Post on 30-Dec-2015
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CLINICAL STUDY AND BASIC CONCEPT
GOOD CLINICAL PRACTICE
Presented by:
Aarohi Shah
M.Pharm
Dept of Pharmaceutics and Pharmaceutical Technology
CLINICAL STUDY AND BASIC CONCEPT
What is a Clinical Trial?
A clinical trial (clinical research) is a research study in human volunteers (preclinical trail – in animals) to answer specific health questions. Carefully conducted clinical trials are the fastest and safest way to find treatments that work in people and ways to improve health.
CLINICAL STUDY AND BASIC CONCEPT
Types of clinical trials
Treatment trials
Prevention trials
Diagnostic trials
Screening trials
Quality of Life trials
CLINICAL STUDY AND BASIC CONCEPT
Clinical trials, FDA approval
Before a company initiates clinical trials (i.e. testing in humans), it must conduct extensive experiments in animal and human cells and in live animals (Preclinical Trial) If this stage of testing is successful, the company files an Investigational New Drug (IND) application with the Food and Drug Administration (FDA) to request permission to conduct clinical trials.
CLINICAL STUDY AND BASIC CONCEPT
Clinical Trials
Preclinical testing
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IND
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FDA
Phase I Phase II Phase III F
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NDA
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FDA
FDA Phase IV
Years 3.5 1 2 3 2.5 12 Total
Additional post marketing testing
Test population
Lab and Animal Studies
20 to 80 healthy volunteers
100 to 300 patient volunteers
1000 to 3000 patient volunteers
Review process/ Approval
Success rate
5000 compounds evaluated
5 enter trials 1 approved
CLINICAL STUDY AND BASIC CONCEPTPreclinical trialsTrial carried out on to the animal species Objective: To evaluate safety, toxicity and tolerance data (by
applying the factor for conversion of animal data to human data)
StudyDrug metabolism pathwayPK of the drugPK-PD relationProtein bindingTissue distributionDevelopment of methodology for quantification of drug and metabolite in biological fluidLong term toxicity Placental transfer kinetic
CLINICAL STUDY AND BASIC CONCEPTPhase 1Trial carried out on healthy volunteers except AIDS
or Cancer.Study
Dose-concentration (in plasma)-response-toxicity studyIV, single dose study (for checking bioavailability)Radioactive tracer study (for evaluation of first pass metabolism)Evaluation of suitability of preclinical animal model (to predict pharmacological effect in human)Effect of food
CLINICAL STUDY AND BASIC CONCEPT
Phase 2First time trial on patient and conducted
in OPEN mannerStudy
Evaluation of difference in PK and PD between the healthy volunteer and patientTo search new therapeutic effect of the drug
CLINICAL STUDY AND BASIC CONCEPT
Phase 3
Study
Search less common side effect of drug (which is conc. independent)
Comparison with the marketed drug
Drug-drug interaction
Study in special population like age, sex race etc.
Develop the dosage form
CLINICAL STUDY AND BASIC CONCEPT
Phase 4
Post marketing surveillance
Not well planned study but random study
Some rare side effect or toxicity may come out
GOOD CLINICAL PRACTICE
Good Clinical Practice (GCP) is an international ethical and scientific quality standard for designing, recording and reporting trials that involve the participation of human subjects.
Compliance with this standard provides public assurance that the rights, safety and well being of trial subjects are protected, consistent with the principles that have their origin in the Declaration of Helsinki, and that the clinical trial data are credible.
Regulations tell you what you are required to do by law. Guidelines tell you the best way to do it
GOOD CLINICAL PRACTICE
FDA GCP RegulationsRegulations contained in 21 CFR Part 50, 56, and 312Part 50 (applies to consenting of subjects), Part 56 (applies to IRB responsibilities) and Part 312 (applies to IND submissions, sponsor responsibility, and investigator responsibility)
GCP Guidelines- International Conference on HarmonizationThe objective of ICH GCP Guidelines is to provide a unified standard for European Union, Japan and United States to facilitate the mutual acceptance of clinical data by the regulatory authorities in the jurisdiction.Published by the FDA in Federal Register in May, 1997Adopted by all parties as GCP standard (considered law in European Union; considered “final guidance” in the US)Based on the Declaration of Helsinki
GOOD CLINICAL PRACTICE
Some important terms (Glossary)InvestigatorSponsorSubject /Trial SubjectInvestigator’s BrochureNon Clinical StudyProtocolBlinding (Masking)Institutional Review Board (IRB)Adverse Event (AE)Serious Adverse Event (SAE)
GOOD CLINICAL PRACTICE
Elements of GCPIRBInvestigatorSponsorClinical trial protocol and protocol amendmentsInvestigator BrochureEssential documents
GOOD CLINICAL PRACTICE
Institutional review board (IRB) or Independent Ethics Committee (IEC)It consists of reasonable number of members, who collectively have qualifications and experience to review and evaluate the science and medical aspects as well as ethics of proposed trials.It should perform the functions in accordance with written procedures, maintain written records of its activities and minutes of its meetings and should comply with GCP.Acts as a safe guard to the rights of the trial subjectShould consider the qualification of the investigator for the proposed trialShould conduct continuing review of each ongoing trial at intervals appropriate to the degree of risk.
GOOD CLINICAL PRACTICE
Investigator Qualified to perform study should have
Appropriate education, training and experience to assume responsibility and should provide evidence of such qualifications.Sufficient time to devote to study timelines.Personally conduct or supervise study.Adequate and qualified staff and facilities.Awareness of and compliance with GCP.Familiar with the investigational product and inventory.Adherence to protocol requirements.Inform subject’s primary physicianEnsure adequate medical care for SAEs.Maintained records should be accurate, complete, legible and timely.
GOOD CLINICAL PRACTICE
Investigator-Communication with IRB
Obtaining written and dated IRB approved consent formSubmission of Investigational BrochureOngoing communication
Report of SAEsIND Safety ReportsSignificant protocol deviations
The investigator should submit written summaries of the status of the trial to the IRB annually or more frequently, if requested by the IRB
GOOD CLINICAL PRACTICE
Investigator- Communication with the Sponsor/CRO
Reporting of any AEs or SAEsNotification of changes in staff and addressRetention of all pertinent study information and records until notified in writing that records are no longer requiredCoordination of publication plansIf trial is blinded, the investigator should promptly document and explain to the sponsor any:
Premature unblindingAccidental unblinidingUnblinding due to serious adverse events
GOOD CLINICAL PRACTICE
Investigator-Communication with Study Subjects
Obtaining valid written informed consentThe information language should be non-technical and understandable to the subject/LAR/impartial Provide subject a copy of a fully executed consentProvide subject with any new informationAnswer questions at any timeThe investigator must inform the subject when medical care is needed for inter-current illness(es) of which investigator becomes aware.It is recommended that the investigator inform subject’s primary physician about subject’s participation in study. If subject wishes to withdraw from the study, the investigator should make reasonable effort to ascertain the reasons – while fully respecting the subject’s rights.
GOOD CLINICAL PRACTICE
Investigator- Investigator – Compliance with Protocol
The investigator should conduct the trial in compliance with:The protocol agreed to by the sponsorIf required, protocol agreed to by the regulatory authority(ies)Ultimately given approval by the IRB
The investigator should not implement any deviation from, or changes of the protocol without:
Agreement by the sponsorPrior review and documented approval from the IRB of an amendment Exception: where necessary to eliminate an immediate hazard (s) to trial subjects or when the changes involve only logistical or administrative aspects of the trial. However, as soon as possible, the implemented deviation or change, the reason for it, and, if appropriate, the proposed protocol amendment(s) should be submitted to:
– The IRB for review and approval– To the sponsor for agreement – If required, to the regulatory authorities
GOOD CLINICAL PRACTICE
Investigator – Investigational Products
It is the investigator’s responsibility for investigational product(s) accountability at the trial siteThe investigator or person who is designated by the investigator should maintain records of:
» The product(s) delivery to the site» The inventory at the site» The use by each subject» The return to the sponsor or disposition of unused
productsThe records should include:
Date, quantities, batch/serial numbers, expiration dates and the unique code numbers assigned to the product(s) and subjectsProducts should be stored as specified by the sponsor and in accordance with applicable regulatory requirementsShould explain to the subject:
Correct use of the productShould check at appropriate intervals that the subject is following the instructions properly to use the product
GOOD CLINICAL PRACTICE
Investigator – Records and Reports
Records should be accurate, complete, legible and timely pertinent to the data reported to the sponsor in the CRFs (Case Report Forms) and other required reportsAll corrections to a CRF should be dated, explained and should not obscure the original entry whether the entry is written or electronic changes or corrections. The investigator should retain records of the changes and corrections.
GOOD CLINICAL PRACTICE
Investigator’s Brochure
For investigational (not FDA-approved) drug trialsSummary of significant physical, chemical, pharmaceutical, pharmacological, toxicological, pharmacokinetic, metabolic, and clinical information that is relevant to the investigational productRelevant animal and clinical studies, adverse events, etc.
GOOD CLINICAL PRACTICE
FDA Form 1572 – to initiate clinical trials
Investigator agrees to comply with conditions required by FDA for use of investigational articles“Contract” that the investigator signs/dates“Warning: A willing false statement is a criminal offense”
Content of Form 1572
Principal Investigator name/addressName/address of site(s) of study conductName/address clinical labs (local/central)Name/address IRBNames of key personnel with study participant contactSubmit CVs of key personnel (signed/dated) listed in form
GOOD CLINICAL PRACTICE
Progress Reports
The investigator should submit written summaries (where required by applicable regulatory requirements) of the trial’s status to the institution.The investigator should submit written summaries of the status of the trial to the IRB annually or more frequently, if requested by the IRBThe investigator should promptly provide written reports to the sponsor and the IRB and where required by the regulatory authorities, the institution on any changes significantly affecting the trial and/or increasing the risk to subjects.
GOOD CLINICAL PRACTICE
Safety Reporting
All serious adverse events (SAE) should be reported immediately to the sponsor except for those SAEs that the protocol or other document identifies as not needing immediate reportingThe immediate and follow up reports should identify Subjects by unique code numbers assigned to trial, but not with identifiers (name, address, identification numbers)The immediate reports should be followed promptly by detailed, written reportsAdverse events and/or laboratory abnormalities identified in the protocol as critical to safety evaluations should be reported to the sponsor within the time periods specified by the sponsor in the protocolFor reported deaths, the investigator should supply the sponsor and the IRB with any additional requested information (e.g., autopsy reports and terminal medical reports)
GOOD CLINICAL PRACTICE
Premature Termination or Suspension of a Trial
If the trial is suspended or prematurely terminated for any reason the investigator should promptly Inform the trial subjects, should assure appropriate therapy and follow-up and where required, should inform the regulatory authorities and the IRBIf the investigator terminates or suspends a trial without prior agreement of the sponsor, the investigator should inform the institution, regulatory authorities(if required), the sponsor and the IRB with detailed written explanation of the termination or suspensionIf the sponsor terminates/suspends a trial, the investigator should promptly inform the institution (per applicable regulatory requirements) and the IRB and provide written explanation of the termination/suspensionIf the IRB terminates/suspends its approval, the investigator should inform the institution and the investigator should promptly notify the sponsor and provide the sponsor with a detailed written explanation of the termination or suspension
GOOD CLINICAL PRACTICE
Final Report
Upon the completion of the trial, the investigator should inform and provide the IRB and the sponsor:
All required reports
Summary of the trial’s outcome
Reports to regulatory authorities if applicable
GOOD CLINICAL PRACTICE
Records Retention Requirements
Essential documents should be retained until at least two (2) years after the last approval of a marketing application in an ICH region.These documents should be retained, however, if required by the applicable regulatory requirements (state or federal) or by an agreement with the sponsor.It is the responsibility of the sponsor to inform the investigator as to when these documents no longer need to be retained.Upon request of the monitor, auditor, IRB or regulatory authority, the investigator/institution should make available for direct access all requested trial-related records.
References
www.fda.gov
www.google.com
EMEA, Inspections
Stanford school of medicine; FACILITATING TRANSLATIONAL RESEARCH AND MEDICINE
CLINICAL RESEARCH