Clinical trial

In health care, clinical trials are conducted to allow safety and efficacy data to be collected for new drugs or devices. Efficacy is the capacity to produce a desired size of an effect under Ideal or Optimal conditions These trials can only take place once satisfactory information has been gathered on the quality of the product and its non-clinical safety, and Health Authority/Ethics Committee approval is granted in the country where the trial is taking place. An institutional review board (IRB also known as an independent ethics committee (IEC or ethical review board (ERB is a Committee that has been Depending on the type of product and the stage of its development, clinical trials enrol healthy volunteers and/or patients into small studies initially, followed by larger scale studies in patients that often compare the new product with the currently prescribed treatment. As positive safety data is gathered, the number of patients can be increased. Clinical trials can vary in size from a single centre in a single country to multi-centres in multiple countries. The Health Authority in the USA is called the FDA (Food and Drug Administration) where a new product application is referred to as an Investigational New Drug application. In Europe, applications are assessed by national Health Authorities and are called Clinical Trial Applications for Investigational Medicinal Products, for example the MHRA (Medicines and Healthcare products Regulatory Agency) in the UK or the MPA (Medical Products Agency) in Sweden.

Overview

In a clinical trial, the investigator first identifies the medication or device to be tested. Then the investigator decides what to compare it with (one or more existing treatments or a placebo), and what kind of patients might benefit from the medication/device. If the investigator cannot obtain enough patients with this specific disease or condition at his or her own location, then he or she assembles investigators at other locations who can obtain the same kind of patients to receive the treatment. During the clinical trial, the investigators: recruit patients with the predetermined characteristics, administer the treatment(s), and collect data on the patients' health for a defined time period. (These data include things like vital signs, amount of study drug in the blood, and whether the patient's health gets better or not. Vital signs are measures of various physiological statistics often taken by Health professionals in order to assess the most basic body functions ) The researchers send the data to the trial sponsor, who then analyzes the pooled data using statistical tests. A statistical hypothesis test is a method of making statistical decisions using experimental data Some examples of what a clinical trial may be designed to do:

assess the safety and effectiveness of a new medication or device on a specific kind of patient (e. g. , patients who have been diagnosed with Alzheimer's disease for less than one year)
assess the safety and effectiveness of a different dose of a medication than is commonly used (e. Alzheimer's disease ( AD) also called Alzheimer disease or simply Alzheimer's, is the most common form of Dementia. g. , 10 mg dose instead of 5 mg dose)
assess the safety and effectiveness of an already marketed medication or device for a new indication, i. e. a disease for which the drug is not approved yet
assess whether the new medication or device is more effective for the patient's condition than the already used, standard medication or device ("the gold standard" or "standard therapy")
compare the effectiveness in patients with a specific disease of two or more already approved or common interventions for that disease (e. g. , Device A vs. Device B, Therapy A vs. Therapy B)

Note that while most clinical trials compare two medications or devices, some trials compare three or four medications, doses of medications, or devices against each other.

Except for very small trials limited to a single location, the clinical trial design and objectives are written into a document called a clinical trial protocol. A Clinical Trial Protocol is a document that describes the objective(s design methodology statistical considerations and organization of a Clinical trial. The protocol is the 'operating manual' for the clinical trial, and ensures that researchers in different locations all perform the trial in the same way on patients with the same characteristics. (This uniformity is designed to allow the data to be pooled. ) A protocol is always used in multicenter trials.

Because the researchers test hypotheses and observe what happens, clinical trials can be seen as the application of the scientific method to understanding human or animal biology. A hypothesis (from Greek) consists either of a suggested explanation for a phenomenon (an event that is observable or of a reasoned proposal suggesting a possible Scientific method refers to bodies of Techniques for investigating phenomena

Synonyms for 'clinical trials' include clinical studies, research protocols and medical research. This article deals with the general meaning of the term "synonym" Biomedical research (or experimental medicine) in general simply known as medical research, is the Basic research or Applied research conducted

The most commonly performed clinical trials evaluate new drugs, medical devices (like a new catheter), biologics, psychological therapies, or other interventions. Medication, also referred to as medicine, can be loosely defined as any substance intended for use in the diagnosis cure mitigation treatment or prevention of disease In Medicine a catheter is a tube that can be inserted into a body cavity duct or vessel Biologics include a wide range of medicinal products such as Vaccines Blood and blood components allergenics Somatic cells Gene therapy, Clinical trials may be required before the national regulatory authority^[1] will approve marketing of the drug or device, or a new dose of the drug, for use on patients.

History

Clinical trials were first introduced in Avicenna's The Canon of Medicine in 1025 AD, in which he laid down rules for the experimental use and testing of drugs and wrote a precise guide for practical experimentation in the process of discovering and proving the effectiveness of medical drugs and substances. TemplateInfobox Muslim scholars --> ( Persian /ابو علی الحسین ابن عبدالله ابن سینا (born The Canon of Medicine ( Arabic: القانون في الطب Al-Qanun fi al-Tibb " The Law of Medicine " Persian In scientific inquiry an experiment ( Latin: Ex- periri, "to try out" is a method of investigating particular types of research questions or For the episode of the American television series The Office, see " Drug Testing " A drug, broadly speaking is any chemical substance that when absorbed into the body A chemical substance is a Material with a definite chemical composition. ^[2] He laid out the following rules and principles for testing the effectiveness of new drugs and medications, which still form the basis of modern clinical trials:^[3]^[4]

"The drug must be free from any extraneous accidental quality. Medication, also referred to as medicine, can be loosely defined as any substance intended for use in the diagnosis cure mitigation treatment or prevention of disease "
"It must be used on a simple, not a composite, disease. "
"The drug must be tested with two contrary types of diseases, because sometimes a drug cures one disease by its essential qualities and another by its accidental ones. "
"The quality of the drug must correspond to the strength of the disease. For example, there are some drugs whose heat is less than the coldness of certain diseases, so that they would have no effect on them. "
"The time of action must be observed, so that essence and accident are not confused. "
"The effect of the drug must be seen to occur constantly or in many cases, for if this did not happen, it was an accidental effect. "
"The experimentation must be done with the human body, for testing a drug on a lion or a horse might not prove anything about its effect on man. "

One of the most famous clinical trials was James Lind's demonstration in 1747 that citrus fruits cure scurvy. James Lind or Jim Lind is the name of James Lind (physician (1716 - 1794 British doctor James F Citrus is a common term and Genus of Flowering plants in the family Rutaceae, originating in tropical and subtropical southeast regions of Scurvy (NLat scorbutus is a disease resulting from a deficiency of Vitamin C, which is required for the synthesis of Collagen in humans ^[5] He compared the effects of various different acidic substances, ranging from vinegar to cider, on groups of afflicted sailors, and found that the group who were given oranges and lemons had largely recovered from scurvy after 6 days.

Types

One way of classifying clinical trials is by the way the researchers behave.

In an observational study, the investigators observe the subjects and measure their outcomes. The researchers do not actively manage the experiment. This is also called a natural experiment. A natural or Quasi-experiment is a naturally occurring instance of observable phenomena which approximate or duplicate the properties of a controlled Experiment. An example is the Nurses' Health Study. The Nurses' Health Study, established in 1976 by Dr Frank Speizer, and the Nurses' Health Study II, established in 1989 by Dr
In an interventional study, the investigators give the research subjects a particular medicine or other intervention. (Usually they compare the treated subjects to subjects who receive no treatment or standard treatment. ) Then the researchers measure how the subjects' health changes.

Another way of classifying trials is by their purpose. The U. S. National Institutes of Health (NIH) organizes trials into five (5) different types:

Prevention trials: look for better ways to prevent disease in people who have never had the disease or to prevent a disease from returning. "NIH" redirects here For other meanings of NIH see NIH (disambiguation. These approaches may include medicines, vitamins, vaccines, minerals, or lifestyle changes.
Screening trials: test the best way to detect certain diseases or health conditions.
Diagnostic trials: conducted to find better tests or procedures for diagnosing a particular disease or condition.
Treatment trials: test experimental treatments, new combinations of drugs, or new approaches to surgery or radiation therapy.
Quality of Life trials: explore ways to improve comfort and the quality of life for individuals with a chronic illness (a. k. a. Supportive Care trials).

Design

A fundamental distinction in evidence-based medicine is between observational studies and randomized controlled trials. Evidence-based medicine (EBM aims to apply Evidence gained from the Scientific method to certain parts of medical practice In Statistics, an observational study draws inferences about the effect of a treatment on subjects where the assignment of subjects into a treated group versus a Control A randomized controlled trial (RCT is a type of scientific Experiment most commonly used in testing the Efficacy or Effectiveness of Healthcare Types of observational studies in epidemiology such as the cohort study and the case-control study provide less compelling evidence than the randomized controlled trial. In Statistics, an observational study draws inferences about the effect of a treatment on subjects where the assignment of subjects into a treated group versus a Control Epidemiology is the study of factors affecting the Health and Illness of populations and serves as the foundation and Logic of interventions made in the A cohort study or panel study is a form of Longitudinal study used in Medicine and Social science. Case-control is a type of Epidemiological Study design. Case-control studies are used to identify factors that may contribute to a medical condition by comparing subjects In observational studies, the investigators only observe associations (correlations) between the treatments experienced by participants and their health status or diseases. In Statistics, an observational study draws inferences about the effect of a treatment on subjects where the assignment of subjects into a treated group versus a Control

A randomized controlled trial is the study design that can provide the most compelling evidence that the study treatment causes the expected effect on human health.

Currently, some Phase II and most Phase III drug trials are designed as randomized, double blind, and placebo-controlled. The blind method is a part of the Scientific method, used to prevent research outcomes from being influenced by either the Placebo effect or the Observer Placebo is a substance or procedure a patient accepts as medicine or therapy but which has no specific therapeutic activity

Randomized: Each study subject is randomly assigned to receive either the study treatment or a placebo.
Blind: The subjects involved in the study do not know which study treatment they receive. If the study is double-blind, the researchers also do not know which treatment is being given to any given subject. This 'blinding' is to prevent biases, since if a physician knew which patient was getting the study treatment and which patient was getting the placebo, he/she might be tempted to give the (presumably helpful) study drug to a patient who could more easily benefit from it. In addition, a physician might give extra care to only the patients who receive the placebos to compensate for their ineffectiveness. A form of double-blind study called a "double-dummy" design allows additional insurance against bias or placebo effect. In this kind of study, all patients are given both placebo and active doses in alternating periods of time during the study.
Placebo-controlled: The use of a placebo (fake treatment) allows the researchers to isolate the effect of the study treatment.

Of note, during the last ten years or so it has become a common practice to conduct "active comparator" studies (also known as "active control" trials). In other words, when a treatment exists that is clearly better than doing nothing for the subject (i. e. giving them the placebo), the alternate treatment would be a standard-of-care therapy. The study would compare the 'test' treatment to standard-of-care therapy.

Although the term "clinical trials" is most commonly associated with the large, randomized studies typical of Phase III, many clinical trials are small. They may be "sponsored" by single physicians or a small group of physicians, and are designed to test simple questions. In the field of rare diseases sometimes the number of patients might be the limiting factor for a clinical trial. Other clinical trials require large numbers of participants (who may be followed over long periods of time), and the trial sponsor is a private company, a government health agency, or an academic research body such as a university.

In designing a clinical trial, a sponsor must decide on the target number of patients who will participate. The sponsor's goal usually is to obtain a statistically significant result showing a significant difference in outcome (e. g. , number of deaths after 28 days in the study) between the groups of patients who receive the study treatments. The number of patients required to give a statistically significant result depends on the question the trial wants to answer. (For example, to show the effectiveness of a new drug in a non-curable disease as metastatic kidney cancer requires many fewer patients than in a highly curable disease as seminoma if the drug is compared to a placebo). Seminoma is one type of Testicular cancer that is believed to originate from the germinal epithelium of the Seminiferous tubules Presentation

The number of patients enrolled in a study has a large bearing on the ability of the study to reliably detect the size of the effect of the study intervention. This is described as the "power" of the trial. The power of a statistical test is the probability that the test will reject a false Null hypothesis (that it will not make a Type II error) The larger the sample size or number of participants in the trial, the greater the statistical power. However, in designing a clinical trial, this consideration must be balanced with the fact that more patients make for a more expensive trial. ^[6]

Phases

Clinical trials involving new drugs are commonly classified into four phases. Each phase of the drug approval process is treated as a separate clinical trial. The drug-development process will normally proceed through all four phases over many years. If the drug successfully passes through Phases I, II, and III, it will usually be approved by the national regulatory authority for use in the general population. Phase IV are 'post-approval' studies.

Before pharmaceutical companies start clinical trials on a drug, they conduct extensive pre-clinical studies. Pre-clinical development is a stage of research that begins before Clinical trials (testing in humans can begin and during which important feasibility iterative testing and

Pre-clinical studies

Pre-clinical studies involve in vitro (i. In vitro ( Latin: within the glass refers to the technique of performing a given experiment in a controlled environment outside of a living Organism e. , test tube or laboratory) studies and trials on animal populations (in vivo). In vivo ( Latin: within the living means that which takes place inside an organism. Wide-ranging dosages of the study drug are given to the animal subjects or to an in-vitro substrate in order to obtain preliminary efficacy, toxicity and pharmacokinetic information and to assist pharmaceutical companies in deciding whether it is worthwhile to go ahead with further testing. Efficacy is the capacity to produce a desired size of an effect under Ideal or Optimal conditions Toxicity is the degree to which a substance is able to damage an exposed organism Pharmacokinetics (in Greek: “pharmacon” meaning drug and “kinetikos” meaning putting in motion the study of time dependency sometimes abbreviated as “PK” is a

Phase 0

Phase 0 is a recent designation for exploratory, first-in-human trials conducted in accordance with the U. A first-in-man study is a Clinical trial where a medical procedure previously developed and assessed through In vitro or Animal testing, or S. Food and Drug Administration’s (FDA) 2006 Guidance on Exploratory Investigational New Drug (IND) Studies. The United States Food and Drug Administration 's investigational new drug (IND program is the means by which a pharmaceutical company obtains permission to ship an ^[7] Phase 0 trials are also known as human microdosing studies and are designed to speed up the development of promising drugs or imaging agents by establishing very early on whether the drug or agent behaves in human subjects as was anticipated from preclinical studies. Microdosing is a technique for studying the behaviour of compounds In vivo through the administration of doses so low they are unlikely to produce whole-body effects but high Imaging agents are chemicals designed to allow clinicians to determine whether a mass is benign or Malignant and locate metastatic Cancer sites Distinctive features of Phase 0 trials include the administration of single subtherapeutic doses of the study drug to a small number of subjects (10 to 15) to gather preliminary data on the agent's pharmacokinetics (how the body processes the drug) and pharmacodynamics (how the drug works in the body). Pharmacokinetics (in Greek: “pharmacon” meaning drug and “kinetikos” meaning putting in motion the study of time dependency sometimes abbreviated as “PK” is a Pharmacodynamics is the study of the Biochemical and Physiological effects of drugs on the body or on microorganisms or parasites within or on the body and the mechanisms

A Phase 0 study gives no data on safety or efficacy, being by definition a dose too low to cause any therapeutic effect. Drug development companies carry out Phase 0 studies to rank drug candidates in order to decide which has the best PK parameters in humans to take forward into further development. They enable base go/no go decisions to be based on relevant human models instead of relying on animal data, which can be unpredictive and vary between species.

Phase I

Phase I trials are the first stage of testing in human subjects. Normally, a small (20-80) group of healthy volunteers will be selected. This phase includes trials designed to assess the safety (pharmacovigilance), tolerability, pharmacokinetics, and pharmacodynamics of a drug. Pharmacovigilance (PV is the pharmacological Science relating to the detection assessment understanding and prevention of adverse effects, particularly Pharmacokinetics (in Greek: “pharmacon” meaning drug and “kinetikos” meaning putting in motion the study of time dependency sometimes abbreviated as “PK” is a Pharmacodynamics is the study of the Biochemical and Physiological effects of drugs on the body or on microorganisms or parasites within or on the body and the mechanisms These trials are often conducted in an inpatient clinic, where the subject can be observed by full-time staff. A patient is any person who receives medical attention care or treatment. The subject who receives the drug is usually observed until several half-lives of the drug have passed. The biological half-life of a substance is the time it takes for a substance (drug radioactive nuclide or other to lose half of its pharmacologic physiologic or radiologic activity Phase I trials also normally include dose-ranging, also called dose escalation, studies so that the appropriate dose for therapeutic use can be found. A dose-ranging study is a Clinical trial where different doses of an Agent (e The tested range of doses will usually be a fraction of the dose that causes harm in animal testing. Animal testing or animal research is the use of non-human Animals in scientific experimentation. Phase I trials most often include healthy volunteers. However, there are some circumstances when real patients are used, such as patients who have end-stage disease and lack other treatment options. Terminal illness is a medical term popularized in the 20th century to describe an active and Malignant Disease that cannot be cured or adequately treated This exception to the rule most often occurs in oncology (cancer) and HIV drug trials. Human immunodeficiency virus ( HIV) is a Lentivirus (a member of the Retrovirus family that can lead to acquired immunodeficiency syndrome Volunteers are paid an inconvenience fee for their time spent in the volunteer centre. Pay ranges from a small amount of money for a short period of residence, to a larger amount of up to approx £4000 depending on length of participation.

There are different kinds of Phase I trials:

SAD: Single Ascending Dose studies are those in which small groups of patients are given a single dose of the drug while they are observed and tested for a period of time. If they do not exhibit any adverse side effects, and the pharmacokinetic data is roughly in line with predicted safe values, the dose is escalated, and a new group of patients is then given a higher dose. An adverse event (AE is any adverse change in health or "side-effect" that occurs in a person who participates in a Clinical trial while the patient is receiving the This is continued until pre-calculated pharmacokinetic safety levels are reached, or intolerable side effects start showing up (at which point the drug is said to have reached the Maximum tolerated dose (MTD).

MAD: Multiple Ascending Dose studies are conducted to better understand the pharmacokinetics & pharmacodynamics of multiple doses of the drug. In these studies, a group of patients receives multiple low doses of the drug, whilst samples (of blood, and other fluids) are collected at various time points and analyzed to understand how the drug is processed within the body. The dose is subsequently escalated for further groups, up to a predetermined level.

Food effect: A short trial designed to investigate any differences in absorption of the drug by the body, caused by eating before the drug is given. These studies are usually run as a crossover study, with volunteers being given two identical doses of the drug on different occasions; one while fasted, and one after being fed. A crossover trial also referred to as a crossover study is a Clinical trial in which patients are given all of the medications to be studied or one medication and

Phase II

Once the initial safety of the study drug has been confirmed in Phase I trials, Phase II trials are performed on larger groups (20-300) and are designed to assess how well the drug works, as well as to continue Phase I safety assessments in a larger group of volunteers and patients. When the development process for a new drug fails, this usually occurs during Phase II trials when the drug is discovered not to work as planned, or to have toxic effects.

Phase II studies are sometimes divided into Phase IIA and Phase IIB. Phase IIA is specifically designed to assess dosing requirements (how much drug should be given), whereas Phase IIB is specifically designed to study efficacy (how well the drug works at the prescribed dose(s)).

Some trials combine Phase I and Phase II, and test both efficacy and toxicity.

Trial design

Some Phase II trials are designed as case series, demonstrating a drug's safety and activity in a selected group of patients. A case series (also known as a clinical series) is a medical research study that tracks patients with a known exposure given similar treatment or examines their medical records Other Phase II trials are designed as randomized clinical trials, where some patients receive the drug/device and others receive placebo/standard treatment. A randomized controlled trial (RCT is a type of scientific Experiment most commonly used in testing the Efficacy or Effectiveness of Healthcare Randomized Phase II trials have far fewer patients than randomized Phase III trials.

Phase III

Phase III studies are randomized controlled multicenter trials on large patient groups (300–3,000 or more depending upon the disease/medical condition studied) and are aimed at being the definitive assessment of how effective the drug is, in comparison with current 'gold standard' treatment. A multicenter research trial is a Clinical trial conducted at more than one medical center or clinic Because of their size and comparatively long duration, Phase III trials are the most expensive, time-consuming and difficult trials to design and run, especially in therapies for chronic medical conditions. In Medicine, a chronic disease is a Disease that is long-lasting or recurrent

It is common practice that certain Phase III trials will continue while the regulatory submission is pending at the appropriate regulatory agency. This allows patients to continue to receive possibly lifesaving drugs until the drug can be obtained by purchase. Other reasons for performing trials at this stage include attempts by the sponsor at "label expansion" (to show the drug works for additional types of patients/diseases beyond the original use for which the drug was approved for marketing), to obtain additional safety data, or to support marketing claims for the drug. Studies in this phase are by some companies categorised as "Phase IIIB studies. "^[8]^[9]

While not required in all cases, it is typically expected that there be at least two successful Phase III trials, demonstrating a drug's safety and efficacy, in order to obtain approval from the appropriate regulatory agencies (FDA (USA), TGA (Australia), EMEA (European Union), etc. The Therapeutic Goods Administration or TGA is the regulatory body for therapeutic goods (including medicines medical devices gene technology and blood products in Australia The European Medicines Agency ( EMEA) is a European agency for the evaluation of medicinal products. ).

Once a drug has proved satisfactory after Phase III trials, the trial results are usually combined into a large document containing a comprehensive description of the methods and results of human and animal studies, manufacturing procedures, formulation details, and shelf life. This collection of information makes up the "regulatory submission" that is provided for review to the appropriate regulatory authorities^[1] in different countries. They will review the submission, and, it is hoped, give the sponsor approval to market the drug.

Most drugs undergoing Phase III clinical trials can be marketed under FDA norms with proper recommendations and guidelines, but in case of any adverse effects being reported anywhere, the drugs need to be recalled immediately from the market. While most pharmaceutical companies refrain from this practice, it is not abnormal to see many drugs undergoing Phase III clinical trials in the market. ^[10]

Phase IV

Phase IV trial is also known as Post Marketing Surveillance Trial. Phase IV trials involve the safety surveillance (pharmacovigilance) and ongoing technical support of a drug after it receives permission to be sold. Pharmacovigilance (PV is the pharmacological Science relating to the detection assessment understanding and prevention of adverse effects, particularly Phase IV studies may be required by regulatory authorities or may be undertaken by the sponsoring company for competitive (finding a new market for the drug) or other reasons (for example, the drug may not have been tested for interactions with other drugs, or on certain population groups such as pregnant women, who are unlikely to subject themselves to trials). The safety surveillance is designed to detect any rare or long-term adverse effects over a much larger patient population and longer time period than was possible during the Phase I-III clinical trials. Harmful effects discovered by Phase IV trials may result in a drug being no longer sold, or restricted to certain uses: recent examples involve cerivastatin (brand names Baycol and Lipobay), troglitazone (Rezulin) and rofecoxib (Vioxx). In Pharmacology, cerivastatin (Baycol Lipobay was a synthetic member of the class of Statins used to lower Cholesterol and prevent Cardiovascular Troglitazone (Rezulin Resulin or Romozin is an Anti-diabetic and Antiinflammatory drug and a member of the drug class of the Thiazolidinediones Rofecoxib (Rofecoxib is a nonsteroidal anti-inflammatory drug ( NSAID) marketed by Merck & Co

Length

Clinical trials are only a small part of the research that goes into developing a new treatment. Potential drugs, for example, first have to be discovered, purified, characterized, and tested in labs (in cell and animal studies) before ever undergoing clinical trials. In all, about 1,000 potential drugs are tested before just one reaches the point of being tested in a clinical trial. For example, a new cancer drug has, on average, at least 6 years of research behind it before it even makes it to clinical trials. But the major holdup in making new cancer drugs available is the time it takes to complete clinical trials themselves. On average, about 8 years pass from the time a cancer drug enters clinical trials until it receives approval from regulatory agencies for sale to the public. Drugs for other diseases have similar timelines.

Some reasons a clinical trial might last several years:

For chronic conditions like cancer, it takes months, if not years, to see if a cancer treatment has an effect on a patient.
For drugs that are not expected to have a strong effect (meaning a large number of patients must be recruited to observe any effect), recruiting enough patients to test the drug's effectiveness (i. e. , getting statistical power) can take several years.
Only certain people who have the target disease condition are eligible to take part in each clinical trial. Researchers who treat these particular patients must participate in the trial. Then they must identify the desirable patients and obtain consent from them or their families to take part in the trial.

The biggest barrier to completing studies is the shortage of people who take part. All drug and many device trials target a subset of the population, meaning not everyone can participate. Some drug trials require patients to have unusual combinations of disease characteristics. It is a challenge to find the appropriate patients and obtain their consent, especially when they may receive no direct benefit (because they are not paid, the study drug is not yet proven to work, or the patient may receive a placebo). In the case of cancer patients, fewer than 5% of adults with cancer will participate in drug trials. According to the Pharmaceutical Research and Manufacturers of America (PhRMA), about 400 cancer medicines were being tested in clinical trials in 2005. Not all of these will prove to be useful, but those that are may be delayed in getting approved because the number of participants is so low. ^[11]

Clinical trials that do not involve a new drug usually have a much shorter duration. (Exceptions are epidemiological studies like the Nurses' Health Study. The Nurses' Health Study, established in 1976 by Dr Frank Speizer, and the Nurses' Health Study II, established in 1989 by Dr )

Administration

Clinical trials designed by a local investigator and (in the U. S. ) federally funded clinical trials are almost always administered by the researcher who designed the study and applied for the grant. Small-scale device studies may be administered by the sponsoring company. Phase III and Phase IV clinical trials of new drugs are usually administered by a contract research organization (CRO) hired by the sponsoring company. A Contract Research Organization (CRO is an organization that offers clients a wide range of pharmaceutical research services (The sponsor provides the drug and medical oversight. ) A CRO is a company that is contracted to perform all the administrative work on a clinical trial. It recruits participating researchers, trains them, provides them with supplies, coordinates study administration and data collection, sets up meetings, monitors the sites for compliance with the clinical protocol, and ensures that the sponsor receives 'clean' data from every site. Recently, site management organizations have also been hired to coordinate with the CRO to ensure rapid IRB/IEC approval and faster site initiation and patient recruitment. Site management organization (SMO could refer to an individual a network of individuals or an organization that sub-contracts Clinical trial -related responsibilities from a

At a participating site, one or more research assistants (often nurses) do most of the work in conducting the clinical trial. The research assistant's job can include some or all of the following: providing the local Institutional Review Board (IRB) with the documentation necessary to obtain its permission to conduct the study, assisting with study start-up, identifying eligible patients, obtaining consent from them or their families, administering study treatment(s), collecting data, maintaining data files, and communicating with the IRB, as well as the sponsor (if any) and CRO (if any). An institutional review board (IRB also known as an independent ethics committee (IEC or ethical review board (ERB is a Committee that has been

Ethical conduct

Clinical trials are closely supervised by appropriate regulatory authorities. All studies that involve a medical or therapeutic intervention on patients must be approved by a supervising ethics committee before permission is granted to run the trial. The local ethics committee has discretion on how it will supervise noninterventional studies (observational studies or those using already collected data). In the U. S. , this body is called the Institutional Review Board (IRB). An institutional review board (IRB also known as an independent ethics committee (IEC or ethical review board (ERB is a Committee that has been Most IRBs are located at the local investigator's hospital or institution, but some sponsors allow the use of a central (independent/for profit) IRB for investigators who work at smaller institutions.

To be ethical, researchers must obtain the full and informed consent of participating human subjects. Informed consent is a legal condition whereby a person can be said to have given Consent based upon an appreciation and understanding of the facts implications (One of the IRB's main functions is ensuring that potential patients are adequately informed about the clinical trial. ) If the patient is unable to consent for him/herself, researchers can seek consent from the patient's legally authorized representative. In California, the state has prioritized the individuals who can serve as the legally authorized representative. California ( is a US state on the West Coast of the United States, along the Pacific Ocean.

In some U. S. locations, the local IRB must certify researchers and their staff before they can conduct clinical trials. They must understand the federal patient privacy (HIPAA) law and good clinical practice. The Health Insurance Portability and Accountability Act ( HIPAA) was enacted by the U International Conference of Harmonisation Guidelines for Good Clinical Practice (ICH GCP) is a set of standards used internationally for the conduct of clinical trials. Good Clinical Practice is an international quality standard that is provided by International Conference on Harmonisation (ICH an international body that defines standards The guidelines aim to ensure that the "rights, safety and well being of trial subjects are protected".

Safety

Responsibility for the safety of the subjects in a clinical trial is shared between the sponsor, the local site investigators (if different from the sponsor), the various IRBs that supervise the study, and (in some cases, if the study involves a marketable drug or device) the regulatory agency for the country where the drug or device will be sold.

Sponsor

For safety reasons, many clinical trials of drugs are designed to exclude women of childbearing age, pregnant women, and/or women who become pregnant during the study. In some cases the male partners of these women are also excluded or required to take birth control measures.
Throughout the clinical trial, the sponsor is responsible for accurately informing the local site investigators of the true historical safety record of the drug, device or other medical treatments to be tested, and of any potential interactions of the study treatment(s) with already approved medical treatments. This allows the local investigators to make an informed judgment on whether to participate in the study or not.
The sponsor is responsible for monitoring the results of the study as they come in from the various sites, as the trial proceeds. In larger clinical trials, a sponsor will use the services of a Data Monitoring Committee (DMC, known in the U. A Data Monitoring Committee (DMC sometimes also called Data Safety Monitoring Board or DSMB is an independent group of experts who monitor patient safety and treatment efficacy data while S. as a Data Safety Monitoring Board). This is an independent group of clinicians and statisticians. The DMC meets periodically to review the unblinded data that the sponsor has received so far. The DMC has the power to recommend termination of the study based on their review, for example if the study treatment is causing more deaths than the standard treatment, or seems to be causing unexpected and study-related serious adverse events. An adverse event (AE is any adverse change in health or "side-effect" that occurs in a person who participates in a Clinical trial while the patient is receiving the
The sponsor is responsible for collecting adverse event reports from all site investigators in the study, and for informing all the investigators of the sponsor's judgment as to whether these adverse events were related or not related to the study treatment. An adverse event (AE is any adverse change in health or "side-effect" that occurs in a person who participates in a Clinical trial while the patient is receiving the This is an area where sponsors can slant their judgment to favor the study treatment.
The sponsor and the local site investigators are jointly responsible for writing a site-specific informed consent that accurately informs the potential subjects of the true risks and potential benefits of participating in the study, while at the same time presenting the material as briefly as possible and in ordinary language. Informed consent is a legal condition whereby a person can be said to have given Consent based upon an appreciation and understanding of the facts implications FDA regulations and ICH guidelines both require that “the information that is given to the subject or the representative shall be in language understandable to the subject or the representative. " If the participant's native language is not English, the sponsor must translate the informed consent into the language of the participant. ^[12]

Local site investigators

A physician's first duty is to his/her patients, and if a physician investigator believes that the study treatment may be harming subjects in the study, the investigator can stop participating at any time. The Hippocratic Oath is an oath traditionally taken by physicians pertaining to the ethical practice of medicine On the other hand, investigators often have a financial interest in recruiting subjects, and can act unethically in order to obtain and maintain their participation.
The local investigators are responsible for conducting the study according to the study protocol, and supervising the study staff throughout the duration of the study.
The local investigator or his/her study staff are responsible for ensuring that potential subjects in the study understand the risks and potential benefits of participating in the study; in other words, that they (or their legally authorized representatives) give truly informed consent. Informed consent is a legal condition whereby a person can be said to have given Consent based upon an appreciation and understanding of the facts implications
The local investigators are responsible for reviewing all adverse event reports sent by the sponsor. (These adverse event reports contain the opinion of both the investigator at the site where the adverse event occurred, and the sponsor, regarding the relationship of the adverse event to the study treatments). The local investigators are responsible for making an independent judgment of these reports, and promptly informing the local IRB of all serious and study-treatment-related adverse events.
When a local investigator is the sponsor, there may not be formal adverse event reports, but study staff at all locations are responsible for informing the coordinating investigator of anything unexpected.
The local investigator is responsible for being truthful to the local IRB in all communications relating to the study.

IRBs

Approval by an IRB, or ethics board, is necessary before all but the most informal medical research can begin.

In commercial clinical trials, the study protocol is not approved by an IRB before the sponsor recruits sites to conduct the trial. However, the study protocol and procedures have been tailored to fit generic IRB submission requirements. In this case, and where there is no independent sponsor, each local site investigator submits the study protocol, the consent(s), the data collection forms, and supporting documentation to the local IRB. Universities and most hospitals have in-house IRBs. Other researchers (such as in walk-in clinics) use independent IRBs.
The IRB scrutinizes the study for both medical safety and protection of the patients involved in the study, before it allows the researcher to begin the study. It may require changes in study procedures or in the explanations given to the patient. A required yearly "continuing review" report from the investigator updates the IRB on the progress of the study and any new safety information related to the study.

Regulatory agencies

If a clinical trial concerns a new regulated drug or medical device (or an existing drug for a new purpose), the appropriate regulatory agency for each country where the sponsor wishes to sell the drug or device is supposed to review all study data before allowing the drug/device to proceed to the next phase, or to be marketed. However, if the sponsor withholds negative data, or misrepresents data it has acquired from clinical trials, the regulatory agency may make the wrong decision.
In the U. S. , the FDA can audit the files of local site investigators after they have finished participating in a study, to see if they were correctly following study procedures. The most general definition of an audit is an evaluation of a person organization system process project or product This audit may be random, or for cause (because the investigator is suspected of fraudulent data). Avoiding an audit is an incentive for investigators to follow study procedures.

Different countries have different regulatory requirements and enforcement abilities. "An estimated 40 percent of all clinical trials now take place in Asia, Eastern Europe, central and south America. “There is no compulsory registration system for clinical trials in these countries and many do not follow European directives in their operations”, says Dr. Jacob Sijtsma of the Netherlands-based WEMOS, an advocacy health organisation tracking clinical trials in developing countries. "[1]

Accidents

In March 2006 the drug TGN1412 caused catastrophic systemic organ failure in the individuals receiving the drug during its first human clinical trials (Phase I) in Great Britain. TGN1412 (also known as CD28-SuperMAB) is the working name of an Immunomodulatory drug which was withdrawn from development originally intended for the treatment of See also Kingdom of Great Britain Great Britain (Breatainn Mhòr Prydain Fawr Breten Veur Graet Breetain is the larger of the two main islands Following this, an Expert Group on Phase One Clinical Trials published a report. ^[13]

Economics

Sponsor

The cost of a study depends on many factors, especially the number of sites that are conducting the study, the number of patients required, and whether the study treatment is already approved for medical use. Clinical trials follow a standardized process.

The costs to a pharmaceutical company of administering a Phase III or IV clinical trial may include, among others:

manufacturing the drug(s)/device(s) tested
staff salaries for the designers and administrators of the trial
payments to the contract research organization, the site management organization (if used) and any outside consultants
payments to local researchers (and their staffs) for their time and effort in recruiting patients and collecting data for the sponsor
study materials and shipping
communication with the local researchers, including onsite monitoring by the CRO before and (in some cases) multiple times during the study
one or more investigator training meetings
costs incurred by the local researchers such as pharmacy fees, IRB fees and postage.
any payments to patients enrolled in the trial (all payments are strictly overseen by the IRBs to ensure that patients do not feel coerced to take part in the trial by overly attractive payments)

These costs are incurred over several years.

In the U. S. there is a 50% tax credit for sponsors of certain clinical trials. The term tax credit describes two different concepts The first is a recognition of partial payment already made towards Taxes due. ^[14]

National health agencies such as the U. S. National Institutes of Health offer grants to investigators who design clinical trials that attempt to answer research questions that interest the agency. "NIH" redirects here For other meanings of NIH see NIH (disambiguation. In these cases, the investigator who writes the grant and administers the study acts as the sponsor, and coordinates data collection from any other sites. These other sites may or may not be paid for participating in the study, depending on the amount of the grant and the amount of effort expected from them.

Investigators

Many clinical trials do not involve any money. However, when the sponsor is a private company or a national health agency, investigators are almost always paid to participate. These amounts can be small, just covering a partial salary for research assistants and the cost of any supplies (usually the case with national health agency studies), or be substantial and include 'overhead' that allows the investigator to pay the research staff during times in between clinical trials.

Patients

In Phase I drug trials, participants are paid because they give up their time (sometimes away from their homes) and are exposed to unknown risks, without the expectation of any benefit. In most other trials, however, patients are not paid, in order to ensure that their motivation for participating is the hope of getting better or contributing to medical knowledge, without their judgment being skewed by financial considerations. However, they are often given small reimbursements for study-related expenses like travel.

Acquiring participants

Newspaper advertisements seeking patients and healthy volunteers to participate in clinical trials.

Phase 0 and Phase I drug trials seek healthy volunteers. Most other clinical trials seek patients who have a specific disease or medical condition. Depending on the kind of participants required, sponsors use various recruitment strategies, including patient databases, newspaper and radio advertisements, flyers, posters in places the patients might go (such as doctor's offices), and personal conversations with the investigator. Various resources are available for individuals who want to participate in a clinical trial. A patient may ask their physician about clinical trials available for their condition or contact other clinics directly. The US government, World Health Organization and commercial organizations provide online clinical trial resources.

Notes

^ ^a ^b The regulatory authority in the USA is the Food and Drug Administration; in Canada, Health Canada; in the EU, the European Medicines Agency; in Japan, the Ministry of Health, Labour and Welfare; the Health Sciences Authority (HSA) in Singapore. Academic clinical trials are a valuable component of the health care system they benefit Patients and help determine the safety and efficacy of new drugs and devices Bioethics is the philosophical study of the ethical controversies brought about by advances in Biology and Medicine. The CIOMS Guidelines, formally known as International Ethical Guidelines for Biomedical Research Involving Human Subjects, is a set of ethical principles regarding Human A Clinical trial is the application of the Scientific method to human health Acquisition or collection of Clinical trial data can be achieved through various methods that may include but are not limited to any of the following paper or electronic medical records Clinical Data Interchange Standards Consortium ( CDISC) is a Non-profit organization, whose mission is "to develop and support global platform-independent data A clinical site is a Medical facility staffed with a Clinical investigator (MD and qualified for performing clinical research Community-based clinical trials are Clinical trials conducted directly through doctors and clinics rather than academic research facilities A Contract Research Organization (CRO is an organization that offers clients a wide range of pharmaceutical research services A Data Monitoring Committee (DMC sometimes also called Data Safety Monitoring Board or DSMB is an independent group of experts who monitor patient safety and treatment efficacy data while Drug development or preclinical development is defined in many pharmaceutical companies as the process of taking a new chemical lead through the stages necessary to allow it A drug recall removes a prescription or Over-the-counter drug from the market The electronic Common Technical Document (eCTD is an interface for the pharmaceutical industry to agency transfer of regulatory information In Health care, a Clinical trial is a comparison test of a Medication or other medical treatment (such as a Medical device) versus a Placebo The European Medicines Agency ( EMEA) is a European agency for the evaluation of medicinal products. A Special Protocol Assessment ( SPA) is a declaration from the Food and Drug Administration that an uncompleted Phase III trial 's design clinical endpoints Health care is the prevention treatment and management of illness and the preservation of mental health through the services offered by the medical, Nursing Health care often accounts for one of the largest areas of spending for both Governments and individuals all over the world and The International Federation of Pharmaceutical Manufacturers and Associations ( IFPMA) is a global non-profit NGO representing research-based pharmaceutical biotech An Investigational Device Exemption ( IDE) allows the investigational device to be used in a clinical study in order to collect safety and effectiveness data required Medical ethics is primarily a field of Applied ethics, the study of Moral values and judgments as they apply to Medicine. In its original application " nocebo " had a very specific meaning in the medical domains of Pharmacology, and Nosology, and Etiology. Nursing ethics is a branch of Applied ethics that concerns itself with activities in the field of Nursing. In the US, an orphan drug is any drug developed under the Orphan Drug Act of January 1983 ("ODA" a Federal law concerning Rare diseases The Philosophy of Healthcare is the study of the Ethics, Processes, and People which constitute the maintenance of health for human A randomized controlled trial (RCT is a type of scientific Experiment most commonly used in testing the Efficacy or Effectiveness of Healthcare A Remote Data Entry ( RDE) system is a computerized system designed for the collection of data in electronic format The World Medical Association (WMA an international organization of Physicians was formally established on September 17, 1947, pursuant to the resolutions Health Canada ( French: Santé Canada) is the department of the government of Canada with responsibility for national Public health The European Medicines Agency ( EMEA) is a European agency for the evaluation of medicinal products. The is one of Cabinet level ministries in the Japanese government.
^ Toby E. Huff (2003), The Rise of Early Modern Science: Islam, China, and the West, p. 218. Cambridge University Press, ISBN 0521529948. Cambridge University Press (known colloquially as CUP is a Publisher given a Royal Charter by Henry VIII in 1534
^ David W. Tschanz, MSPH, PhD (August 2003). "Arab Roots of European Medicine", Heart Views 4 (2).
^ D. Craig Brater and Walter J. Daly (2000), "Clinical pharmacology in the Middle Ages: Principles that presage the 21st century", Clinical Pharmacology & Therapeutics 67 (5), p. 447-450 [448].
^ James Lind: A Treatise of the Scurvy (1754) (2001). Year 2001 ( MMI) was a Common year starting on Monday according to the Gregorian calendar. Retrieved on 2007-09-09. Year 2007 ( MMVII) was a Common year starting on Monday of the Gregorian calendar in the 21st century. Events 1000 - Battle of Svolder, Viking Age. 1379 - Treaty of Neuberg, splitting the Austrian
^ The power of a trial is not a single, unique value; it estimates the ability of a trial to detect a difference of a particular size (or larger) between the treated (tested drug/device) and control (placebo or standard treatment) groups. For example, a trial of a lipid-lowering drug versus placebo with 100 patients in each group might have a power of . Lipids are broadly defined as any fat- Soluble ( lipophilic) naturally-occurring Molecule, such as fats oils waxes cholesterol sterols fat-soluble 90 to detect a difference between patients receiving study drug and patients receiving placebo of 10 mg/dL or more, but only have a power of . 70 to detect a difference of 5 mg/dL.
^ Guidance for Industry, Investigators, and Reviewers Exploratory IND Studies. Food and Drug Administration (January 2006). Retrieved on 2007-05-01. Year 2007 ( MMVII) was a Common year starting on Monday of the Gregorian calendar in the 21st century. Events 305 - Diocletian and Maximian retire from the office of Roman Emperor.
^ Guidance for Institutional Review Boards and Clinical Investigators. FDA (1999-03-16). Year 1999 ( MCMXCIX) was a Common year starting on Friday (link will display full 1999 Gregorian calendar) Events 597 BC - Babylonians capture Jerusalem, replace Jehoiachin with Zedekiah as king Retrieved on 2007-03-27. Year 2007 ( MMVII) was a Common year starting on Monday of the Gregorian calendar in the 21st century. Events 196 BC - Ptolemy V ascends to the throne of Egypt. 1309 - Pope Clement V excommunicates
^ Periapproval Services (Phase IIIb and IV programs). Covance Inc. (2005). Retrieved on 2007-03-27. Year 2007 ( MMVII) was a Common year starting on Monday of the Gregorian calendar in the 21st century. Events 196 BC - Ptolemy V ascends to the throne of Egypt. 1309 - Pope Clement V excommunicates
^ Arcangelo, Virginia Poole; Andrew M. Peterson (2005). Pharmacotherapeutics for Advanced Practice: A Practical Approach. Lippincott Williams & Wilkins. ISBN 0781757843.
^ Web Site Editor (2007). "Clinical Trials - What Your Need to Know" (in English). American Cancer Society.
^ http://www.gts-translation.com/medicaltranslationpaper.pdf| Back Translation for Quality Control of Informed Consent Forms
^ Expert Group on Phase One Clinical Trials (Chairman: Professor Gordon W. Duff) (2006-12-07). Year 2006 ( MMVI) was a Common year starting on Sunday of the Gregorian calendar. Events 43 BC - Marcus Tullius Cicero assassinated 1696 - Connecticut Route 108, one of the oldest highways Expert Group on Phase One Clinical Trials: Final report. The Stationery Office. The Stationery Office ( TSO) is a British publishing company that was created in 1996 when the publishing arm of Her Majesty's Stationery Office Retrieved on 2007-05-24. Year 2007 ( MMVII) was a Common year starting on Monday of the Gregorian calendar in the 21st century. Events 1218 - The Fifth Crusade leaves Acre for Egypt. 1276 - Magnus Ladulås is crowned
^ Tax Credit for Testing Expenses for Drugs for Rare Diseases or Conditions. FDA (2001-04-17). Year 2001 ( MMI) was a Common year starting on Monday according to the Gregorian calendar. Events 69 - After the First Battle of Bedriacum, Vitellius becomes Roman Emperor. Retrieved on 2007-03-27. Year 2007 ( MMVII) was a Common year starting on Monday of the Gregorian calendar in the 21st century. Events 196 BC - Ptolemy V ascends to the throne of Egypt. 1309 - Pope Clement V excommunicates

References

Rang HP, Dale MM, Ritter JM, Moore PK (2003). Pharmacology 5 ed. Edinburgh: Churchill Livingstone. ISBN 0-443-07145-4
Finn R, (1999). Cancer Clinical Trials: Experimental Treatments and How They Can Help You. , Sebastopol: O'Reilly & Associates. ISBN 1-56592-566-1
Chow S-C and Liu JP (2004). Design and Analysis of Clinical Trials : Concepts and Methodologies, ISBN 0-471-24985-8
Pocock SJ (2004), Clinical Trials: A Practical Approach, John Wiley & Sons, ISBN 0-471-90155-5

External links

Clinical Trials at the Open Directory Project

The Open Directory Project ( ODP) also known as dmoz (from directory

Dictionary

-noun

A comparison test of a medication or other medical treatment (such as a medical device), versus a placebo (inactive look-a-like), other medications or devices, or the standard medical treatment for a patient's condition.

© 2009 citizendia.org; parts available under the terms of GNU Free Documentation License, from http://en.wikipedia.org
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Contents

Overview

History

Types

Design

Phases

Pre-clinical studies

Phase 0

Phase I

Phase II

Trial design

Phase III

Phase IV

Length

Administration

Ethical conduct

Safety

Sponsor

Local site investigators

IRBs

Regulatory agencies

Accidents

Economics

Sponsor

Investigators

Patients

Acquiring participants

See also

Notes

References

External links

Dictionary

clinical trial

-noun