ABSTRACT
The sales of dietary supplements continue to increase year after year. Despite their use by a large percentage of Americans, there is little evidence for the vast majority of products regarding their safety or efficacy. National Center for Complementary and Integrative Health supports a broad range of research on dietary supplements, including clinical trials. Our experience with these trials has shaped our current policies and priorities for clinical research. This perspective outlines those policies and priorities that are shaping our investments going forward. SIGNIFICANCE STATEMENT: The sales of dietary supplements continue to increase year after year. Despite their use by a large percentage of Americans, there is little evidence for the vast majority of products regarding their safety or efficacy. National Center for Complementary and Integrative Health supports a broad range of research on dietary supplements, including clinical trials. Our experience with these trials has shaped our current policies and priorities for clinical research. This perspective outlines those policies and priorities that are shaping our investments going forward.
Subject(s)
Biological Products/adverse effects , Clinical Trials as Topic/standards , Dietary Supplements/adverse effects , National Center for Complementary and Integrative Health (U.S.)/standards , Research Design/standards , Biological Products/administration & dosage , Clinical Trials as Topic/economics , Humans , National Center for Complementary and Integrative Health (U.S.)/economics , Policy , United StatesABSTRACT
This study aims to benchmark and analyze the process development and manufacturing costs across the biopharmaceutical drug development cycle and their contribution to overall research and development (R&D) costs. This was achieved with a biopharmaceutical drug development lifecycle cost model that captured the costs, durations, risks and interdependencies of the clinical, process development and manufacturing activities. The budgets needed for process development and manufacturing at each phase of development to ensure a market success each year were estimated. The impact of different clinical success rate profiles on the process development and manufacturing costs at each stage was investigated, with a particular focus on monoclonal antibodies. To ensure a market success each year with an overall clinical success rate (Phase I to approval) of ~12%, the model predicted that a biopharmaceutical company needs to allocate process development and manufacturing budgets in the order of ~$60 M for pre-clinical to Phase II material preparation and ~$70 M for Phase III to regulatory review material preparation. For lower overall clinical success rates of ~4%, which are more indicative of diseases such as Alzheimer's, these values increase to ~$190 M for early-phase and ~$140 Mfor late-phase material preparation; hence, the costs increase 2.5 fold. The costs for process development and manufacturing per market success were predicted to represent 13-17% of the R&D budget from pre-clinical trials to approval. The results of this quantitative structured cost study can be used to aid decision-making during portfolio management and budget planning procedures in biopharmaceutical development.
Subject(s)
Antibodies, Monoclonal/therapeutic use , Benchmarking/methods , Biological Products/therapeutic use , Drug Approval/methods , Drug Development/methods , Drug Industry/methods , Benchmarking/economics , Clinical Trials as Topic/economics , Drug Approval/economics , Drug Costs/statistics & numerical data , Drug Development/economics , Drug Evaluation, Preclinical/economics , Drug Industry/economics , Humans , Models, Economic , Pharmaceutical Preparations/economics , Research/economics , Research/statistics & numerical data , Technology, Pharmaceutical/economics , Technology, Pharmaceutical/methodsABSTRACT
Christian Lienhardt and co-authors discuss the conclusions of the PLOS Medicine Collection on advances in clinical trial design for development of new tuberculosis treatments.
Subject(s)
Antitubercular Agents/therapeutic use , Clinical Trials as Topic/methods , Tuberculosis/drug therapy , Antitubercular Agents/pharmacology , Clinical Trials as Topic/economics , Clinical Trials, Phase II as Topic/economics , Clinical Trials, Phase II as Topic/methods , Clinical Trials, Phase III as Topic/economics , Clinical Trials, Phase III as Topic/methods , Drug Development , Drug Evaluation, Preclinical , Humans , Medication Adherence , Time Factors , Translational Research, Biomedical , Vulnerable PopulationsSubject(s)
Alkaptonuria/drug therapy , Clinical Trials as Topic/methods , Clinical Trials as Topic/standards , Compassionate Use Trials , Rare Diseases/drug therapy , Adolescent , Alkaptonuria/genetics , Alkaptonuria/metabolism , Alkaptonuria/urine , Animals , Autopsy , Child , Clinical Trials as Topic/economics , Cyclohexanones/pharmacology , Cyclohexanones/therapeutic use , Disease Models, Animal , Disease Progression , Drug Approval , Endpoint Determination , Female , Homogentisic Acid/metabolism , Humans , Infant , Male , Mice , National Health Programs , National Institutes of Health (U.S.) , Nitrobenzoates/pharmacology , Nitrobenzoates/therapeutic use , Observational Studies as Topic , Off-Label Use , Orphan Drug Production , Rare Diseases/genetics , Rare Diseases/metabolism , Rare Diseases/urine , Rats , Sample Size , Tyrosine/metabolism , Tyrosinemias/drug therapy , Tyrosinemias/enzymology , United States , United States Food and Drug Administration/legislation & jurisprudenceABSTRACT
INTRODUCTION: Care-seeking for sexual dysfunction is limited by embarrassment, efficacy/safety concerns, and cost. Nutritional supplements (NSs) are low-cost but unproven. AIM: To provide hypotheses on whether effective NS combinations for sexual dysfunction can be created following known pharmacology principles and tested with sufficient rigor in Internet-based "exo-clinical" trials (XCTs). METHODS: PubMed and Google searches were conducted to review the feasibility of XCTs of NS combinations for sexual dysfunction. Findings were synthesized into recommendations for XCTs to treat the most common sexual problems. MAIN OUTCOME MEASURE: The hierarchy of references used for making recommendations was controlled clinical trials over uncontrolled trials. The frequency of sexual dysfunction was determined in population-representative national surveys. RESULTS: XCTs of cognitive behavioral therapy show conclusive efficacy for anxiety and depression. 5 small XCTs showed efficacy for female sexual dysfunction and erectile dysfunction (ED), and 2 XCTs of NS for other medical problems substantiated feasibility. To test the feasibility of XCTs for the most common forms of sexual dysfunction-ED, hypoactive sexual desire disorder (HSDD), and sexual performance anxiety-protocol outlines were generated for frugal XCTs; the total estimated subject time burden is ≤1 hour. CONCLUSION: An XCT is a cost-effective method of evaluating new treatments, including sexual dysfunction and common mental disorders, if compliance is maintained by regular outreach while minimizing the time burden on subjects and handling consent and privacy issues appropriately. NS combinations might expand the opportunities for relief of sexual dysfunction if formulated with pharmacologically active doses of NS with already supported efficacy and safety. The feasibility of XCTs of NS combinations for sexual dysfunction might be tested most productively in men with ED, in women with HSDD, and in men and women with sexual performance anxiety. Pyke RE. Exo-Clinical Trials of Nutritional Supplements for Sexual Dysfunction: Precedents, Principles, and Protocols. Sex Med Rev 2019;7:251-258.
Subject(s)
Clinical Trials as Topic , Dietary Supplements , Sexual Dysfunction, Physiological/therapy , Sexual Dysfunctions, Psychological/therapy , Clinical Trials as Topic/economics , Evaluation Studies as Topic , Feasibility Studies , Female , Humans , Internet , Male , Psychotherapy , Sexual Dysfunction, Physiological/diet therapy , Sexual Dysfunction, Physiological/psychology , Sexual Dysfunctions, Psychological/diet therapy , Sexual Dysfunctions, Psychological/psychologyABSTRACT
Recently, there is an increasing number of clinical trials on Traditional Chinese medicine (TCM) published, but the implementation of Clinical Trial Registration (CTR), Ethical Review (ER), and Informed Consent (IC) in clinical trials of TCM is unclear. This study aims to investigate the status of CTR, ER, and IC in clinical trials of TCM.Clinical trials of TCM published in 10 high-quality Chinese journals in 2016 were selected as a sample. Information of clinical trial registration, ethical review, and informed consent of clinical trials was extracted for analysis. Two authors independently screened the literature and extracted the relevant information.A total of 659 clinical trials met the criteria and were included for analysis. Only 9 clinical trials reported information of clinical trial registration (1.4%). The number for ethical review and informed consent were 156 (23.7%) and 502 (76.2%).Trial registration, protocol approval, and informed consent were not well executed. Especially registration and ethical review of clinical trials in TCM should be carefully concerned by researchers, clinicians, and journal editors. Training on methodology of clinical trial should be strengthened.
Subject(s)
Clinical Trials as Topic/ethics , Ethical Review , Informed Consent , Medicine, Chinese Traditional/standards , Registries , Access to Information , Clinical Trials as Topic/economics , Clinical Trials as Topic/standards , Cross-Sectional Studies , Humans , Medicine, Chinese Traditional/economics , Quality Improvement , Research Support as TopicABSTRACT
At the design stage of a study, it is crucial to compute the sample size needed for treatment effect estimation with maximum precision and power. The optimal design depends on the costs, which may be known at the design stage, and on the outcome variances, which are unknown. A balanced design, optimal for homogeneous costs and variances, is typically used. An alternative to the balanced design is a design optimal for the known and possibly heterogeneous costs, and homogeneous variances, called costs considering design. Both designs suffer from loss of efficiency, compared with optimal designs for heterogeneous costs and variances. For 2 × 2 multicenter trials, we compute the relative efficiency of the balanced and the costs considering designs, relative to the optimal designs. We consider 2 heterogeneous costs and variance scenarios (in 1 scenario, 2 treatment conditions have small and 2 have large costs and variances; in the other scenario, 1 treatment condition has small, 2 have intermediate, and 1 has large costs and variances). Within these scenarios, we examine the relative efficiency of the balanced design and of the costs considering design as a function of the extents of heterogeneity of the costs and of the variances and of their congruence (congruent when the cheapest treatment has the smallest variance, incongruent when the cheapest treatment has the largest variance). We find that the costs considering design is generally more efficient than the balanced design, and we illustrate this theory on a 2 × 2 multicenter trial on lifestyle improvement of patients in general practices.
Subject(s)
Clinical Trials as Topic/methods , Biostatistics , Clinical Trials as Topic/economics , Clinical Trials as Topic/statistics & numerical data , General Practice , Health Care Costs , Health Promotion , Humans , Life Style , Linear Models , Models, Statistical , Multicenter Studies as Topic/statistics & numerical data , Randomized Controlled Trials as Topic/statistics & numerical data , Sample Size , Treatment OutcomeABSTRACT
Eighty percent of drugs that enter human clinical testing are never approved for use. This means that for every five drugs that make it into the clinic, there are four that failed to show effectiveness for treating the disease or condition the drug was designed to treat.This high failure rate means there are many existing, partially developed therapeutic candidates with known pharmacology, formulation, and potential toxicity. Finding new uses for existing experimental drugs or biologics "repositioning" builds upon previous research and development efforts, so new candidate therapies can be advanced to clinical trials for a new use more quickly than starting from scratch.Federal funding initiatives in the U.S. and UK started to support pre-clinical /or early stage trials for repositioning existing experimental drugs or biologics (therapies). This chapter covers some of the process issues that have been solved and the remaining challenges that are still in need of solutions. The chapter is primarily written from a U.S. federal funding perspective. The general concepts could be applied more globally to benefit rare and neglected disease populations. The drug development and process bottlenecks are the same for both rare and common disease.
Subject(s)
Clinical Trials as Topic/methods , Drug Evaluation, Preclinical/methods , Drug Repositioning/methods , Off-Label Use , Orphan Drug Production , Rare Diseases/drug therapy , Research Design , Clinical Trials as Topic/economics , Drug Costs , Drug Evaluation, Preclinical/economics , Drug Repositioning/economics , Humans , Off-Label Use/economics , Orphan Drug Production/economics , Patient Safety , Public-Private Sector Partnerships , Rare Diseases/diagnosis , Rare Diseases/economics , Rare Diseases/epidemiology , Research Support as Topic , Risk AssessmentSubject(s)
Clinical Trials as Topic/methods , Clinical Trials as Topic/standards , Drug Evaluation, Preclinical/methods , Drug Evaluation, Preclinical/standards , Drug-Related Side Effects and Adverse Reactions/prevention & control , Patient Safety/standards , Research Design/standards , Animals , Clinical Trials as Topic/economics , Clinical Trials as Topic/ethics , Dose-Response Relationship, Drug , Drug Evaluation, Preclinical/economics , Drug-Related Side Effects and Adverse Reactions/economics , Ethics, Research , France , Healthy Volunteers , Humans , Male , Mice , Models, Animal , Risk Assessment/standards , Treatment Failure , United States , United States Food and Drug Administration/organization & administrationSubject(s)
Neurodegenerative Diseases/economics , Neurodegenerative Diseases/therapy , Stem Cell Transplantation/economics , Stem Cell Transplantation/methods , Stem Cells/physiology , Clinical Trials as Topic/economics , Humans , National Health Programs/economics , Neurodegenerative Diseases/physiopathology , Stem Cell Transplantation/ethicsABSTRACT
Society faces a crisis of rising antibiotic resistance even as the pipeline of new antibiotics has been drying up. Antibiotics are a public trust; every individual's use of antibiotics affects their efficacy for everyone else. As such, responses to the antibiotic crisis must take a societal perspective. The market failure of antibiotics is due to a combination of scientific challenges to discovering and developing new antibiotics, unfavorable economics, and a hostile regulatory environment. Scientific solutions include changing the way we screen for new antibiotics. More transformationally, developing new treatments that seek to disarm pathogens without killing them, or that modulate the host inflammatory response to infection, will reduce selective pressure and hence minimize resistance emergence. Economic transformation will require new business models to support antibiotic development. Finally, regulatory reform is needed so that clinical development programs are feasible, rigorous, and clinically relevant. Pulmonary and critical care specialists can have tremendous impact on the continued availability of effective antibiotics. Encouraging use of molecular diagnostic tests to allow pathogen-targeted, narrow-spectrum antibiotic therapy, using short rather than unnecessarily long course therapy, reducing inappropriate antibiotic use for probable viral infections, and reducing infection rates will help preserve the antibiotics we have for future generations.
Subject(s)
Anti-Bacterial Agents/therapeutic use , Clinical Trials as Topic/legislation & jurisprudence , Drug Approval/legislation & jurisprudence , Drug Discovery/standards , Drug Industry/standards , Drug Resistance, Bacterial/drug effects , Drug Utilization/standards , Anti-Bacterial Agents/economics , Anti-Bacterial Agents/standards , Clinical Trials as Topic/economics , Clinical Trials as Topic/trends , Drug Approval/statistics & numerical data , Drug Discovery/economics , Drug Discovery/methods , Drug Industry/economics , Drug Industry/methods , Humans , Microbial Sensitivity Tests , United States , United States Food and Drug AdministrationABSTRACT
Maintaining research and development (R&D) productivity at a sustainable level is one of the main challenges currently facing the pharmaceutical industry. In this article, we discuss the results of a comprehensive longitudinal review of AstraZeneca's small-molecule drug projects from 2005 to 2010. The analysis allowed us to establish a framework based on the five most important technical determinants of project success and pipeline quality, which we describe as the five 'R's: the right target, the right patient, the right tissue, the right safety and the right commercial potential. A sixth factor - the right culture - is also crucial in encouraging effective decision-making based on these technical determinants. AstraZeneca is currently applying this framework to guide its R&D teams, and although it is too early to demonstrate whether this has improved the company's R&D productivity, we present our data and analysis here in the hope that it may assist the industry overall in addressing this key challenge.
Subject(s)
Biomedical Research , Drug Design , Drug Discovery , Drug Industry , Drugs, Investigational/therapeutic use , Models, Organizational , Animals , Biomedical Research/economics , Clinical Trials as Topic/economics , Decision Making, Organizational , Drug Discovery/economics , Drug Evaluation, Preclinical/economics , Drug Industry/economics , Drugs, Investigational/adverse effects , Drugs, Investigational/economics , Drugs, Investigational/pharmacology , Efficiency, Organizational , Humans , Organizational Culture , Research Support as Topic , Technology, Pharmaceutical/economicsABSTRACT
The success of device-based research in the clinical neurosciences has overshadowed a critical and emerging problem in the biomedical research environment in the United States. Neuroprosthetic devices, such as deep brain stimulation (DBS), have been shown in humans to be promising technologies for scientific exploration of neural pathways and as powerful treatments. Large device companies have, over the past several decades, funded and developed major research programs. However, both the structure of clinical trial funding and the current regulation of device research threaten investigator-initiated efforts in neurologic disorders. The current atmosphere dissuades clinical investigators from pursuing formal and prospective research with novel devices or novel indications. We review our experience in conducting a federally funded, investigator-initiated, device-based clinical trial that utilized DBS for thalamic pain syndrome. We also explore barriers that clinical investigators face in conducting device-based clinical trials, particularly in early-stage studies or small disease populations. We discuss 5 specific areas for potential reform and integration: (1) alternative pathways for device approval; (2) eliminating right of reference requirements; (3) combining federal grant awards with regulatory approval; (4) consolidation of oversight for human subjects research; and (5) private insurance coverage for clinical trials. Careful reformulation of regulatory policy and funding mechanisms is critical for expanding investigator-initiated device research, which has great potential to benefit science, industry, and, most importantly, patients.
Subject(s)
Biomedical Research/economics , Clinical Trials as Topic/economics , Deep Brain Stimulation/instrumentation , Device Approval , Hyperalgesia/therapy , Paresthesia/therapy , Thalamic Diseases/therapy , Equipment Design , Financing, Government , Financing, Organized , Humans , Hyperalgesia/physiopathology , Insurance Coverage/economics , Neural Pathways/physiopathology , Paresthesia/physiopathology , Thalamic Diseases/physiopathology , Thalamus/physiopathology , United StatesSubject(s)
Disease Models, Animal , Drug Evaluation, Preclinical/methods , Drug Evaluation, Preclinical/standards , Research Design , Translational Research, Biomedical/methods , Translational Research, Biomedical/standards , Amyotrophic Lateral Sclerosis/genetics , Amyotrophic Lateral Sclerosis/pathology , Amyotrophic Lateral Sclerosis/therapy , Animals , Cause of Death , Clinical Trials as Topic/economics , Clinical Trials as Topic/standards , Disease Progression , Dose-Response Relationship, Drug , Drug Evaluation, Preclinical/economics , False Positive Reactions , Guidelines as Topic , Half-Life , Humans , Mice , Organ Specificity , Reproducibility of Results , Superoxide Dismutase/deficiency , Superoxide Dismutase/genetics , Superoxide Dismutase/metabolism , Superoxide Dismutase-1 , Survival Analysis , Translational Research, Biomedical/economics , Treatment FailureSubject(s)
Central Nervous System Agents/therapeutic use , Drug Discovery , Drug Industry , Drugs, Investigational/therapeutic use , Neuropharmacology/methods , Pharmacology, Clinical/methods , Psychopharmacology/methods , Central Nervous System Agents/adverse effects , Central Nervous System Agents/economics , Clinical Trials as Topic/economics , Databases, Chemical , Drug Discovery/economics , Drug Evaluation, Preclinical/economics , Drug Industry/economics , Drug Industry/trends , Drugs, Investigational/adverse effects , Drugs, Investigational/economics , European Union , Humans , Neuropharmacology/economics , Neuropharmacology/trends , Pharmacology, Clinical/economics , Pharmacology, Clinical/trends , Psychopharmacology/economics , Psychopharmacology/trends , Research Support as Topic , Societies, ScientificABSTRACT
OBJECTIVE: To evaluate the efficiency of initiation with endothelin receptor antagonists, ambrisentan or bosentan, followed by sequential combination with phosphodiesterase-5 inhibitors and prostanoids in the treatment of pulmonary arterial hypertension, from the Spanish National Health System perspective. METHODS: A Markov model was developed based on the four New York Heart Association functional classes. A panel of three experts reached a consensus on patient management based on clinical practice. Patients revised their treatment every 12 weeks, based on their health status and previous medication records. Pharmacological treatment costs and costs associated with very frequent adverse events (AE) were considered in a horizon of 60 weeks. Outcomes were measured in qualityadjusted life years (QALY). A probabilistic sensitivity analysis was performed. RESULTS: No clinically relevant differences in QALY per-patient and year were found for initiation with ambrisentan and bosentan: 0.6853 and 0.6902, respectively. Initiation with ambrisentan resulted in lower pharmacological treatment and AE management costs: ?35,550 and ?117 versus ?40,224 and ?171. In the sensitivity analysis, initiation with ambrisentan resulted in a negative significant cost difference: ?-4,982; CI95%[?- 8,014; ?-2,500]; while no significant differences in QALY were found: -0.0044; CI95%[-0.0189; 0.0101]. CONCLUSIONS: Initiation with ambrisentan followed by sequential combination with phosphodiesterase-5 inhibitors and prostanoids yields comparable outcomes at lower costs than initiation with bosentan.
Objetivo: Se pretende evaluar la eficiencia del tratamiento secuencial de combinación de la hipertensión arterial pulmonar iniciado con antagonistas del receptor de la endotelina, ambrisentan o bosentan, seguido de inhibidores de la fosfodiesterasa- 5 y prostanoides, desde la perspectiva del Sistema Nacional de Salud. Métodos: Se desarrolló un modelo de Markov basado en las cuatro clases funcionales de la New York Heart Association. Un panel de tres expertos alcanzó un consenso sobre el manejo del paciente basado en la práctica clínica. Los pacientes revisaron su tratamiento cada 12 semanas, en función de su estado de salud y de la medicación recibida previamente. Se incluyeron costes farmacológicos y costes asociados al manejo de eventos adversos (EA) muy frecuentes, en un horizonte de 60 semanas. Los resultados se expresaron en términos de los años de vida ajustados por calidad (AVAC). Se realizó un análisis de sensibilidad probabilístico. Resultados: No se encontraron diferencias clínicamente relevantes en los AVAC por paciente y año para el inicio con ambrisentan y bosentan: 0,6853 y 0,6902, respectivamente. El inicio con ambrisentan resultó en un coste farmacológico y asociado al manejo de EA menor: 35.550 ??y 117 ??frente a 40.224 ??y 171 ?. En el análisis de sensibilidad, el inicio con ambrisentan presentó una diferencia de costes totales negativa y significativa: -4.982 ?; IC95%[-8.014 ?; -2.500 ?]; mientras que no se detectaron diferencias significativas en los AVAC: -0,0044; IC95%[-0,0189; 0,0101]. Conclusiones: El tratamiento secuencial de combinación de la HAP iniciado con ambrisentan, seguido de inhibidores de la fosfodiesterasa- 5 y prostanoides, proporciona resultados en salud comparables y menores costes que el tratamiento iniciado con bosentan.
Subject(s)
Computer Simulation , Hypertension, Pulmonary/drug therapy , Models, Economic , Phenylpropionates/therapeutic use , Pyridazines/therapeutic use , Sulfonamides/therapeutic use , Bosentan , Chemical and Drug Induced Liver Injury/economics , Chemical and Drug Induced Liver Injury/etiology , Clinical Trials as Topic/economics , Cost-Benefit Analysis , Diuretics/economics , Diuretics/therapeutic use , Drug Costs , Drug Therapy, Combination , Edema/chemically induced , Edema/drug therapy , Edema/economics , Health Care Costs , Humans , Hypertension, Pulmonary/economics , Markov Chains , Multicenter Studies as Topic/economics , National Health Programs/economics , Phenylpropionates/adverse effects , Phenylpropionates/economics , Phosphodiesterase 5 Inhibitors/adverse effects , Phosphodiesterase 5 Inhibitors/economics , Phosphodiesterase 5 Inhibitors/therapeutic use , Prostaglandins/adverse effects , Prostaglandins/economics , Prostaglandins/therapeutic use , Pyridazines/adverse effects , Pyridazines/economics , Quality-Adjusted Life Years , Retrospective Studies , Sulfonamides/adverse effects , Sulfonamides/economics , Treatment OutcomeABSTRACT
A biomarker is defined as an objectively measured characteristic of a normal or pathologic biologic process. Identification and proper validation of biomarkers of epileptogenesis (the development of epilepsy) and ictogenesis (the propensity to generate spontaneous seizures) might predict the development of an epilepsy condition; identify the presence and severity of tissue capable of generating spontaneous seizures; measure progression after the condition is established; and determine pharmacoresistance. Such biomarkers could be used to create animal models for more cost-effective screening of potential antiepileptogenic and antiseizure drugs and devices, and to reduce the cost of clinical trials by enriching the trial population, and acting as surrogate markers to shorten trial duration. The objectives of the biomarker subgroup for the London Workshop were to define approaches for identifying possible biomarkers for these purposes. Research to identify reliable biomarkers may also reveal underlying mechanisms that could serve as therapeutic targets for the development of new antiepileptogenic and antiseizure compounds.
Subject(s)
Anticonvulsants/therapeutic use , Biomarkers/blood , Drug Discovery , Drugs, Investigational/therapeutic use , Epilepsy/drug therapy , Epilepsy/physiopathology , Animals , Anticonvulsants/adverse effects , Anticonvulsants/economics , Brain/physiopathology , Clinical Trials as Topic/economics , Cost-Benefit Analysis , Disease Models, Animal , Disease Progression , Drug Evaluation, Preclinical/economics , Drug Resistance , Drugs, Investigational/adverse effects , Drugs, Investigational/economics , Electroencephalography/drug effects , Epilepsy/etiology , Epilepsy/prevention & control , Humans , Precipitating FactorsABSTRACT
INTRODUCTION: Magnetic resonance spectroscopy (MRS) will continue to play an ever increasing role in drug discovery because MRS does readily define biomarkers for several hundreds of clinically distinct diseases. Published evidence based medicine (EBM) surveys, which generally conclude the opposite, are seriously flawed and do a disservice to the field of drug discovery. AREAS COVERED: This article presents MRS and how it has guided several hundreds of practical human 'drug discovery' endeavors since its development. Specifically, the author looks at the process of 'reverse-translation' and its influence in the expansion of the number of preclinical drug discoveries from in vivo MRS. The author also provides a structured approach of eight criteria, including EBM acceptance, which could potentially re-open the field of MRS for productive exploration of existing and repurposed drugs and cost-effective drug-discovery. EXPERT OPINION: MRS-guided drug discovery is poised for future expansion. The cost of clinical trials has escalated and the use of biomarkers has become increasingly useful in improving patient selection for drug trials. Clinical MRS has uncovered a treasure-trove of novel biomarkers and clinical MRS itself has become better standardized and more widely available on 'routine' clinical MRI scanners. When combined with available new MRI sequences, MRS can provide a 'one stop shop' with multiple potential outcome measures for the disease and the drug in question.
Subject(s)
Drug Discovery , Drug Evaluation, Preclinical/methods , Magnetic Resonance Spectroscopy/methods , Biomarkers/metabolism , Clinical Trials as Topic/economics , Clinical Trials as Topic/methods , Clinical Trials as Topic/standards , Drug Design , Drug Evaluation, Preclinical/economics , Humans , Magnetic Resonance Spectroscopy/economicsABSTRACT
Since several years risk-based monitoring is the new "magic bullet" for improvement in clinical research. Lots of authors in clinical research ranging from industry and academia to authorities are keen on demonstrating better monitoring-efficiency by reducing monitoring visits, monitoring time on site, monitoring costs and so on, always arguing with the use of risk-based monitoring principles. Mostly forgotten is the fact, that the use of risk-based monitoring is only adequate if all mandatory prerequisites at site and for the monitor and the sponsor are fulfilled.Based on the relevant chapter in ICH GCP (International Conference on Harmonisation of technical requirements for registration of pharmaceuticals for human use - Good Clinical Practice) this publication takes a holistic approach by identifying and describing the requirements for future monitoring and the use of risk-based monitoring. As the authors are operational managers as well as QA (Quality Assurance) experts, both aspects are represented to come up with efficient and qualitative ways of future monitoring according to ICH GCP.