased maximal compliance by 76.1 ml mm Hg−1 (95% CI: 8.8, 143.4) compared with placebo, and was similar to that observed in healthy volunteers. Patients were significantly more nauseous (p = 0.04) during motilin compared with placebo, whereas healthy volunteers did not experience nausea. Motilin reduced gall bladder volume by 33% (95% CI: 20, 45) in the FD patients and by 6% (95% CI: −13, 25) in the healthy volunteers. The difference in gall bladder volume was significant between the groups. Motilin significantly reduced proximal gastric volume and compliance in dyspeptic patients and healthy volunteers by a similar magnitude. In dyspeptic patients, motilin induced nausea, and evoked a greater gall bladder volume reduction.

Published

2002