Introduction:- Developers of drugs, biologicals, and medical devices must ensure product safety, demonstrate medical benefit in people, and mass produce the product. Preclinical development starts before clinical trials and the main goals are to determine safety and effectiveness of the intervention. Research may include pharmacodynamics, pharmacokinetics, absorption, distribution, metabolism and excretion studies, and toxicity testing. During preclinical studies, in vitro and in vivo testing is performed. Toxicity includes studies of which organs are targeted and long-term carcinogenic effects or effects on mammalian reproduction. Two species of animals are normally used in drug development studies. Choice is determined on which animal gives the best correlation to human studies.

Medical devices are usually studied in larger animal species. No Observed Adverse Effect Level (NOAEL), the level of exposure at which there is no biologically or statistically significant increase in the frequency or severity of any adverse effects in the exposed population when compared to its appropriate control, is established based on preclinical trials. These are used to determine initial Phase I clinical trial dosage levels on a mass active pharmaceutical ingredient (API) per mass patient basis. If preclinical studies show that the therapy is safe and effective, clinical trials, defined as “scientifically controlled studies of the safety and effectiveness of a therapeutic agent using consenting human subjects”, are started. The four possible outcomes are:

1) the new treatment has a large beneficial effect and is superior to standard treatment;

2) the new treatment is equivalent to standard treatment;

3) the new treatment is neither clearly superior nor clearly inferior to standard treatment; or

4) a new treatment is inferior to standard treatment.

The US Food and Drug Administration (FDA) role begins after preclinical evaluation for safety and effectiveness. These prospective studies are designed to answer specific questions about biomedical or behavioral interventions and must adhere to the principles of good clinical practices (GCP). Classification of the trial may reflect how the researchers behave (observational versus interventional clinical trials), by their purpose (prevention, screening, diagnostic, treatment, quality of life, or expanded access clinical trials), or whether the trial design allows changes based on data accumulated during the trial (fixed versus adaptive clinical trials). Ten areas that are carefully assessed in these clinical studies are protection of human subjects, sampling, degree of

masking, randomization, intention to treat analysis, selection of interventional and comparison groups, selection of end points, interpretation of results, trial duration, and selection of traditional versus equivalence testing. Randomized controlled trials (RCT) are the gold standard and are often used to evaluate the efficacy or effectiveness of various types of medical intervention and may provide information about adverse effects.

Classifications of RCT’s include study design (parallel-group, crossover, cluster, or factorial), outcome of interest (efficacy versus effectiveness), and evaluation of a hypothesis (superiority, non-inferiority, or equivalence). The people being studied are randomly allocated to one of the different treatments that are under study. The ideal randomization process maximizes statistical power, minimizes selection bias, and minimizes allocation bias. Clinical trial phases are steps in the research to determine if an intervention would be beneficial or detrimental to humans and include Phases 0, I, II, III, IV, and V clinical studies. During Phase 0, pharmacodynamics and pharmacokinetics are determined. Safety studies are evaluated during Phase I, efficacy during Phase II, and confirmation of safety and efficacy during Phase III. Sentry studies are done in Phase IV and comparative effectiveness research and community-based research in Phase V. Although this sounds easy and straightforward, definitions and purposes of the different phases become muddied and studies to determine if a therapy should be used in the general population of patients may be complex and results difficult to interpret. Clinical trials may go so wrong that unplanned changes in the population studied, end points or analysis plan must be made. Understanding the basis of clinical trial phases will help researchers plan and implement clinical study protocols and, by doing so, improve the number of therapies coming to market for patients.

Phase 0 Clinical Trials:-


Exploratory IND studies (also known as Phase 0 studies) are conducted early in clinical phase studies and involve limited human exposure and have no therapeutic or diagnostic intent. Doses are subtherapeutic and patients are monitored by the clinical researcher and involve about 10 study patients. Duration of a patient’s participation is usually less than 1 week. Phamacodynamics and pharmacokinetics are studied. These trials are before the traditional dose escalation, safety, and tolerance studies, do not replace the Phase I clinical trials and do not indicate whether a therapy has a positive impact on the targeted pathology. These studies help in eliminating candidate therapies before they reach Phase I studies.

These trials were developed:-

  • to shorten the critical path for drug development,
  • to explore pharmacokinetic and pharmacodynamic profiles of IND’s in humans,
  • to help in accelerating identification of promising drugs, and to reduce development time and costs.

Limitations of these trials include:-

  • lack of therapeutic intent,
  • motivation of patients to participate,
  • may delay or exclude patients from other clinical trials that may have therapeutic intent,
  • microdosing pharmacokinetics and relationship to therapeutic dose, and availability of sensitive analytical methods. Attrition rates are high and only about 8% come to market.

Phase I Clinical Trials:- A Phase I clinical trial evaluates the best way to administer a drug, its frequency and dose, the maximum tolerated dose (MTD), and side effects. Tolerability, pharmacokinetics, and pharmacodynamics are evaluated. These studies determine, most importantly, if the treatment is safe. Trials usually include 20 to 100 patients and are monitored by the clinical researcher. Doses are increased if there are no severe side effects and patients are tested to determine if he or she is responding to the therapy. These escalation dose studies are used to determine the best and safest dose that can be administered and is a fraction of the dose that caused harm during animal testing. Unnecessary exposure of subjects to subtherapeutic doses while maintaining safety and rapid accrual is the primary goal of Phase I trials. Subjects, in most cases, are healthy volunteers although patients with a certain disease may be required. Contract research organizations usually conduct these studies and stipends may be given. Testing is usually sequential with data being reviewed after every patient or small group of patients. Dose-toxicity and dose-efficacy curves are determined during this phase and include single ascending dose trials (Phase IA), multiple ascending dose trials (Phase IB), and food effect studies.

Dose escalation methods may be rule-based or model-based.

  • Rule-based designs do not stipulate any prior assumption of the dose-toxicity curve and allow escalation and de-escalation of the dose with diminishing fractions of the preceding dose depending on presence or absence of toxicity. They are easy to implement and do not require special software.
  • The traditional 3 + 3 design proceeds with cohorts of 3 patients. The starting dose is based on extrapolation from animal toxicological data. Increasing dose levels have been fixed in advance and usually follow a modified Fibonacci sequence in which the dosing increments become smaller as the dose increases. If none of the patients experience a dose-limiting toxicity, 3 more patients will be treated at the next higher dose. If 1 of the patients experiences a dose-limiting toxicity, the same dose is repeated in 3 more patients. Dose escalation continues until at lease 2 patients from a cohort of 3 to 6 experience dose-limiting toxicities. Recommended dose for Phase II trials is defined as the dose level just below the toxic dose level.
  • Alternate rule-based dose escalation methods include the “2 + 4,” “3 + 3 + 3,” and “3 + 1 + 1” (“best of five”) rules. In the “2 + 4” design, if one dose-limiting toxicity is observed in a first cohort of 2 patients, an additional cohort of 4 patients is added.
  • The stopping rule is the same as for the “3 + 3” studies. With the “3 + 3 + 3” study, a third cohort of 3 patients is added if 2 of 6 patients in the first 2 cohorts have a dose-limiting toxicity. If at least 3 of 9 patients experience a dose-limiting toxicity, the study is terminated. The “best of 5” design requires that 1 additional patient is added if 1 or 2 dose-limiting toxicities are observed in the first 3 patients. Another patient is added if 2 dose-limiting toxicities are seen among the 4 treated patients. Escalation is continued if no dose-limiting toxicities are seen of 3, 1 of 4, or 2 of 5 patients. If 3 or more dose-limiting toxicities are seen, the trial is stopped.
  • Accelerated titration designs combine variations of the 3 + 3 design and the model-based design. Patient assignment to doses is based on prespecified rules. Pharmacologically guided dose escalation is a variation of the 3 + 3 design method. This assumes that animal model studies accurately reflect dose-limiting toxicities based on plasma drug concentrations. In the first stage, plasma exposure is extrapolated from preclinical data. Pharmacokinetic data are then obtained for each patient to determine subsequent dosing. The isotonic regression model assumes toxicity is nondecreasing with dose and fits an isotonic regression to accumulated data. The dose given is that with estimated toxicity thought closest to the maximum tolerable toxicity.
  • The “rolling six design” allows for accrual of 2 to 6 patients concurrently onto a dose level based on the number of patients enrolled and evaluable, the number having dose-limiting toxicity (DLT), and the number still at risk of developing DLT. This design is intended to shorten the study duration in which there is prior information about the dose range and is useful in pediatric populations.
  • The “biased coin up-and-down design” requires that the treatment response or the toxicity evaluation is observed quickly, allocates a dose to each patient based on the toxicity information of the last completed subject and allows multiple patients to be concurrently studied.
  • Another rule-based design allows subsequent patients to be assigned to doses according to the toxicity outcomes at the current dose by calculating the toxicity probability interval under the beta-binomial model.
  • Model-based designs use statistical models that look for a dose level that produces a probability of doselimiting toxicity by using toxicity data from all enrolled patients to compute a more precise dose-toxicity curve.
  • Bayesian models are commonly used. These models require an estimation of θ (characterizes the shape of the dose-toxicity curve.) Occurrence of toxicity results in adjustment of θ based on Bayes’ theorem. These designs provide a confidence interval for recommended doses for Phase II clinical trials. The continual reassessment method was the first Bayesian model-based method used in Phase I clinical trial designs. The initial estimate of θ is sought from experts familiar with the preclinical data or who have experience with similar drugs. Patients are treated at the dose thought to be closest to the MTD and estimation of the probability of a dose limiting toxicity is calculated for each new patient who enters the study until a prespecified condition is met at which time the trial is stopped.

Modifications of this method have included:-

  1. treating the patient at the lowest started dose level,
  2. increasing the dose by only one prespecified level at a time,
  3. not allowing dose escalation for the immediate next patient if a previous patient experienced a dose-limiting toxicity,
  4. treating several patients at the same dose level and expanding the cohort of patients.

Escalation with overdose control was suggested as an alternative Bayesian approach to overcome the limitation of patients being exposed to high toxic doses.

Other model-based designs include time-to-event endpoint and the efficacy and toxicity methods. These model-based methods result in good estimations of the target probability of DLT at the recommended dose for Phase II clinical trials without treating too many patients at a suboptimal dose. Dose-escalation strategies for trials of combinations of agents have included alternate escalation of the agents in the series of dose levels, simultaneous escalation of both agents, escalation of one agent to the recommended dose for Phase II trials while holding the other agent at a fixed dose, and escalation of one agent to the recommended dose for Phase II trials while holding the other agent at a low dose. In a review, Riviere and colleagues determined that 88% of the trials had a traditional or modified 3 + 3 dose escalation design used. The calculated median DLT rate was 6%. The authors recommended that the starting doses, dose levels, and dose-escalation steps must ensure patient safety, treat as few patients as possible at subtherapeutic doses, and identify optimal drug combinations for further evaluation. No specific clinical trial designs have been formulated for molecularly targeted agents that have a proven relevant target and a validated method for measuring target inhibition.

Phase II Clinical Trials:- Phase I/II dose finding studies determine the most successful dose (MSD) which is the dose which maximizes the product of the probability of seeing no toxicity together with the probability of seeing a therapeutic response. While a Phase I clinical study focuses on determining the MTD, Phase II studies evaluate potential efficacy and characterizes treatment benefit for the disease in a convincing manner. The intervention is not presumed to have

any therapeutic effect whatsoever. These studies are performed on larger groups (100 to 300 subjects) and are designed to assess how well the drug works and to continue safety assessments. Therapeutic doses which were determined during Phase I are administered and patients are monitored by the clinical researcher. Trials are often conducted in a multi-institution setting.

Phase II may be divided into

  1. Phase IIA which are pilot clinical trials to evaluate efficacy and safety in selected populations with the disease or condition to be treated, diagnosed or prevented (objectives may be on dose-response, type of patient, frequency of dosing, or other identifiers of safety and efficacy) and
  2. Phase IIB which are the most rigorous trials designed to demonstrate efficacy.

The development process usually fails during this Phase II when the drug is discovered not to work as planned or to have toxic effects. The Phase II design depends on the quality and adequacy of Phase I studies. A vulnerable aspect of both phases is the type of patient enrolled. Patients in Phase II trials generally have more exclusion criteria than those in Phase III trials. Case series and randomized clinical trial designs have been used. Single stage and multi-stage Phase II clinical trial designs are often developed on the basis that one endpoint is of interest. A commonly used Phase II design is based on the work of Gehan, a version of a two-stage design. Other designs have more stages or a sequential aspect. Hybrid designs have been used to improve efficiency. In an update, Gehan reviewed statistical aspects of plans for Phase II cancer clinical trials including a minimum number of patients plan, a two-stage decision theory approach, a limited patient accrual plan, a predictive probability plan, and a one-sample multiple testing procedure plan. The author makes recommendations regarding the plan that best fits the needs of the study.

  • Adaptive clinical trial designs based on accumulated data at interim have also been used in Phase II clinical trials because of flexibility and efficiency. This design may allow the researcher to modify or redesign the trial while the study is ongoing. However, researchers have hesitated in their use-there is confusion with respect to definition, controversy regarding sample size re-estimation methods, and logistical barriers in using adaptive designs within existing trial frameworks.
  • In 2010, The FDA classified adaptive designs into “well understood” and “less well understood”
  1. “Well understood” designs have been in use for years with corresponding statistical methods that have been well established and the FDA is familiar with the study designs through the review of submissions using them.
  2. In the “less well understood” designs, relative merits and limitations have not been completely evaluated, valid statistical methods have not been developed, and the FDA does not have a lot of experience with submissions using the study designs. Chow et al. give a broader definition of adaptive design-one that allows adaptations in trial procedures and/or statistical procedures after initiation of the trial without undermining the validity and integrity of the trial.
  • Adaptive clinical trial designs include an:-
  1. adaptive randomization design,
  2. an adaptive group sequential design,
  • a flexible sample size re-estimation design,
  1. a drop-the-losers design,
  2. an adaptive dose-finding design,
  3. a biomarker-adaptive design,
  • an adaptive treatments witching design,
  • an adaptive-hypothesis design,
  1. a Phase I/II or II/III adaptive seamless trial design and
  2. a multiple adaptive design.

Phase III Clinical Trials:- Phase III trials are the full scale evaluation of treatment and are designed to compare efficacy of the new treatment with the standard treatment. These are the most rigorous and extensive type of scientific clinical investigation of a new treatment. This is the “pre-marketing phase” of clinical trials. These are usually the most expensive and time-consuming of the trials. The trials may be difficult to design and run. Large groups (100 to 3000 subjects) are recruited and trial designs have included randomized controlled trials (parallel design), uncontrolled trials (single treatment), historical controls, no-randomized concurrent trials, factorial designs, and group sequential designs. Patients are monitored by the clinical researcher and personal physician.

Phase III clinical trials may be divided into:-

  • Phase IIIA which are trials done after efficacy of the therapy is demonstrated but before regulatory submission of a New Drug Application (NDA) or other dossier and
  • Phase IIIB which are conducted after submission of an NDA or other dossier but before approval and launch.

Traditional endpoints for trials have included overall survival, time to tumor progression, overall response rate, time to treatment failure and patient-reported outcomes. Overall survival has been the gold standard for the demonstration of clinical benefits. Subpart H allows for accelerated approval of drugs for serious and life threatening diseases where the drug demonstrates an advantage over available therapy. This is based on a surrogate endpoint that likely predicts clinical benefit. While randomized Phase III clinical trials have been the gold standard evidence for the approval of new drugs, problems associated with drug development have included limited clinical benefit in large RCT’s, prediction of a successful Phase III trial from Phase II data, determination of toxicity, design of studies with drug combinations, and cost of the trial.

In 2010, the FDA published guidance on adaptive design clinical trials. Evaluators of adaptive clinical trial studies answer the following 6 questions:

1) Is there a good rationale and have alternative designs been considered?

2) Does the proposal fit well in the context of the development program and the data that will be available for the marketing authorization application?

3) Can the proposal be implemented without important damage to trial integrity?

4) Is the type I error rate controlled?

5) Has the potential bias of treatment effect estimates been evaluated?

6) Is the proposal practical and feasible?

These questions are also asked of other designs. The European Organisation for Research and Treatment of Cancer recognize that these designs can be advantageous, but warn that they must prevent bias that could be uncontrollable. Recommended techniques include randomisation, blinding, prospectively planned adaptations and upfront implementation of the process and firewalls needed to ensure restricted access to interim analysis results and blinding of staff involved in day-to-day trial proceedings.

Phase IV Clinical Trials:- Upon authorization by the FDA, therapies determined to have proven safety, efficacy and quality may be made available to the general population. Patients and their physicians have expectations of benefit. However, not all safety or efficacy issues have been determined. The FDA requires continued evaluation after release to evaluate safety signs that may affect the benefit-risk ratio. These Phase IV studies include “all studies (other than routine surveillance) performed after drug approval and related to the approved indication”. These are post-marketing surveillance studies. The focus of the trials is on how drugs work in the real world. Anyone seeking treatment from their physician may be treated with the therapy. Their personal physician monitors the results of treatment. Efficacy and detection of rare or long-term adverse effects over a much larger patient population and longer time period are evaluated, healthcare costs and outcomes are determined, and pharmacogenetics are studied. New clinical indications for a drug may be established and large number of patients and physicians are involved. The FDA may require that a developer conduct a Phase IV trial as a stipulation for drug approval. Less than half of studies are completed or even initiated by developers. Phase IV trials may result in a drug being removed from the market or restricted to certain indications. Initially, these trials were run much like Phase III studies and were conducted for marketing purposes. Studies were done at institutions with investigators familiar with clinical trials and had inclusion and exclusion criteria similar to those of Phase III studies. Results did not reflect what would happen under normal conditions. As a result, innovative studies were designed to involve ordinary physicians in naive research communities. Goals have been broadened and include evaluation of specific pharmacological effects, establishing the incidence of adverse reactions, determining effects of long-term administration of a therapy, establishing a new clinical indication for the therapy, evaluation of the therapy in higher risk populations, etc. A main issue of concern is the mix of medical research and clinical practice. Reported serious adverse drug reactions submitted to the FDA’s Med Watch program have increased from 150,000 in 2000 to 370,000 in 2009. Physician and consumers or drug manufacturers submit these reports. Criticisms have included reliance on voluntary reporting of adverse events, trust in drug manufacturers to collect/ evaluate/report drug safety data that may risk financial interests, and dependence on one government body to approve a drug and then require studies that might lead to withdrawal from the market. Preffered solutions have included large-scale simple RCTs with few eligibility and treatment criteria , preplanned meta analyses of a series of related trials, and establishment of a national health data network to evaluate post-marketing surveillance independent of the FDA-approval process.

Phase V Clinical Trials:- This translational research is designed to “move from bench to bedside”. Phase V clinical trials refer to comparative effectiveness research and community-based research. Research is done on data collected. All reported uses are evaluated. Patients are not monitored. Its main focus is to determine integration of a new therapy into wide spread clinical practice. Filed under: cornell cooperative extension, evidence-based living, policy, the learning center tagged with: cooperative extension programs, evaluation, evidence-based programs, research methods, research translation.


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