INDEX
Transcription
INDEX
INDEX MA TE RI AL Adverse effect, 211 Adverse event coding systems, 66–68 Adverse event reporting, 29–30, 42 challenges to, 62–66, 69 in data management, 58 United States versus European Union, 69 Adverse events (AEs), 211 becoming aware of, 62 challenges to reporting, 65–66 data accuracy/completeness associated with, 47 in final study clinical report, 68 good clinical practices and, 202 ISO 14155-1 standard and, 149, 155 ISO 14155-2 standard and, 157 in PMA P970029, 167–168, 169, 170 reporting times of, 64–65 resolution of, 63 Adverse events analysis, 64 Agreements, with ISO 14155-1 standard, 154 Allocation of treatments, principles of, 75 Alternative therapies, critical literature review and, 10 Alternative therapy risks, in clinical trial design, 3 Amputation, in LACI study, 82 Analysis datasets, for statistical analysis plan, 12 CO PY RI GH TE D Abbreviated IDE (A-IDE) devices, investigational product applications and, 116 Abbreviations, xi–xii Abciximab, noninferiority margin for, 32–33 Absolute risk difference, 211 Absolute values, in outcome tables, 29 ACAS® (Asymptomatic Carotid Atherosclerosis Study), PMA P040012 and, 176 Accountability, in medical device versus drug trial designs, 125 ACCULINKTM Carotid Stent System, 86, 174 in PMA P040012 study, 175, 176, 177, 181, 186 ACCUNETTM Embolic Protection System, 163, 175, 176 Accuracy, of data, 47–49 ACE inhibitors, in OPTIMAAL trials, 30, 31 Active control groups historic controls versus, 71 in medical device clinical trials, 73 Adjusted analyses, in statistical analysis plan, 18 Adjustments, in statistical analysis plan, 16–17 Administration, in medical device versus drug trial designs, 125 The Design and Management of Medical Device Clinical Trials: Strategies and Challenges, by Salah Abdel-aleem Copyright © 2010 John Wiley & Sons, Inc. 221 222 INDEX Analysis lesion, in PMA P070015, 187 Analyzed data in clinical trial management, 47 in study management, 49–55 Anatomic conditions, in ARCHeR studies, 183 Angina, in PMA P970029, 163, 164, 165, 169, 172 Angiographic binary restenosis (ABR), in PMA P070015, 186, 191 Angiographic data, missing from SPIRIT trial, 193 Angiographic late loss, in PMA P070015, 186–188 Angiographic results from PMA P070015, 192 from SPIRIT III 4.0-mm arm, 195, 196, 197 Angioplasty. See BARI (Bypass Angioplasty Revascularization Investigation) trial; Percutaneous transluminal angioplasty (PTA) Angiotensin II Antagonist. See OPTIMAAL (OPtimal Trial in Myocardial Infarction with the Angiotensin II Antagonist Losartan) trials Annexes, with ISO 14155-1 standard, 155 Annual reporting requirements, in medical device and drug product approval, 118 Anonymity, institutional review boards and, 209 Anticipated adverse events, reporting, 63 Anticoagulants, and protocol/ restricting procedural steps, 45–46 Application integrity policy (AIP), in study management, 48 Approval process, FDA, 128 A priori biological rationale, in subgroup analysis, 52, 53, 54 ARCHeR Registry study, 80 ARCHeR trials, 176–186 overview of, 174, 175 Arrhythmia, 24 Aspirin, myocardial infarction and, 52 Assay sensitivity, in superiority/ equivalence/noninferiority trials, 32 Associate investigator (AI), in informed consent documents, 38 Atorvastatin. See CARDS (Collaborative Atorvastatin Diabetes Study) Audits developing clinical SOPs and, 3 in drug/device product development, 130–131 Authorized representatives, 211 in CE marking, 147 Background, critical literature review and, 10 BARI (Bypass Angioplasty Revascularization Investigation) trial, 51, 53, 54, 55 Baseline characteristics of LACI study patients, 84 of SPIRIT III 4.0-mm arm, 194, 195 Baseline data, in CardioWest TAH-t study, 95 Baseline lesion and vessel characteristics in ARCHeR studies, 182–183 in PMA P070015, 190 of SPIRIT III 4.0-mm arm, 194, 195 Baseline patient demographics in ARCHeR studies, 182–183 in PMA P070015, 190 of SPIRIT III 4.0-mm arm, 194 INDEX Baseline patient group characteristics in HeartMate II LVAS study, 90 in PMA P970029, 170 with historic controls, 96 Belmont Report: Respect for Persons, 35, 42 bioethics in, 199, 200 ethical guidelines and principles in, 204–205 institutional review boards and, 208 Benchmarks, for objective performance criteria, 78 Benefits, of global clinical trials, 139. See also Risk/benefit analysis Best-case historic control, LACI study and, 82 Bias control groups and, 73 and masking/blinding in clinical protocols, 13–14 minimization of, 69–70 in missing data analysis, 60 BIMO inspections, in drug/device product development, 131–132 Binary measures, in statistical analysis plan, 15 Bioethics. See also Ethics challenges in, 200–201 in clinical research, 199–210 Biological products, where to report misconduct related to, 105 Bioresearch monitoring information system (BMIS), 104 Bioresearch monitoring (BIMO) program inspection data audits in, 48 in drug/device product development, 130–132 Biostatistics, in clinical trials, 44 Biotechnology companies, in study management, 44 Blame shifting, in detecting misconduct, 102 223 Blinding in clinical protocols, 12–14 in medical device versus drug trial designs, 122 Body surface area (BSA), in HeartMate II clinical study, 88 Bridge to transplantation (BTT) CardioWest TAH-t as, 93, 95 HeartMate II LVAS as, 88, 92 Budgeting, of investigator-initiated clinical trials, 133–134. See also Costs; Financial disclosure entries; Funds; Payment Budgets, for clinical studies, 8 Bypass, in LACI study, 82 CABG interventions, PMA P970029 and, 165, 166 Canadian Cardiovascular Society classification, PMA P970029 and, 165, 169 Candidate control therapies, in LACI study, 81 Captopril, losartan versus, 30–31, 31–32 Cardiac Arrhythmia Suppression Trial (CAST), 24 Cardiac risk factors, in PMA P970029, 170 Cardiogenic shock, 4 Cardiogenic shock trials, deleting inclusion/exclusion criteria in, 45 Cardiovascular histories, in HeartMate II LVAS study, 90 CardioWest total artificial heart, 87 clinical studies of, 93–96 CARDS (Collaborative Atorvastatin Diabetes Study), early termination in, 61–62 CARET (beta carotene and alpha tocopherol) study, early termination in, 61 Carotid endarthroscopy (CEA), PMA P040012 and, 176 224 INDEX Case report forms (CRFs) data accuracy/completeness associated with, 47 for foreign clinical sites, 144–145 in study documentation, 49 study statistician and, 20 terms and conditions for, 8–9 Categories, defining, 28 Cause–effect relationships, for adverse events, 63 Cause of death, in ARCHeR studies, 180 Cell measures/counts, in outcome tables, 29 CE logo, 211 CE (Conformité Européene) marking, 146–148, 211 European harmonization and, 147–148 FDA clinical trials versus, 157–160 ISO 14155-1 standard and, 149, 151 process of, 146–147, 148, 158 CE mark standards, xiv, 146–148 in European Union medical device regulation, 137–138 CE mark studies challenges of, 137–161 FDA studies versus, 15 purposes of, 160 Center for Biologics Evaluation and Research (CBER), drug/device combination products and, 126, 127, 128 Center for Devices and Radiological Health (CDRH) ARCHeR studies and, 181–186 drug/device combination products and, 126, 127, 128 in medical device regulation, 112 PMA P970029 and, 173 Center for Drug Evaluation and Research (CDER), drug/device combination products and, 126, 128 Certificate of Confidentiality, institutional review boards and, 209 Challenges to adverse event reporting, 62–66, 69 to and within informed consent forms, 35–41 associated with data accuracy/ completeness, 47–49 bioethical, 200–201 of CE marking, 146, 148 to CE mark studies, 160–161 to clinical study design, 1–42 of clinical trial distribution, 145 to designing statistical analysis plan, 11–12 of global clinical studies, 137–161 to global harmonization task force, 142–143 to medical device regulation, 107–135 in medical device versus drug trial designs, 125–126 posed by drug/device combination products, 126–129 to reporting adverse events, 65–66 to research contracts, 7, 8 to study management, 43–70 this book and, xiv–xv to using historic controls, 71–72 Checks, in statistical analysis plan, 18 Chemical action, in drug versus medical device definitions, 113 Children, consenting by, 40 Circulatory System Devices Panel approval of HeartMate II LVAS by, 92, 96 PMA P970029 and, 173 on XIENCE V Everolimus Eluting Coronary Stent System, 197 Class I (general controls) medical devices, 114, 119, 137–138, 158 INDEX Class II (general/special controls) medical devices, 114, 119, 137–138, 158, 160 Class III (premarket approval) medical devices, 114, 119, 137–138, 158, 160 Classification, of medical devices, 114, 119, 137–138, 158. See also ICD-9 (International Classification of Disease Version 9) system Cleveland Clinic, PMA P970029 and, 165 Clinical data, in medical device and drug product approval, 118 Clinical data managers, study statistician and, 20 Clinical event adjudication committee (CEC), in bias minimization, 70 Clinical investigation plan (CIP) ISO 14155-1 standard and, 153–154 ISO 14155-2 standard and, 149, 156, 157 Clinical investigations in EU medical device regulations, 159 ISO 14155-1 standard and, 149, 151 Clinical investigators, in drug/device product development, 130–131 Clinical personnel. See Personnel Clinical protocol procedures, patient compliance with, 46 Clinical protocols. See also Protocols; Study protocol adverse event coding systems and, 66 design of, xiii enrolled subjects and, 7 in informed consent form, 36 investigational devices in, 7 masking/blinding in, 12–14 this book and, xiv–xvs 225 Clinical regulations, medical device versus drug, 113. See also Regulations Clinical research. See also Research and development bioethics in, 199–210 criteria for reproducible, 47 Clinical research associates (CRAs) in fraud prevention, 103 in study management, 44 Clinical research staff. See Personnel Clinical scientists, this book and, xiv–xv Clinical studies. See also Clinical trials of CardioWest total artificial heart, 93–96 challenges of global, 137–161 challenges to designing, 1–42 changing primary outcomes of, 20–22 contract signing for, 8 design and management of, xiii, xiv–xv early termination in, 61–62 of HeartMate II LVAS, 88–92 reducing sample sizes of, 25 sample size determination of, 24–25 this book and, xiii–xv Clinical study teams, in completing study protocols, 20 Clinical trial designs, commonly used, 75–77 Clinical trial distribution, of foreign clinical trials, 145 Clinical trial outcomes, in CardioWest TAH-t study, 95 Clinical trial records, access to, 57–58 Clinical trials. See also Clinical studies; Superiority trials adverse event reporting in, 29–30, 42, 58, 62–66 analysis, design, and management of, xiii, xiv–xv 226 INDEX Clinical trials (cont’d) bias minimization in, 69–70 bioethics in, 199–210 cost-effectiveness of, 43 enrolled subjects in, 7 examples using historic controls, 80 FDA versus CE marking, 157–160 fraud and misconduct in, 99–105 global, 137–161 historic controls for, 71–97 human rights and, 35–41 industry-initiated, 132, 133 investigator-initiated, 132–135 management of, 43–70 of medical devices, 107 medical device versus drug regulation in, 112–113 meta-analysis studies and, 56–57 multinational, 66 randomization in, 74–75, 75–77 reporting results of, 28–30 risk/benefit analysis in, 3, 41–42 subgroup analysis in, 33–35 WHO GCP principles and, 203 XIENCE VTM Everolimus Eluting Coronary Stent System, 186–197 Clopidogren, noninferiority margin for, 33 Cluster randomization trial design, 75 Code of Federal Regulations (CFR) bioethics and, 205 clinical trial conduct and, 35–36 institutional review boards and, 206 ISO 14155-1 standard and, 152–153 medical device and drug regulation under, 115, 119 on non-significant risk devices, 111–112 objective performance criteria and, 79 “short form” signatures and, 41 Coding systems, for adverse events, 66–68 Cohorts in CardioWest TAH-t study, 93 in HeartMate II LVAS study, 88–89, 90, 91 Co-investigators (CO-PIs), clinical trials initiated by, 132–135 Columns, in outcome tables, 29 Combination products, drug/device, 126–129 Combined endpoints, 22–23 Common Rule, bioethics and, 205 Communication, in drug/device combination product development, 127–128 Comparable groups, randomization and, 74 Comparable treatments, principles of, 75 Comparison population, for CardioWest TAH-t study, 94–95 Competent authority, in CE marking, 158, 161 Competitive studies, in investigator selection, 6 Complaints, handling misconduct, 103–104 Completeness, of data, 47–49 Compliance in data management, 59 implementations of, 46 with study protocols, 46 Compliance classifications, in drug/ device product development, 131 Composite endpoints, 22–23 Comprehension, of informed consent documents, 37 Confidence intervals (CIs), 211 in clinical research, 26–27, 27–28 in selecting noninferiority margin, 33 INDEX Confidence limits, 212 Confidentiality bioethics and, 200, 201 in data management, 58 510(K) medical devices and, 110 institutional review boards and, 209 WHO GCP principles and, 203 Confidentiality breaches, as protocol deviations, 68 Conflicts of interest, in global clinical trials, 140 Conformity assessment, 212 Conformity assessment model, in CE marking, 146–147, 158 Conformity assessment modules, 212 Confounders, in statistical analysis plan, 17 Consensus, for objective performance criteria, 78. See also Transatlantic Inner Societal Consensus (TASC) Consent. See Informed consent entries Continued access protocol (CAP), in HeartMate II clinical study, 88 Continuous data, 212 Continuous-scale measurement, in statistical analysis plan, 16 Contract sign-off, documentation at, 134–135 Contraindication, 212 Control groups, 212 for medical device clinical trials, 73 purpose of, 73 Control group selection, in LACI study, 81 Control therapies, in LACI study, 81 Cooperation, and masking/blinding in clinical protocols, 13 Core laboratory, in bias minimization, 70 Correspondence, in study documentation, 49 227 Cost-effectiveness, of clinical trials, 43 Cost-effectiveness analysis, 212 Cost reduction, in medical device and pharmaceutical industries, 2 Costs, of global clinical trials, 139. See also Budgeting; Budgets; Financial disclosure entries; Funds; Payment Counts, in statistical analysis plan, 15–16 Critical limb ischemia (CLI), LACI study and, 82–83 Critical trials, design differences in medical device/drug, 121–124 Crossover trial design, 75, 76 Cultural variations in European clinical trials, 139–140 in global clinical trials, 141–142 Culture, WHO GCP principles and, 203 Customs, in European clinical trials, 139–140 Data accuracy and completeness of, 47–49 Data examining across study sites, 60–62 Data for BIMO inspections, 132 Data in changing primary outcomes, 20–21 Data in clinical trial management, 47 Data integrity of, 48, 55–56 misconduct related to, 99 in statistical analysis plan, 16, 17 storage in US, 56 Data analysis, in study management, 49–55 Data audits, 48 228 INDEX Databases in data management, 58 foreign clinical sites and, 143 with historic controls, 96 using historic controls from, 72 Data collection, for CE mark studies, 161 Data dredging, guarding against, 33–34 Data entry, in data management, 58 Data evaluation, in bias minimization, 70 Data identifiers, of fraud, 101–102 Data imputation, in missing data analysis, 59, 60 Data integrity, in study management, 44 Data listings, for statistical analysis plan, 12 Data management in clinical trials, 44 fraud and misconduct in, 59 missing data analysis in, 59–60 quality assurance in, 58–59 Data management systems, responsibilities of, 56 Data managers, study statistician and, 20 Data Monitoring Safety Board, in changing primary outcomes, 21 Data Protection Act, ISO 14155-1 standard and, 152 Data quality, 55–56 Data safety and monitoring board (DSMB) in bias minimization, 70 in PMA P970029, 167 Data trawling, guarding against, 33–34 Deaths, in ARCHeR studies, 180 Declaration of conformity, 212 Declaration of Helsinki. See Helsinki Declaration Deficiencies, BIMO inspections and, 132 Demographics in ARCHeR studies, 182–183 in PMA P070015, 190 of SPIRIT III 4.0-mm arm, 194 De Novo reclassification, for 510(K) medical devices, 111 Description, of adverse events, 62 Deviations from protocol adverse event coding systems and, 66–67 examples of, 67–68 reporting, 68 Deviations reports, adverse event coding systems and, 67 Device accountability, in medical device versus drug trial designs, 125 Device-related adverse events, reporting, 29–30 Devices, in adverse event reporting, 69. See also Investigational device exemptions (IDEs); Investigational devices; Medical device industry; Unanticipated adverse device effects (UADEs, UDAEs) Device sponsor information, for 510(K) medical devices, 109 Device trials, study sites in, 60–62 Diabetes. See also CARDS (Collaborative Atorvastatin Diabetes Study) as inclusion/exclusion criterion, 45 BARI trial and, 51 Diary cards, fraud identified via, 102 Difference, in clinical research, 27 Differential subgroup effects, 34 in statistical analysis plan, 18 Digoxin, 55 Directive, 212 Directorate General Enterprise, in CE marking, 147 Disease risks, in clinical trial design, 3 Distribution risks, with foreign clinical trials, 145–146 INDEX Documentation for adverse events, 63–64 BIMO inspections and, 131–132 bioethics and, 201 in CE marking, 147 in changing primary outcomes, 21 at contract sign-off, 134–135 in data management, 59 good clinical practices and, 202 in informed consent process, 39–40 for ISO 14155-1 standard, 153 in study management, 49 Dose dependent, 212 Double-blind studies, 13, 212 in bias minimization, 70 Drug research and development, clinical trials in, 43 Drugs clinical trial regulations for, 112–113 combined with medical devices, 126–129 defined, 113 FDA regulation of, 115 global trials of, 138–142 investigational product applications for, 115 mechanisms of action of, 113, 114 medical device classification and, 114 pathways to product approval for, 115–121 trial design for, 121–124 where to report misconduct related to, 105 Duke Activity Status Index (DASI) questionnaire, PMA P970029 and, 166, 169–170 Early termination, in clinical studies, 61–62 Eclipse TMR 2000 Holmium Laser System, in PMA P970029, 229 164–165, 167. See also Transmyocardial laser revascularization (TMR) Effectiveness, 212 Effectiveness parameters, of CardioWest TAH-t study, 93 Effectiveness results, in PMA P970029, 171 Efficacy, in ARCHeR studies, 185 Efficiencies, in medical device and pharmaceutical industries, 2 Electronic database training, in data management, 58 EN 540 standards, ISO 14155-1 standard and, 152–153 Encainide, 24 Endpoints. See also Primary outcomes; Secondary outcomes; Study endpoints to be analyzed, 25 in CardioWest TAH-t study, 94, 95–96 challenges to selecting, 11–12, 14–15 changing during studies, 20–22 in clinical trial design, 2, 3, 4 combined, 22–23 composite, 22–23 in FDA PMA cases, 163 features and characteristics of, 14 hard and soft, 21–22 of LACI study, 80, 86 and masking/blinding in clinical protocols, 14 meta-analysis studies and, 56–57 objective performance criteria and, 80 of PMA P970029, 165–166 selecting good primary, 15 statistical analysis plan and, 15–17, 18–19 statistical terms to define measurements of, 25–28 surrogate, 23–24 230 INDEX Enrolled subjects. See also Subject entries bioethics and, 199–200 in clinical trial design, 2 consenting by vulnerable, 40–41 defined, 7 in HeartMate II LVAS study, 88–89, 89–90 in LACI study, 83–85 misconduct related to, 99 protocol deviations among, 67 re-consenting, 40 screening logs for, 4–5 statistical power and number of, 52 study protocol compliance by, 46 terms and conditions for, 8–9 EPISTENT trial, noninferiority margin for, 32 Equivalence. See Substantial equivalence Equivalence hypothesis, in LACI study, 84–85 Equivalence/noninferiority trial design, 75, 76–77 Equivalence trials, 30–33, 213. See also Substantial equivalence Essential requirements, 213 in CE marking, 146–147, 158 Ethical guidelines and principles, 204–205 World Health Organization, 202–203 Ethics. See also Bioethics; Regional ethical issues control groups and, 73 in European clinical trials, 139–140 in informed consent process, 39 with ISO 14155-1 standard, 154, 155 and masking/blinding in clinical protocols, 13, 14 Ethics committees (ECs) bioethics and, 200, 201 in global clinical trials, 140 WHO GCP principles and, 203 Europe FDA studies versus those in, 15 global clinical trials in, 139–140 European Commission, 213 in CE marking, 147 European Directives, CE marking in, 146 European Economic Area (EEA), 213 European Free Trade Area (EFTA), 213 European Standard (EN), in CE marking, 147 European Union (EU), 213 CE mark standard of, xiv, 146–148 medical device regulation in, 137– 138, 157–158 regional ethical issues in, 140–141 United States versus, 45–46, 69, 137–138, 144–145, 157–160 Evaluation teams, and masking/ blinding in clinical protocols, 12–14 Evidence, critical literature review and supporting/weighted, 10 Excimer laser atherectomy, in LACI study, 81 Exclusion, of patients from studies, 4 Exclusion criteria in CardioWest TAH-t study, 94 deleting, 45 meta-analysis studies and, 56–57 for PMA P970029, 165 Exemptions, from informed consent form, 41. See also Investigational device exemptions (IDEs) Exempt reviews, by institutional review boards, 206–207 Exercise treadmill testing, in PMA P970029, 170–172 Expedited reviews, by institutional review boards, 207 Experience, in investigator selection, 5–6 INDEX Exploratory analyses, in statistical analysis plan, 18 Fabrication, fraud, and misconduct via, 100–101 False Claims Act, 102–103 False payment claims, 102–103 Falsification, fraud, and misconduct via, 100–101 FDA PMA cases, xiv, 163–197. See also Food and Drug Administration (FDA); Premarket approval (PMA) European Union and, 138 HeartMate II LVAS study, 92 using historic controls and, 72–73 FDA TMR studies, this book and, xiv. See also Transmyocardial laser revascularization (TMR) Feasibility studies, for medical devices, 121 Federal-wide Assurance (FWA), institutional review boards and, 206 Final study clinical report, adverse events reported in, 68 Financial disclosure, good clinical practices and, 202. See also Budgeting; Budgets; Costs; Funds; Payment Financial disclosure requirements, for 510(K) medical devices, 110 510(K) medical devices, 107 determination of, 108–111 European Union and, 138 premarket approval for, 112, 118–120 Flecainide, 24 Follow-ups in adverse event reporting, 68 in ARCHeR studies, 181 in handling misconduct claims, 103, 104 historic controls and, 71–72 231 Food and Drug Administration (FDA), 213 on accessing clinical trial records, 57–58 adverse event coding systems used by, 66 in adverse event reporting, 69 application integrity policy and, 48 approval of HeartMate II LVAS by, 92, 96 BIMO program of, 130–132 CE marking versus, 15, 157–160 clinical trial conduct and, 35–36 in clinical trial design, 2–3 contract sign-off and, 135 data audits by, 48 in detecting, correcting, and preventing fraud and misconduct, 100 developing clinical SOPs and, 3 drug/device combination products and, 126–129 European Union and, 138 historic controls and, 71–73, 97 ICF exemptions and, 41 investigational devices approved by, 7 investigational product applications and, 115–118, 119 ISO 14155-1 standard and, 150–151 in LACI study, 81, 86 LVADs and TAHs and, 97 medical device and drug regulation by, 115 medical device development and, 115 medical device regulation by, 107–108, 109–111 in medical device versus drug trial designs, 123–124, 125, 126 meetings with study sponsors, 129–130 232 INDEX Food and Drug Administration (FDA) (cont’d) on non-significant risk devices, 111–112 PMA P040012 and, 176, 181–186 PMA P970029 and, 166 practice of medicine and, 121 premarket approval by, 112 recommendation on acceptance of foreign clinical sites, 143 reporting adverse events and, 66 reporting misconduct to, 104–105 in selecting noninferiority margin, 33 sponsor reporting to, 123–124 statistical analysis plan and, 19 this book and, xiv timing of adverse events and, 65 on XIENCE V Everolimus Eluting Coronary Stent System, 197 Foreign study sites conducting global clinical trials in, 143–145 FDA recommendations on acceptance, 143 Fraud in clinical trials, 99–105 consequences of, 101 data identifiers of, 101–102 in data management, 59 defined, 100–101 detecting, correcting, and preventing, 100, 103 entities committing, 101 frequency of, 100 reasons for, 101 this book and, xiv warning signs of, 101–102 Full reviews, by institutional review boards, 207–208 Funds, for medical device development, 115. See also Budgeting; Budgets; Costs; Financial disclosure entries; Payment Global clinical studies, challenges of, 137–161. See also Global clinical trials Global clinical trials. See also Global clinical studies operational tips on conducting, 143–145 this book and, xiv Global harmonization task force (GHTF), global clinical trials and, 142–143, 148 Global trial considerations, 138–142 Good clinical practice (GCP) standards, 213 bioethics of, 199, 201–203 for CE mark studies, 160 in data management, 59 in detecting, correcting, and preventing fraud and misconduct, 100, 103 developing clinical SOPs and, 3 in drug/device product development, 131 guidance principles of, 200–201 World Health Organization and, 202–203 Good laboratory practice (GLP), in drug/device product development, 130 Good manufacturing practice (GMP), bioethics and, 201 Good surrogate endpoints, 24 Groupings, in statistical analysis plan, 16 Hard endpoints, 21–22 Harmonization, CE marking and, 147–148 Harmonized standards (EN), 213 Heart disease. See CARDS (Collaborative Atorvastatin Diabetes Study) INDEX Heart failure left ventricular assist devices and, 86–87 in PMA P970029, 163, 164 HeartMate II LVAS, 87 clinical studies of, 88–92 FDA approval of, 92 overall study patient outcomes, 91–92 primary study objective, 90 study design, 88–89 study overview, 88 study patient population, 89–90 Helsinki Declaration, 35, 42 bioethics in, 199, 200 ethical guidelines and principles in, 204 foreign clinical sites and, 143 Hemodynamic insufficiency, in CardioWest TAH-t study, 94 Heterogeneity, in subgroup analysis, 53 HIPAA (Health Insurance Portability Accountability Act), ISO 14155-1 standard and, 152 Historical data, pooling of, 78 Historic controls, 213 in CardioWest TAH-t study, 93 challenges to, 71–72 definition of, 77 examples of clinical studies with, 80 in FDA PMA cases, 163 in LACI study, 81–86 for PMA P040012, 175–186 recommendations for, 96–97 selection of, 71–97 this book and, xiv Holmium laser system, in PMA P970029, 164–165, 167 Human rights, clinical trial conduct and, 35–41. See also Bioethics; Ethics entries Hypotension, 4 233 Hypotheses, 213 in captopril versus losartan trial, 31 in clinical research, 26 in pivotal trial designs, 75–77 in subgroup analysis, 52, 54, 55 ICAI study historic controls in, 82 LACI study versus, 83 ICD-9 (International Classification of Disease Version 9) system, 66 IDE exemptions, investigational product applications and, 116, 117–118. See also Investigational device exemptions (IDEs) Identification, of adverse events, 62–63 ID numbers, in patient screening logs, 5 Ignorance, misconduct due to, 99 Impossible events, fraud identified via, 102 Inadvertent deviations, as protocol deviations, 67 Inclusion criteria in CardioWest TAH-t study, 93–94 deleting, 45 meta-analysis studies and, 56–57 in PMA P070015, 187 in PMA P970029, 165 Indemnification, in research contracts, 8, 9 Independent ethics committees (IECs) bioethics and, 201 WHO GCP principles and, 203 Independent study core laboratory, in bias minimization, 70 IND exemptions, investigational product applications and, 116– 117. See also Investigational new drugs (INDs) Industry-initiated clinical trials, 132, 133 contract sign-off for, 134–135 234 INDEX Inferences, in statistical analysis plan, 16–17 Information in adverse event reporting, 62–63 bioethics and, 200, 201 institutional review boards and, 209–210 in using historic controls, 72 WHO GCP principles and, 203 Informed consent bioethics and, 201 in global clinical trials, 140, 142–143 good clinical practices and, 202 ISO 14155-1 standard and, 153, 154 in medical device versus drug trial designs, 125 obtaining, 38 protocol deviations in, 68 Informed consent documents challenges of writing, 37 signatures on, 38 Informed consent form (ICF) basic elements of, 36 challenges to and within, 35–41 in clinical trial design, 3 developing clinical SOPs and, 3 as documentation, 39–40 ethics in, 39 with ISO 14155-1 standard, 154 misconduct related to, 99 requirement exceptions from, 41 waiver of, 36–37 Informed consent process clinical trial conduct and, 36 “short form,” 39 Inspections, in drug/device product development, 131–132 Institutional review board (IRB) accessing clinical trial records by, 57–58 bioethics and, 200, 201, 205 clinical studies budgets and, 8 consenting by vulnerable subjects and, 40 contract sign-off and, 135 foreign clinical sites and, 143 good clinical practices and, 202 in informed consent documents, 38, 39 on non-significant risk devices, 111–112 reporting adverse events and, 66 review processes of, 206–210 sponsors and FDA and, 123–124 structure of, 205–206 study subject re-consenting and, 40 timing of adverse events and, 65 WHO GCP principles and, 203 Institutions contract sign-off and, 135 in fraud prevention, 103 Insurance, in research contracts, 8, 9 Insurance protection, in global clinical trials, 140 Integrity, of data, 48, 55–56 Integrity hold, 48 Intention-to-treat (ITT) analysis, 214 advantages and limitations of, 50 requirements for, 51 in study management, 49, 50 Interaction effects, in subgroup analysis, 34 International Conference on Harmonization (ICH) bioethics and, 199 foreign clinical sites and, 143 International Organization for Standardization (ISO). See also ISO 14155 standard in CE marking, 147 European Union and, 138 International studies, with historic controls, 96 Intervention errors, as protocol deviations, 67 Investigational device exemptions (IDEs) in adverse event reporting, 69 decision process for, 116–118 INDEX foreign clinical sites and, 144 investigational product applications and, 115–118 for medical devices, 108 for non-significant risk devices, 111–112 sponsors and FDA and, 123–124 Investigational devices in adverse event reporting, 69 in clinical protocols, 7 Investigational device system, defined, 7 Investigational new drugs (INDs), 214. See also IND exemptions investigational product applications and, 115, 116 sponsors and FDA and, 123 Investigational product applications, in medical device and drug product approval, 115–118 Investigational product risks, in clinical trial design, 3 Investigational products, WHO GCP principles and, 203 Investigations ISO 14155-1 standard and, 149, 151 in medical device versus drug trial designs, 123 Investigative product, critical literature review and, 10 Investigator brochure anticipated adverse events in, 63 bioethics and, 201 with ISO 14155-1 standard, 153 Investigators. See also Principal investigator (PI) bioethics and, 200, 201 in changing primary outcomes, 21 in clinical trial design, 2 clinical trials initiated by, 132–135 contract sign-off and, 135 in drug/device product development, 130–131 good clinical practices for, 201–202 235 institutional review boards and, 209 and masking/blinding in clinical protocols, 12–14 nonmedical persons as, 6–7 selection for studies, 3, 5–7 Ischemic heart disease, 4 ISIS-2 study, multiple testing problem and, 52 ISO 14155 standard, 148–157. See also International Organization for Standardization (ISO) future of Part 1, 155 general requirements under, 151–152 new definitions under, 151 Part 1 of, 149–155 Part 2 of, 149, 156–157 purposes of, 148–149 IVUS results, from PMA P070015, 191, 192 Jurisdiction, for drug/device combination products, 127, 128 Kaplan–Meier survival estimates, 168, 169 Key budget items, in investigatorinitiated clinical trials, 133–134 Key inclusion criteria, in PMA P070015, 187 Key limitations of SPIRIT III 4.0-mm arm, 197 of SPIRIT III RCT, 193 Labeling of drug/device combination products, 127 in medical device and drug product approval, 121 Laboratory, in bias minimization, 70 LACI (laser angioplasty for critical limb ischemia) clinical study, 80–86 236 INDEX LACI Phase 2 Registry, results of, 83–84 Late lumen loss (LL), in PMA P070015, 186–187, 188 Left ventricular assist devices (LVADs), 80 in CardioWest TAH-t study, 95 described, 86–87 Left ventricular assist systems (LVASs), 87. See also HeartMate II LVAS Legally authorized representative (LAR), in informed consent documents, 38 Length of time, for medical device development, 115 Lesion types, in LACI study, 83–84 Literature review for clinical studies, 9–10 in clinical trial design, 3 in EU medical device regulations, 159 with ISO 14155-2 standard, 156 Logs, patient screening, 4–5 Losartan, versus captopril, 30–31. See also OPTIMAAL (OPtimal Trial in Myocardial Infarction with the Angiotensin II Antagonist Losartan) trials Major adverse cardiac events (MACE) in PMA P070015, 186, 188, 189–191 with SPIRIT III 4.0-mm arm, 194–196 Malicious intent, misconduct due to, 99 Management. See Data management; Study management Marketing, ISO 14155-1 standard and, 149 Marketing applications, in medical device and drug product approval, 118 Masking, 214 in clinical protocols, 12–14 in medical device versus drug trial designs, 122 Mathematical transformations, in statistical analysis plan, 16 Mean, 214 in clinical research, 26 Measurements, in statistical analysis plan, 16 Mechanisms of action, medical device versus drug, 113, 114 MEDDEV (medical device) guidelines, ISO 14155-1 standard and, 149, 150–151 MedDRA (Medical Dictionary for Regulatory Activities) system, 66 Median, in clinical research, 26 Medical care, bioethics and, 201 Medical device clinical trials, control groups for, 73 Medical device industry, challenges facing, 2 Medical devices classification of, 114, 119, 137–138, 158 clinical trial regulations for, 112–113 combined with drugs, 126–129 defined, 113 European Union regulation of, 137–138 FDA regulation of, 115 FDA standards for, 107–108, 109–111 global trials of, 138–142 investigational product applications for, 115–118 ISO 14155-2 standard for, 156–157 ISO 14155 standard for, 148–157 mechanisms of action of, 113, 114 pathways to product approval for, 115–121 in PMA P970029, 164–165 INDEX regulation of development of, 107–135 trial design for, 121–124 where to report misconduct related to, 105 Medical Devices Directive (MDD), 137, 159 Medical Management (MM) patients, in PMA P970029, 167–173 Medical practice, FDA and, 121 Medicare, clinical studies budgets and, 8 Medication errors, as protocol deviations, 67 Medications, in LACI study, 81 MEDWATCH (MedWatch) system, 65–66 Meta-analysis studies, 214 criteria for using, 56–57 critical literature review and, 10 Mild adverse events, 63 Misbranding, in medical device and drug product approval, 121 Misconceptions, in statistical analysis plan, 17 Misconduct in clinical trials, 99–105 in data management, 59 defined, 100–101 detecting, correcting, and preventing, 100 handling claims of, 103–104 reporting research, 104–105 this book and, xiv tips for detecting serious, 102 Missing data avoidance of, 60 in detecting misconduct, 102 handling, 60 in SPIRIT trial, 193 in statistical analysis plan, 16 Missing data analysis, 59–60 Moderate adverse events, 63 Monitoring, in bioethics, 200 237 Monitoring investigations, in medical device versus drug trial designs, 123 Monitors. See also Bioresearch monitoring information system (BMIS); Data Monitoring Safety Board in detecting misconduct, 102 with ISO 14155-1 standard, 154, 155 in medical device versus drug trial designs, 122–123 Morbidity, in PMA P970029, 172, 173 Moricizine, 24 Mortality, in PMA P970029, 172, 173 Multicenter studies, of CardioWest TAH-t, 93 Multicenter trials, budgets for, 8 Multinational clinical trials, reporting adverse events and, 66 Multiple databases, with historic controls, 96 Multiple subgroup testing, 35 Multiple testing problem, in subgroup analysis, 51–52, 53 Multivariate analysis, of data across study sites, 61 Mutual recognition agreement (MRA), 214 Myocardial infarction (MI), 22–23, 24. See also OPTIMAAL (OPtimal Trial in Myocardial Infarction with the Angiotensin II Antagonist Losartan) trials aspirin and, 52 in women, 54, 55 NASCET® (North American Symptomatic Carotid Endarterectomy Trial), PMA P040012 and, 176 National Commission for the Protection of Human Subjects of Biomedical and Behavioral Research, 205 238 INDEX National Formulary, in drug versus medical device definitions, 113 National Institutes of Health (NIH), BARI trial and, 51 National Research Act bioethics in, 199 ethical guidelines and principles in, 204 New drug application (NDA), 214 New York Heart Association (NYHA), in HeartMate II LVAS study, 89–90 No blind studies, 13 Noninferiority, defined, 30 Noninferiority margin (M), in noninferiority trials, 32–33 Noninferiority trial design, 75, 77, 214 Noninferiority trials defined, 30 selecting noninferiority margin for, 32–33 superiority trials versus, 30 Nonmedical persons, as investigators, 6–7 Nonrandomized concurrent control, in medical device clinical trials, 73 Nonrandomized design of CardioWest TAH-t study, 93 of LACI study, 86 Non-significant risk (NSR) devices, determination of, 111–112 Normal distribution, in statistical analysis plan, 17 Normalization, in statistical analysis plan, 16, 17 Notification of Intent to Market New Device, in medical device and drug product approval, 119 Notified body (NOBO), 214 in CE marking, 146–147, 158 Nuremberg Code, 35, 42 ethical guidelines and principles in, 204 Objective performance criteria (OPC), 78–80 advantages and disadvantages of, 79 described, 78, 80 determining, 79–80 FDA and, 78, 79 in FDA PMA cases, 163 historic controls and, 97 for PMA P040012, 175, 176 in using historic controls, 72 when to use and not to use, 78–79 Observational study, 214 Odds ratio (O.R.), in clinical research, 27 Office for Human Research Protections (OHRB), accessing clinical trial records by, 58 Office of Combination Products (OCP), drug/device combination products and, 127 “Off-label” devices, 121, 214 in adverse event reporting, 69 Open-label clinical trial, 214 OPTIMAAL (OPtimal Trial in Myocardial Infarction with the Angiotensin II Antagonist Losartan) trials, 30–31 Ordinal measurement scales, in statistical analysis plan, 16 OTW (over-the-wire) ACCULINKTM Carotid Stent System, 175, 181, 184 Outcome measure information, precision of, 29 Outcomes. See also Primary outcomes; Secondary outcomes; Study outcomes from CardioWest TAH-t study, 95 from LACI study, 84–85, 86 from PMA P070015, 191 from SPIRIT III 4.0-mm arm, 196 Outcome tables, in clinical research, 29 INDEX Outcome variables, in statistical analysis plan, 16 Outline, for statistical analysis plan, 11–12 Panel review, in medical device and drug product approval, 118 Parallel trial design, 75–76 Parameters, in statistical analysis plan, 18 Parametric tests, in statistical analysis plan, 17 Pathology endpoints, 21–22 Patient demographics, in HeartMate II LVAS study, 90 Patient enrollment, enhancing via study criteria relaxation, 45–46. See also Subject enrollment Patient outcomes, in HeartMate II LVAS study, 91–92 Patient population for CardioWest TAH-t study, 94–95 in clinical trial design, 2 with global clinical trials, 139 in HeartMate II LVAS study, 89–90 with historic controls, 96–97 for LACI study, 80 in missing data analysis, 60 in PMA P970029, 163 Patients. See also Enrolled subjects; Subject entries in ARCHeR studies, 182–183 bioethics and, 199–200 in CardioWest TAH-t study, 93–94 control groups and, 73 in HeartMate II clinical study, 88–89 historic controls and, 96 institutional review boards and, 206–210 in LACI study, 81, 83–84, 85–86 and masking/blinding in clinical protocols, 12–14 239 in PMA P070015, 190 in PMA P970029, 164–173 of SPIRIT III 4.0-mm arm, 194 selection for studies, 3–5 terms and conditions for enrolling, 8–9 Patient screening log, 4–5 Patient withdrawals, missing data resulting from, 60 Payment, terms and conditions for, 9. See also Budgeting; Budgets; Costs; Financial disclosure entries; Funds Peer-reviewed journals, critical literature review and, 10 Percentages, in outcome tables, 29 Percent change, in clinical research, 27 Percutaneous transluminal angioplasty (PTA), in LACI study, 82, 83 Performance data, for 510(K) medical devices, 110 Per-protocol (PP) analysis, 214–215 in study management, 49–50 Personnel BIMO inspections and, 131–132 bioethics and, 201 in clinical trial design, 3 in completing study protocols, 19–20 in detecting misconduct, 102 developing clinical SOPs and, 3 fraud by, 101 in fraud prevention, 103 good clinical practices and, 202 Pharmaceutical companies, in study management, 44 Pharmaceutical industry, challenges facing, 2 Pharmacokinetics, 215 Phase I–III trials, for drugs, 121 Pivotal trial designs commonly used, 75–77 in PMA P070015, 187–188 240 INDEX Pivotal trials, patient selection for, 4 Placebo, in noninferiority trials, 30 Placebo effect, 215 Placebo groups, in medical device clinical trials, 73, 74 Planned criteria, in LACI study, 83–84 Planned emergency research, ICF exemptions for, 41 Planned statistical analyses, in statistical analysis plan, 18 PMA P040012 ARCHeR trials in, 174, 175 historic controls for, 175–186 study design for, 175 PMA P070015 endpoints of, 186–188 SPIRIT trial designs for, 187, 188, 189, 193 statistical analysis for, 189–197 PMA P970029, 163 adverse events observed in, 167–168 angina improvement in, 169, 172 conclusions drawn from, 173 exercise treadmill testing in, 170–172 inclusion/exclusion criteria for, 165 medical devices in, 164–165 morbidity/mortality in, 172, 173 panel recommendation in, 173 patient enrollment and disposition in, 167 patient MM to TMR rollover during, 172–173 potential adverse events in, 169, 170 primary objective of, 165–166 purpose of, 164 quality of life and, 169–170 safety and effectiveness results of, 171 study design for, 164–165 study overview, 165 treatment failure in, 166, 172 Policies on handling misconduct claims, 103–104 US ethical, 205 Pooling, of historical data, 78 Post hoc analysis, skepticism of, 55 Practice of medicine, FDA and, 121 Precision, of outcome measure information, 29 Pre-clinical regulations, medical device versus drug, 113 Predicate “creep,” in medical device regulation, 112 Predicate device information, for 510(K) medical devices, 109, 111 Premarket approval (PMA). See also FDA PMA cases for 510(K) medical devices, 110, 118–120 in medical device and drug product approval, 118–120 in medical device regulation, 112 of medical devices, 114 Premarket notification submissions, for 510(K) medical devices, 108–111 Premarket phase, FDA–sponsor meetings during, 129–130 Previous research experience, in investigator selection, 5–6 Primary effectiveness endpoint, in LACI study, 80, 85–86 Primary endpoint results from SPIRIT III 4.0-mm arm, 195, 196 in PMA P070015, 191 of SPIRIT III 4.0-mm arm, 194, 196 Primary endpoints. See also Endpoints; Primary outcomes in CardioWest TAH-t study, 94, 95–96 in FDA PMA cases, 163 in PMA P070015, 186–188 Primary hypothesis, in clinical research, 26 INDEX Primary jurisdiction, for drug/device combination products, 127, 128 Primary mode of action (PMOA) standard, for drug/device combination products, 127, 128 Primary objectives of ARCHeR studies, 176–177 of CardioWest TAH-t study, 93 of HeartMate II clinical study, 88, 90 of HeartMate II LVAS study, 90 of PMA P970029, 165–166 Primary outcomes CE mark versus FDA, 15 changing during studies, 20–22 of clinical studies, 14 defined, 22 in statistical analysis plan, 17, 18–19 in subgroup analysis, 53 Primary safety endpoint, in LACI study, 80 Principal investigator (PI) in adverse event awareness, 62 bioethics and, 200, 201 and clinical trial fraud and misconduct, 100 clinical trials initiated by, 132–135 in detecting misconduct, 102 good clinical practices and, 202 in informed consent documents, 38 with ISO 14155-1 standard, 153– 154, 154–155 in medical device versus drug trial designs, 122, 124 reporting of protocol deviations by, 68 in research contracts, 7 study subject re-consenting and, 40 timing of adverse events and, 64–65 Principles, World Health Organization GCP, 202–203 241 Privacy bioethics and, 200 institutional review boards and, 209 Privacy of data, in data management, 58 Procedural success in PMA P070015, 189–191 with SPIRIT III 4.0-mm arm, 194–196 Procedure changes, as protocol deviations, 67 Procedure-related adverse events, reporting, 29 Procedures, in statistical analysis plan, 18 Product approval, pathways to, 115–121 Products, WHO GCP principles and, 203 Product types, medical device versus drug, 113 PRoFess trial, noninferiority margin for, 33 Prospective studies, of HeartMate II LVAS, 88–89 Protocol compliance, implementations of, 46 Protocol deviation reports, 67, 68 Protocol deviations/violations adverse event coding systems and, 66–67 data accuracy/completeness associated with, 47 examples of, 67–68 reporting, 68 Protocol procedural steps, deleting, 45–46 Protocols, 215. See also Clinical protocols; Study protocols in adverse event awareness, 62 for anticipated adverse events, 63 bioethics and, 201 with foreign clinical sites, 144 good clinical practices and, 202 in WHO GCP principles, 203 242 INDEX PTCA interventions, PMA P970029 and, 165, 166 Publication policy critical literature review and, 9–10 in research contracts, 8, 9 Pulmonary artery diastolic (PAD) pressure, in HeartMate II LVAS study, 90 Pulmonary capillary wedge pressure (PCWP), in HeartMate II LVAS study, 89–90 p–value (probability value), 215. See also Significance levels in clinical research, 26, 27–28 in statistical analysis plan, 19 in subgroup analysis, 34, 35, 55 Quality, of data, 55–56 Quality assurance in data management, 58–59 WHO GCP principles and, 203 Quality of life in HeartMate II LVAS study, 92 in PMA P970029, 169–170 Randomization advantages and disadvantages of, 74–75 in bias minimization, 70 with historic controls, 96 in LACI study, 81–82 in medical device clinical trials, 73 in medical device versus drug trial designs, 122 meta-analysis studies and, 56 in pivotal trial designs, 75–77 in PMA P970029 patient MM to TMR rollover, 172–173 in statistical analysis plan, 16–17 in subgroup analysis, 53 Randomized clinical trials (RCTs), historic controls and, 71–73. See also TAXUS RCT trial design Randomized control clinical trials, advantages and disadvantages of, 74–75 Randomized trial, 215 Raw data, in clinical trial management, 47 Readability, of informed consent documents, 37 Recommendations, for study management, 44 Re-consenting study subjects, 40 Record retention, in medical device versus drug trial designs, 124 Records access to, 57–58 fraud identified via, 102 good clinical practices and, 202 WHO GCP principles and, 203 Records inspection, in medical device versus drug trial designs, 125 Regional ethical issues, of global clinical trials, 140–141 Regression analysis, of data across study sites, 61 Regulation. See also Code of Federal Regulations (CFR); Regulations of drug/device combination products, 128 of EU medical devices, 137–138, 157–158, 158–159 of global clinical trials, 140–141 of investigator-initiated clinical trials, 132–133 of medical device development, 107–135 of medical practice, 121 Regulations. See also Regulation medical device classification related to, 114 medical device versus drug, 113 for medical devices, 108 in medical practice, 121 this book and, xiv INDEX US and EU, 144 US ethical, 205 Regulatory agencies accessing clinical trial records by, 57–58 in adverse event reporting, 69 Regulatory challenges, to using historic controls, 71–72 Regulatory clearance, under ISO 14155-1 standard, 151–152 Regulatory guidelines for CE mark studies, 160 compliance with, 2 Regulatory knowledge, misconduct related to, 99 Regulatory trends, in foreign clinical trials, 145–146 Reimbursement, subject, 7, 8, 9 Relaxation of study criteria, enhancing patient enrollment via, 45–46 Renin-Angiotensin system (RAS), 30 Report forms, terms and conditions for, 8–9 Reporting of adverse events, 65–66 of adverse event timing, 64–65 of protocol deviations/violations, 67, 68 of subgroup analyses, 54 Reports, good clinical practices and, 202 Representatives, in CE marking, 147 Reproducible clinical research, criteria for, 47 Requirements for CE mark devices, 161 in CE marking, 146–147 for CE mark studies, 160 in EU medical device regulations, 158–159 under ISO 14155-1 standard, 151–152 243 Research and development. See also Clinical research; Reproducible clinical research bioethics in, 199–210 clinical trials in, 43 global clinical trials and, 141–142 meta-analysis studies in, 56–57 study protocol compliance in, 46 Research contracts challenges to, 7, 8 in clinical trial design, 2 defined, 7–8 Researchers, this book and, xiii, xiv–xv Research experience, in investigator selection, 5–6 Research misconduct, reporting, 104–105 Resolution, of adverse events, 63 Respect, as WHO GCP principle, 203 Responsibilities in clinical trial design, 3 good clinical practices and investigator, 202 of institutional review boards, 205–206 Restricting procedural steps, deleting, 45–46 Revascularization, 22–23. See also BARI (Bypass Angioplasty Revascularization Investigation) trial Review, of severe and serious adverse events, 64 Review of literature, for clinical studies, 9–10 Risk, in drug versus medical device definitions, 113. See also Risks Risk/benefit analysis bioethics and, 200 in clinical trial design, 3, 41–42 WHO GCP principles and, 203 Risk mitigation, in clinical trial design, 3 244 INDEX Risks. See also Cardiac risk factors bioethics and, 200 in clinical trial design, 3 critical literature review and, 10 with foreign clinical trials, 145–146 institutional review boards and, 208–209 WHO GCP principles and, 203 Rows, in outcome tables, 29 RX (rapid exchange) ACCULINKTM Carotid Stent System, 86, 174 in PMA P040012 study, 175, 176, 177, 181, 184, 186 RX (rapid exchange) ACCUNETTM Embolic Protection System, 163, 175, 176 Safeguard clause, 215 Safety in ARCHeR studies, 183–184 bioethics and, 200 in HeartMate II clinical study, 88 in PMA P970029, 171 Safety determination, for CE mark studies, 161 Safety parameters, in CardioWest TAH-t study, 93 Sample size determination, of clinical studies, 24–25 Sample sizes with ISO 14155-2 standard, 157 reducing, 25 SAPPHIRE® trial, PMA P040012 and, 176 Scale, reporting, 28 Scientific challenges, to using historic controls, 71–72 Scientists, in global clinical trials, 141– 142. See also Clinical scientists Screening logs, for patients, 4–5 Secondary endpoints. See Secondary outcomes Secondary objectives in HeartMate II clinical study, 88 of PMA P970029, 165–166 Secondary outcomes changing during studies, 21 of clinical studies, 14 defined, 22 in statistical analysis plan, 17, 18–19 Sensitive information, institutional review boards and, 209–210 Sensitivity analysis, of missing data, 60 Sequential trial design, 75, 76 Serious adverse events. See also Severe adverse events (SAEs) in ARCHeR studies, 177–181 ISO 14155-1 standard and, 149–150 reporting, 29, 62–63 review of, 64 severe adverse events versus, 63 Seriousness, of adverse events, 62–63 Serious protocol deviations/ violations, adverse event coding systems and, 66–67 Severe adverse events (SAEs), 63. See also Serious adverse events good clinical practices and, 202 with ISO 14155-1 standard, 155 with ISO 14155-2 standard, 157 review of, 64 serious adverse events versus, 63 Severity, of adverse events, 63 “Short form,” signatures on, 41 “Short form” consent process, 39 Signatures fraud identified via, 102 on informed consent documents, 38, 41 Significance, in clinical research, 26, 28 Significance levels, in statistical analysis plan, 17, 19 Significant risk (SR) devices, classification as, 112 Significant treatment effects, detecting in subgroup analysis, 54, 55 INDEX Single blind studies, 13 Site data, fraud identified via, 102 Site differences, in bias minimization, 70 Site preparation, for BIMO inspections, 131–132 Sloppiness, misconduct due to, 99 Soft endpoints, 21–22 Source documents for adverse events, 63–64 in detecting misconduct, 102 in study management, 49 Source records, fraud identified via, 102 SPIRIT III 4.0-mm arm, 193–197 summary of, 197 SPIRIT III RCT trial, summary of, 193 SPIRIT trial designs, in PMA P070015, 187, 188, 189, 193 Sponsor information, for 510(K) medical devices, 109 Sponsors accessing clinical trial records by, 57–58 bioethics and, 200, 201 in CE marking, 147 in changing primary outcomes, 20, 21 clinical studies budgets and, 8 in clinical trial design, 2 and clinical trial fraud and misconduct, 99–100 in completing study protocols, 19 critical literature review and, 9–10 developing clinical SOPs and, 3 in drug/device product development, 130, 131–132 FDA meetings with, 129–130 in FDA PMA cases, 163 foreign clinical sites and, 143 in fraud prevention, 103 global clinical trials and, 138–142 historic controls and, 97 indemnification by, 9 245 insurance carried by, 9 of investigator-initiated clinical trials, 132–133 in investigator selection, 5–6 with ISO 14155-1 standard, 154, 155 of LACI study, 84, 85–86 medical device regulations and, 108 in medical device versus drug trial designs, 122, 123–124 study subject re-consenting and, 40 timing of adverse events and, 64, 65 using historic controls and, 72 Sponsor site preparation, for BIMO inspections, 131–132 SPORTIF trials, noninferiority margin for, 33 Staff. See Personnel Standard deviation (SD), 216 in clinical research, 26 Standard error (SE), 216 Standardization, bias minimization via, 69–70 Standard of care, with historic controls, 97 Standard operating procedures (SOPs) in clinical trial design, 2 development of clinical, 3 ISO 14155-1 standard and, 151 Standards for global clinical trials, 139 for medical devices, 107–108, 109–111 Standards of care, 215 Statement of similarity, in medical device and drug product approval, 119 Statistical adjustments, in statistical analysis plan, 16–17 Statistical analysis, in subgroup analysis, 54 246 INDEX Statistical analysis plan (SAP) challenges to designing, 11–12 in clinical trial design, 2–3 components of, 17–19 data quality in, 56 p–value in, 19 requirements of, 18–19 study endpoints and, 15–17 this book and, xiv Statistical inferences, in statistical analysis plan, 16–17 Statistical methods in clinical trials, 44 multiple testing problem and, 51–52, 53 power of, 52 in statistical analysis plan, 17 in subgroup analysis, 53, 54 Statistical power problem, in subgroup analysis, 52 Statistical significance, 216 Statistical terminology, to define endpoint measurements, 25–28 Statistical tests randomization and, 74 in statistical analysis plan, 16 in subgroup analysis, 34, 53, 54 Statisticians, in completing study protocols, 20 Statistics, with ISO 14155-2 standard, 157 Stent thrombosis, in PMA P070015, 192 Stent thrombosis levels of evidence, in PMA P070015, 187 Strategies for drug/device combination product development, 127–128 in statistical analysis plan, 17 Stratification, 216 Stratification factors, in statistical analysis plan, 16–17 Structured document template, for statistical analysis plan, 11 Students, this book and, xiii Study centers, in clinical trial design, 2 Study committees, in bias minimization, 70 Study completion, terms and conditions for, 8–9 Study core laboratory, in bias minimization, 70 Study data, managing, 58–59 Study design, of CardioWest TAH-t study, 93 Study endpoints, 215. See also Endpoints challenges to selecting, 11–12, 14–15 in clinical trial design, 2, 3, 4 describing, 21–22 features and characteristics of, 14 statistical analysis plan and, 15–17 Study management application integrity policy in, 48 challenges to, 43–70 data accuracy/completeness in, 47 data audits in, 48 integrity holds in, 48 issues in, 43–44 recommendations for, 44 Study outcomes historic controls and, 77 missing data analysis and, 59 Study power, in missing data analysis, 59 Study procedures, adverse events and, 63 Study products adverse events and, 63 challenges to designing, 11–12 Study protocols. See also Clinical protocols in CardioWest TAH-t study, 93–94 in clinical research, 26–28 compliance with, 46 responsibilities of clinical personnel in, 19–20 INDEX Study sites in adverse event awareness, 62 budgeting key items at, 133–134 CE mark, 160 conducting global clinical trials in, 143–145 contract sign-off at, 134–135 examining data across, 60–62 FDA recommendations on acceptance of foreign, 143 selection for studies, 3, 5–7 Study source documents, in study management, 49 Study statisticians, in completing study protocols, 20 Study subjects. See Enrolled subjects Study teams, in completing study protocols, 20 Subgroup analysis, 33–35, 216. See also Subgroup/subset analyses a priori definition of, 53, 54 challenging issues due to, 55 interpreting, 54–55 logistics of, 35 points to consider for, 53 problems with, 51–55 reporting, 54 in study management, 44, 51 Subgroups/subsets appropriately defined, 52 in statistical analysis plan, 18 Subgroup/subset analyses, in statistical analysis plan, 18 Subject enrollment. See also Enrolled subjects enhancing via study criteria relaxation, 45–46 in LACI study, 81 in medical device versus drug trial designs, 121 for PMA P970029, 167 protocol deviations in, 67 terms and conditions for, 8–9 247 Subject injury, in research contracts, 8, 9 Subject injury reimbursement plan, in research contracts, 7, 8, 9 Subjectivity in FDA PMA cases, 163 and masking/blinding in clinical protocols, 13–14 Subject reimbursement, in clinical studies, 8 Subject replacement, terms and conditions for, 8–9 Subject reporting, and masking/ blinding in clinical protocols, 13 Substantial equivalence for 510(K) medical devices, 108, 109, 110–111 in medical device and drug product approval, 119, 120 Substantive information requirements, for 510(K) medical devices, 109 Suggestive treatment effects, detecting in subgroup analysis, 54 Summary data for 510(K) medical devices, 110, 119–120 in subgroup analysis, 54 Superiority, defined, 30 Superiority trials, 30–33, 77 Supporting evidence, critical literature review and, 10 Surrogate endpoints, 23–25, 216 examples of, 23 in FDA PMA cases, 163 problems with, 24–25 Surveillance authorities, 215 SynCardia Systems, Inc., 96 System Organ Class (SOC) terminology, adverse event coding systems and, 66 TARGET4 trial, noninferiority margin for, 32–33 248 INDEX Target lesion revascularization (TLR), in PMA P070015, 186, 188 Target vessel failure (TVF), in PMA P070015, 186, 188, 189, 191 Target vessel revascularization (TVR), in PMA P070015, 186, 188 TASC types, in LACI study, 83. See also Transatlantic Inner Societal Consensus (TASC) TAXUS RCT trial design, PMA P070015 and, 188, 189, 190, 191, 192, 193, 194, 195, 196, 197. See also Randomized clinical trials (RCTs) Technical file (TF), 214 Technology in global clinical trials, 142 in medical device versus drug trial designs, 122 Terminology for adverse event coding systems, 66 to define endpoint measurements, 25–28 Term of study, for CardioWest TAH-t study, 94 Test groups, in medical device clinical trials, 73 Tests in clinical research, 26, 27 in statistical analysis plan, 16, 17 Therapeutic effects, detecting in subgroup analysis, 54 Thrombosis, in PMA P070015, 192 Time to clearance, in medical device and drug product approval, 118 Time to event, in statistical analysis plan, 16 Time to market in medical device and pharmaceutical industries, 2 medical device development and, 115 Time to transplant/death, in CardioWest TAH-t study, 95 Timing of adverse events, 64–65 of FDA–sponsor meetings, 129–130 Tirofiban, noninferiority margin for, 32–33 TMR 2000 Holmium Laser System, in PMA P970029, 164–165, 167. See also Transmyocardial laser revascularization (TMR) Total artificial heart (TAH) devices, 80, 87. See also CardioWest total artificial heart Toxicities, study subject re-consenting and, 40 Traditional clinical practices, in global clinical trials, 140 Training, in data management, 58 Transatlantic Inner Societal Consensus (TASC), on LACI study, 81, 82, 83 Transmyocardial laser revascularization (TMR), xiv in PMA P970029, 164, 165, 166, 167, 168, 169, 170, 171, 172, 173 Treadmill testing, in PMA P970029, 170–172 Treatment bioethics in, 200 in LACI study, 80 Treatment allocation, principles of, 75 Treatment decisions, and masking/ blinding in clinical protocols, 13–14 Treatment failure, in PMA P970029, 166, 172 Treatment options, in subgroup analysis, 52 Treatment procedures, in CardioWest TAH-t study, 94 Trial data, in changing primary outcomes, 20–21 INDEX Trial design commonly used types of, 75–77 historic controls and, 71–73 medical device versus drug, 121–124 in subgroup analysis, 52 Trial outcomes, in CardioWest TAH-t study, 95 Trial records, access to, 57–58 Trials. See Clinical trials Triple blind studies, 13 t-test, 216 Two-tailed t-test, 216 Type 2 diabetes. See CARDS (Collaborative Atorvastatin Diabetes Study) Unanticipated adverse device effects (UADEs, UDAEs), 63 in medical device versus drug trial designs, 124 ISO 14155-1 standard and, 150 timing of adverse events and, 64–65 Unfavorable anatomic conditions, in ARCHeR studies, 183 United States. See also Food and Drug Administration (FDA); National entries; US entries ACCULINKTM trials in, 175 CE mark studies versus those in, 15 clinical data storage in, 56 ethical regulations and policies of, 205 European Union versus, 45–46, 69, 137–138, 144–145, 157–160 foreign clinical sites and, 144–145 pivotal PMA P070015 trial designs in, 187–188 submitting false/fraudulent payment claims to, 102–103 Units in outcome measure information, 29 US versus EU, 144–145 249 UNOS IA/IB studies, of HeartMate II LVAS, 88–89, 90 Unrelated adverse events, reporting, 29–30 US Department of Health and Human Service, on foreign clinical sites, 143. See also United States US Homeopathic Pharmacopoeia, in drug versus medical device definitions, 113 US Pharmacopoeia, in drug versus medical device definitions, 113 Validation in data management, 58 of historic controls, 79 with historic controls, 96 Valid statistical tests, randomization and, 74 Variance, in clinical research, 26 Variation of data, across study sites, 60–62 Ventricular arrhythmia, 24 Ventricular assist devices (VADs), 87 Violations, in CE marking, 148 Violations of protocol, adverse event coding systems and, 66–67 Violations reports, adverse event coding systems and, 67 Volume information, in medical device and drug product approval, 118 Vulnerable subjects, consenting by, 40–41 Waivers, of informed consent form, 36–37 Websites on medical device versus drug trial designs, 126 for reporting misconduct, 104–105 Weighted evidence, critical literature review and, 10 250 INDEX Weighted historic control (WHC), PMA P040012 and, 176 Whistleblowers in detecting misconduct, 102 false payment claims exposed by, 103 Witnesses, in informed consent process, 39 Women, myocardial infarction in, 54, 55 World Health Organization (WHO), good clinical practices and, 202–203 XIENCE VTM Everolimus Eluting Coronary Stent System, clinical trial of, 186–197 YAG laser, in PMA P970029, 164–165