Table 1

Summary of included studies

Authors (country)RCT designSettingIntervention(s)ComparatorParticipantsRecruited to intervention(s)Recruited to comparatorRisk of bias*Comments†
Avenell et al (UK)16Parallel groupSecondary careOpen trial design comparing vitamin D, with calcium, with vitamin D and calcium, with no tabletsConventional trial comparing vitamin D, with calcium, with vitamin D and calcium, with placeboPatients aged ≥70 attending a fracture clinic or orthopaedic ward134/180 (74.4%)233/358 (65.1%)ABetween-group difference was statistically significant (OR 1.56; 95% CI 1.05 to 2.33)
Bentley and Thacker (USA)17FactorialUniversity (multicentre, n=5)A: Info on a high-risk trial for a drug not yet tested on humans, pays $1800Not applicablePharmacy studentsUnclearNot applicableCAssessed willingness to take part in hypothetical studies by risk and reward; did not differentiate recruitment rates between groups (270 participants); between-group differences were statistically significant for both risk level (p<0.0005) and level of payment (p=0.015)
B: Info on a high-risk trial for a drug not yet tested on humans, pays $800Unclear
C: Info on a high-risk trial for a drug not yet tested on humans, pays $350Unclear
D: Info on a medium-risk study for a generic drug already on the market, pays $1800Unclear
E: Info on a medium-risk study for a generic drug already on the market, pays $800Unclear
F: Info on a medium-risk study for a generic drug already on the market, pays $350Unclear
G: Info on a low-risk study measuring the salivary levels of stress hormones, pays $1800Unclear
H: Info on a low-risk study measuring the salivary levels of stress hormones, pays $800Unclear
I: Info on a low-risk study measuring the salivary levels of stress hormones, pays $350Unclear
Cooper et al (UK)18Parallel groupSecondary carePartially randomised patient preference design allocating to medical management or transcervical resection of the endometrium or preferred optionConventional RCT design allocating to medical management or transcervical resection of the endometriumFirst time attendees at a gynaecological clinic90/135 (96.3%)97/138 (70.3%)ANo information on statistical significance given
Coyne et al (USA)19ClusterSecondary care (multicentre, n=44)Easy-to-read consent statements (altered text style, layout, font size, vocabulary; reading level 7th–8th grade)Standard consent statementsPatients eligible for participation in a cancer treatment trial75/89 (84.3%)68/137 (49.6%)CInvolved consent statements for three cancer treatment trials (one lung, two breast cancer); actual accrual to the parent studies was not significantly different (p=0.32)
DiGuiseppi et al (USA)20Parallel groupHealth Maintenance Organisation (HMO) (multicentre)Telephone administered questionnaire on hazardous drinking and willingness to participate in lifestyle interventionFace-to-face administered questionnaire on hazardous drinking and willingness to participate in lifestyle interventionPatients aged ≥18 attending the HMO with an acute injury64/99 (64.6%)190/370 (51.4%)CConsidered different methods of screening, which included willingness to participate in a hypothetical trial; the telephone group was somewhat more often associated with willingness to participate (OR 1.49; 95% CI 0.97 to 2.30)
Du et al (USA)21Parallel groupSecondary care18 min educational video giving an overview of clinical trials and the importance of cancer clinical research to societyStandard care (ie, normal first visit to the oncologist)Patients aged 21–80 attending a multidisciplinary lung clinic at a cancer centre11/63 (17.5%) to therapeutic trials; 16/63 (25.4%) to all trials7/63 (11.1%) to therapeutic trials; 10/63 (15.9%) to all trialsBConsidered recruitment to a range of cancer trials categorised into ‘therapeutic’, and ‘therapeutic and non-therapeutic’; between-group difference was not statistically significant for therapeutic trials (p=0.308) or for all trials (p=0.187)
Du et al (USA)22Parallel groupSecondary care18 min educational video giving an overview of clinical trials and the importance of cancer clinical research to societyStandard care (ie, normal visit to the oncologist)Women aged 21–80 attending a breast cancer clinic at a cancer centre10/98 (10.4%)6/98 (6.1%)CBetween-group difference was not statistically significant (p=0.277)
Ellis et al (Australia)23Parallel groupSecondary careInformation booklet explaining trials, how treatment is selected in an RCT, discussion of treatment options, advantages and disadvantages of participation, where to get more info plus usual discussion about treatment options from the clinician, inc. RCTs if appropriate (no standardisation of what is discussed)Usual discussion about treatment options from the clinician, inc RCTs if appropriate (no standardisation of what is discussed)Women undergoing definitive surgery for early stage breast cancer at a cancer institute12/30 (40.0%) at follow-up14/30 (46.7%) at follow-upCStudied willingness to participate in a hypothetical trial; between-group difference was statistically significant (p=0.05)
Ford et al (USA)24Parallel groupCommunity (multicentre, n=2)A: Enhanced recruitment letter, phone screening by an African American interviewer, baseline questionnaire by mail, reminder calls/mailings for baseline info and consentStandard recruitment letter, phone screening by an African American/Caucasian interviewer, baseline questionnaire by mail, reminder calls/mailings for return of baseline info and consentAfrican American men aged 55–74, eligible for a prostate, lung and colorectal cancer screening trial78/3079 (2.5%)95/3297 (2.9%)BBetween-group difference was statistically significant (p<0.01)
B: Enhanced recruitment letter, phone screening by an African American interviewer, baseline questionnaire by phone, reminder calls/mailings for consent form87/3075 (2.8%)
C: Enhanced recruitment letter, phone screening by an African American interviewer, reminder for project session held at church, baseline questionnaire at church session116/2949 (3.9%)
Fowell et al (UK)25Clustered cross-overSecondary care (multicentre, n=2)Cluster randomisationZelen's design (only those randomised to intervention arm asked for consent)Cancer inpatients receiving palliative care and starting on a syringe driver6/24 (25%)0/29 (0%)CConsidered the effect of trial design on potential recruitment rate; aimed to explore the feasibility of the two designs for studies of dying patients; between-group difference was statistically significant (p=0.02)
Free et al (UK)26Parallel groupCommunity (multicentre, n=2)A: A letter containing study and consent information, and a £5 noteNormal trial procedures (letter and patient information sheet)Members of the public who are aged ≥16, are daily smokers and willing to quit in the next month13/246 (5.3%)1/245 (0.4%)AEvaluated interventions in separate trials; between-groups differences were statistically significant for both the financial incentive (OR 4.9; 95% CI 2.0 to 7.7) and text messages (OR 4.2; 95% CI 2.2 to 6.1)
B: Four text messages over 1 week containing quotes from existing participantsNormal trial procedures (letter and patient information sheet)17/405 (4.2%)0/406 (0%)
Freer et al (UK)27Parallel groupTertiary neonatal intensive care unitA: Five page US version of a study information leaflet (inc. more detail on study process, risks, benefits and patient rights) plus standard verbal explanationUS version of an information leaflet without verbal explanationParents of immature infant(s) admitted to the NICU but not requiring intensive care5/9 (56%)3/9 (33%)BConsidered the impact of information on parents’ understanding of a research study and the validity of their consent to participation in a hypothetical trial; no information on statistical significance given
B: Less detailed single sheet UK version of a study information leaflet plus standard verbal explanationUK version of an information leaflet without verbal explanation5/9 (56%)4/10 (40%)
Fureman et al (USA)28Parallel groupExisting trial (university based)Enhanced video on an HIV vaccine trial plus a 1 h pamphlet presentation (5 min pre-test, 26 min of video, 10 min to review pamphlet, RA initiated Q&A session, post-test questionnaire, survey at 1 monthStandard half hour pamphlet-only presentation (5 min pre-test, 10 min to review a trial info pamphlet, RA initiated Q&A session, post-test questionnaire, survey at 1 monthParticipants in the Risk Assessment Project (injection drug users)1.84 (post-test 1); 1.69 (post-test 2)1.70 (post-test 1); 1.50 (post-test 2)CStudied recruitment to a hypothetical trial (targeted 98 individuals for intervention, 88 for comparator); results provided as mean willingness scores; between-group difference was not statistically significant (p>0.1)
Graham et al (USA)29Parallel groupHealth Maintenance Organisation (multicentre)A: Electronic questionnaire on hazardous drinking and willingness to participate in lifestyle interventionStandard self-complete paper questionnairePatients aged ≥18 attending the HMO with an acute injury69/151 (45.7%)76/141 (53.9%)CConsidered different methods of screening, which included willingness to participate in a hypothetical trial; between-group difference was statistically significant (p=0.001)
B: Oral questionnaire read aloud to patients in the clinic, potential answers printed on cards and patients asked to point42/78 (53.8%)
Halpern et al (USA)30Within-subject designSecondary careA: Variation in trial information on (1) the percentage of previous patients experiencing an adverse effect from the study drug (10%, 20%, 30%) and (2) payment participants would receive ($100, $1000, $2000)Not applicablePatients with mild to moderate hypertension attending an outpatient clinicUnclearNot applicableCAssessed willingness to take part in hypothetical studies by risk and reward; did not provide recruitment rates (126 participants); there was a statistically significant increase in willingness to participate as risk of adverse effects reduced (p<0.001), payment level rose (p<0.001), and the risk of being assigned to placebo decreased (p=0.02)
B: Variation in trial information on (1) the percentage of patients who would be assigned to placebo (10%, 30%, 50%) and (2) the payment level (payment in range typically offered to participants in phase 3 trials of antihypertensive drugs)Unclear
Harris et al (UK)31FactorialCommunityA: Personal recruitment letter and info plus telephone reminder (up to four) plus questionnaire on physical activityNot applicableHouseholds of older people aged ≥65, able to walk outside and registered with one GP practice69/140 (49.3%)Not applicableABetween-group difference was statistically significant for telephone reminders (OR 1.5; 95% CI 1.0 to 2.3), but not for the inclusion of a questionnaire (OR 0.9; 95% CI 0.6 to 1.3)
B: Personal recruitment letter and info plus telephone reminder (up to four)65/140 (46.4%)
C: Personal recruitment letter and info plus questionnaire on physical activity47/140 (33.6%)
D: Personal recruitment letter and info only59/140 (42.1%)
Hemminki et al (Estonia)32Parallel groupLocal clinics (multicentre)Non-blinded allocation comparing active HRT treatment with no treatmentTraditional blinded allocation comparing active HRT treatment with placeboPostmenopausal women aged 50–641027/2159 (47.6%)796/2136 (37.3%)ABetween-group difference was statistically significant (p<0.001)
Hutchison et al (UK)33Parallel groupSecondary careVideo giving generic and site-specific trial info with a focus on randomisation, pictures of patients receiving care and a voiceover discussing uncertainty plus standard practiceStandard practice of clinician from tumour site team discussing trial and administering trial specific info sheet and consent form; at next visit patient sees a clinician from the same team to decide on treatment and whether it will be part of a trialPatients with colorectal, breast or lung cancer, and eligible for a cancer treatment trial62/86 (72.1%)66/87 (75.9%)AConsidered recruitment to a range of cancer trials; between-group difference was not statistically significant (p=0.661)
Ives et al (UK)34Parallel groupSecondary careStandard trial information plus booklet entitled, Clinical Trials in HIV and AIDS: Information for people who are thinking about joining a trial”Standard trial information (information sheet specific to proposed trial plus discussion with trial doctor and research nurse)Patients attending an HIV hospital clinic15/23 (65.2%)11/27 (40.7%)CConsidered recruitment of patients eligible for participation in eight trials being carried out at the participating institution; no information on statistical significance given
Jeste et al (USA)35Parallel groupSecondary careMultimedia consent with DVD presenting key information from consent form, including simultaneous narrative explanation; researcher also present to answer questionsRoutine consent procedure plus 10 min control DVD giving general information about research; researcher also present to answer questionsOutpatients aged >40 with schizophrenia, and healthy comparison subjects41/62 (66.1%) patients with schizophrenia; 23/31 (74.2%) healthy comparisons44/66 (67.2%) patients with schizophrenia; 22/29 (75.9%) healthy comparisonsBStudied agreement to participate in a hypothetical trial; between-group differences were not statistically significant (no p value provided)
Karunaratne et al (Australia)36Parallel groupSecondary careComputer-based, interactive presentation of study information inc. diagrams, video clips, hyperlinks, quiz pagesConventional paper-based study informationPatients aged 18–70 attending an outpatient diabetic clinic23/30 (76.7%)17/30 (56.7%)CConsidered participant understanding of consent materials, including interest in participating in a hypothetical trial; between-group difference was statistically significant (p=0.01)
Kendrick et al (UK)37Parallel groupPrimary care (multicentre)Mailed invitation to participate in an injury prevention trial, including a home safety questionnaireMailed invitation to participate excluding home safety questionnaireFamilies with children aged<5 years, living in deprived areas217/1203 (18.0%)157/1190 (13.2%)ABetween-group difference was statistically significant (p=0.001)
Kerr et al (UK)38Parallel groupFurther education colleges (multicentre, n=5)A: Leaflet describing a trial of two treatments for arthritis, where A and B are described as standard treatmentsNot applicableStudents aged ≥18 enrolled on further education/leisure courses24/29 (82.8%)Not applicableCStudied willingness to participate in a hypothetical trial; did not provide recruitment rates (130 participants); between-group difference was statistically significant (p<0.001), with those who had a preference for a standard treatment—available outside of the trial—less willing to participate than those with no preference
B: Leaflet describing a trial of two treatments for arthritis, where A is described as new treatment and B as standard treatment10/17 (58.8%)
C: Leaflet describing a trial of two treatments for arthritis, where B is described as new treatment and A as standard treatment13/16 (81.3%)
D: Leaflet describing a trial of two treatments for back pain, where A and B are described as standard treatments26/31 (83.9%)
E: Leaflet describing a trial of two treatments for back pain, where A is described as new treatment and B as standard treatment10/15 (66.7%)
F: Leaflet describing a trial of two treatments for back pain, where B is described as new treatment and A as standard treatment10/16 (62.5%)
Kimmick et al (USA)39ClusterSecondary care and academic institutions (multicentre, n=126)Educational intervention of standard info plus an educational symposium, geriatric oncology educational materials, monthly mailings and emails for 1 year, lists of available protocols for use on patient charts, case discussion seminarStandard information of periodic notification of all existing CALGB (Cancer and Leukaemia Group B) trials by the CALGB Central Office, and CALGB web site accessPractitioners and researchers from CALGB institutions36% in year 1; 31% in year 232% in year 1; 31% in year 2CConsidered recruitment of older people to existing CALGB treatment trials for a range of cancers; between-group difference was not statistically significant at year 1 (p=0.35) or at year 2 (p=0.83)
Larkey et al (USA)40Parallel groupExisting trial sites (multicentre, n=2)A: Hispanic lay advocates; attended 6 h long training sessions, five quarterly meetings and received brochures with interest cards to distribute to other womenAnglo women controls, received quarterly ‘phone calls and brochures with interest cards to distribute to other womenParticipants in the Women's Health Initiative trial13/31 referrals (41.9%)2/19 referrals (10.5%)BDetermined whether Hispanic women already enrolled in a study and trained as lay advocates would refer/enrol more participants than untrained Hispanic women and Anglo controls; between-group difference was statistically significant (p<0.01)
B: Hispanic women controls, received quarterly ‘phone calls and brochures with interest cards to distribute to other women0/3 referrals (0.0%)
Liénard et al (France)41ClusterSecondary care (multicentre, n=135)Site visits including an initiation visit to review trial protocol, inclusion/exclusion criteria, safety, randomisation, etc plus ongoing review visitsNo site visits (unless requested)Centres recruiting to an RCT for breast cancer302271ANo denominator data provided; between-group difference was not statistically significant (no p value provided)
Litchfield et al (UK)42ClusterPrimary care (multicentre, n=28)Internet-based collection of trial dataPaper-based collection of trial data28 participating GP practices45/52 (86.5%)28/28 (100%)BConsidered efficiency and ease of use of internet versus conventional paper-based data capture, and looked at recruitment incidentally; between-group difference was statistically significant (p=0.04)
Llewellyn-Thomas et al (Canada)43Parallel groupSecondary careA: Booklet with negatively framed intervention about treatment side-effects and survivalBooklet with neutrally framed intervention about treatment side-effects and survivalColorectal cancer patients attending cancer hospital outpatients20/30 (66.7%)23/30 (76.7%)BDetermined the impact of probabilistic info on entry to a hypothetical trial; between-group difference was not statistically significant (p>0.40)
B: Booklet with positively framed intervention about treatment side-effects and survival18/30 (60.0%)
Llewellyn-Thomas et al (Canada)44Parallel groupSecondary careSearchable computerised info on imaginary trial, including purpose, description of treatment arm and randomisation, possible benefits, side-effects, patients’ rightsTape-recorded info on imaginary trial, including purpose, description of treatment arm and randomisation, possible benefits, side-effects, patients’ rightsPatients attending the outpatient department of a cancer hospital31/50 (62.0%)21/50 (42.0%)BStudied recruitment to a hypothetical trial; between-group difference was statistically significant (p<0.05, unadjusted)
Mandelblatt et al (USA)45Parallel groupCommunity (multicentre, n=3)5–10 min educational counselling session about the trial delivered by non-physician study staff (inc benefits and risk of participation and need for minority participation) plus an informational brochureInformational brochure onlySpanish speaking women who were eligible for a trial on women at high risk of breast cancer178/232 (76.7%) general intent;118/232 (50.9%) if mild side-effects mentioned;108/232 (46.6%) if uterine cancer mentioned147/218 (67.4%) general intent;118/218 (54.1%) if mild side-effects mentioned;97/218 (44.5%) if uterine cancer mentionedCResults relate to intention to participate (‘might, probably or definitely would’); between-group difference was statistically significant for general intention to participate (p=0.03)
Miller et al (USA)46Parallel groupSecondary care, primary care and communityEligibility screening and recruitment by a senior investigatorEligibility screening and recruitment by a Research AssistantPatients aged 18–75, eligible for participation in two chronic depression treatment trials28/162 (17.3%)22/185 (11.9%)CConsidered the relationship between interviewer experience and positive predictive value and cost of telephone screening, and looked at recruitment incidentally; between-group difference was not statistically significant (p=0.30)
Monaghan et al (Worldwide)47ClusterExisting trial sites (multi-centre, n=167)Additional communication—usual plus frequent emails, regular personalised mail-outs of league tables/graphs of performance against other sites, certificates of achievement for recruitment/other study items (1/month)Usual communication (provided via the regional centre) plus occasional direct communications from the co-ordinating centre in the form of generic newsletters, emails and faxesClinical sites in 19 countries recruiting to a diabetes and vascular disease treatment trial37.5 (27.0–51.5)37.0 (21.0–54.5)AResult provided as median number of participants recruited; between-group difference was not statistically significant (p=0.68)
Myles et al (Australia)48Parallel groupSecondary careA: Prerandomised to experimental drug and asked to provide consent; if no consent, standard treatment givenStandard randomisation method (equal chance of either drug)Inpatients aged ≥18, scheduled for elective surgery90/169 (53.3%)84/151 (55.6%)BConsidered recruitment to a hypothetical trial; between-group difference was not statistically significant (p=0.66)
B: Prerandomised to standard drug and asked to provide consent; if no consent, experimental treatment given79/149 (53.0%)
C: Told that physician thinks experimental drug superior, if consent given, has 70% chance of receiving this; if no consent, standard treatment given91/150 (60.7%)
D: Allowed to increase or decrease chance of receiving experimental drug if consent given, and if no preference, 50% chance of receiving it; if no consent, standard treatment given85/150 (56.7%)
Nystuen and Hagen (Norway)49Parallel groupCommunity (multicentre, n=6)Written invitation to participate in a community-based trial followed by a ‘phone reminder if no response within 2 weeks; guide used for discussionWritten invitation to participate in a community-based trial followed by no reminder if no response within 2 weeksSick-listed employees attending a participating social security office31/256 (12.1%)11/242 (4.5%)ABetween-group difference was statistically significant (p=0.003)
Perrone et al (Italy)50Parallel groupCommunityA: randomised consent to new treatment; if no consent given standard treatmentOn consent to participate, standard or new treatment assigned at random; if no consent, given standard treatmentMembers of the general public aged 16–80, attending a scientific exhibition997/1151 (86.6%)836/985 (84.9%)CStudied recruitment to a hypothetical trial; between-group difference was significant for both the single (p=0.08) and double consent scenarios (p<0.0001)
B: randomised consent to standard treatment; if no consent given new treatment246/474 (51.9%)
C: if consents to participate, standard or new treatment assigned at random; if no consent, can choose standard or new treatment482/607 (79.4%)
Pighills et al (UK)51Parallel groupPrimary care (multicentre)A: Newspaper article about the trial included with recruitment materialsUsual recruitment materials onlyMen and women aged ≥70 who had at least one fall in the previous 12 months73/2243 (3.3%)71/2245 (3.2%)BEvaluated interventions in separate trials; between-group differences were not statistically significant (p=0.80; p=0.62)
B: Inclusion of a more ‘upbeat’ newspaper article about the trialInclusion of the Intervention A newspaper article57/1374 (4.1%)54/1371 (3.9%)
Simel and Feussner (USA)52Parallel groupSecondary careConsent form including a statement that the new treatment may work twice as fast as usual treatmentConsent form including a statement that the new treatment may work half as fast as usual treatmentPatients attending an ambulatory care clinic35/52 (67.3)20/48 (41.7%)BConsidered recruitment to a hypothetical trial; between-group difference was statistically significant (p<0.01)
Simes et al (Australia)53Parallel groupSecondary careIndividual approach to consent—patients given info about aims, expected results, potential toxicities of treatment; details of treatment left to discretion of consultant; patients given opportunity to ask questions, verbal consent obtainedTotal disclosure approach—patients fully informed about all trial aspects by consultant: patients given opportunity to ask questions, also given a consent form outlining the info; this was kept overnight and written consent obtained next dayPatients attending an oncology unit27/29 (93.1%)23/28 (82.1%)AConsidered recruitment of patients eligible for 16 trials being carried out at the participating institution; between-group difference was statistically significant (p=0.01)
Treschan et al (Austria)54 Parallel groupSecondary careA: Info on study of wound healing said to have no risk but involving additional procedures described as provoking considerable pain and discomfortInfo on study of wound healing described as posing essentially no risk and producing no significant painPatients aged 19–80, and scheduled for minor surgery with general anaesthesia 18/51 (35%) 30/47 (64%) BStudied willingness to participate in a hypothetical trial, although patients were not aware of this until after the decision to take part; between-group difference was statistically significant (p<0.001)
B: Info on study of wound healing said to have no pain but involving additional procedures described as inducing risk of injury13/50 (26%)
Trevena et al (Australia)55Sequential startPrimary careOpt-out recruitment; letter from doctor advising that practice taking part in screening trial; would be contacted unless practice advised to withhold contact detailsOpt-in recruitment; letter from doctor advising that practice taking part in screening trial; would only be contacted if contact details returnedPatients aged 50–74 eligible for a colorectal cancer screening trial40/60 (66.7%)44/92 (47.8%)ACompared the effect of opt-in requirements in new privacy laws with an opt-out approach that was previously permissible; no information on statistical significance given
Wadland et al (USA)56Parallel groupPrimary careConsent form read out to potential participants by study co-ordinatorConsent form read by potential participantsCurrent smokers aged ≥1827/51 (53%)25/53 (47%)CSmoking cessation study carried out in two practices, with the intervention evaluated in one; between-group differences were not statistically significant (no p value provided)
Weinfurt et al (USA)57Parallel groupSecondary careA: Consent documents containing a disclosure indicating that the clinic received per capita payments covering the costs of the research (including investigator's salary)Consent documents containing no financial disclosurePatients of a cardiovascular outpatient clinic aged ≥18, and diagnosed with coronary artery disease3.51 (SD 1.30)3.50 (SD 1.29)CStudied willingness to participate in a hypothetical trial; did not provide recruitment rates (470 participants); results provided as mean willingness scores; between-group difference was statistically significant (p=0.02); patients in the equity group were also less willing to participate than those in the per capita (p=0.01) and no disclosure groups (p=0.03)
B: Consent documents containing a disclosure describing an investment by the investigator in the company sponsoring the research (‘equity’)3.20 (SD 1.32)
Weinfurt et al (USA)58Parallel groupCommunityA: Info inc a general disclosure that the investigator may gain financially from the study plus a statement that ethics committee does not think this affects patient safety or study qualityNot applicableAged ≥18 with asthma or diabetes and a member of a panel of adults who agreed to be contacted about research opportunities3.28 (SD 0.04)Not applicableCStudied willingness to participate in a hypothetical trial; did not provide recruitment rates (3623 participants); results provided as mean willingness scores; between-group difference was statistically significant (p<0.001)
B: Info inc a disclosure that the drug company pays running costs to the investigator plus a statement that ethics committee does not think this affects safety or quality3.46 (SD 0.04)
C: Info inc a disclosure that the drug company pays monies out with the study to the investigator plus a statement that ethics committee does not think this affects safety or quality3.22 (SD 0.04)
D: Info inc a disclosure that the investigator has an investment in the drug company plus a statement that ethics committee does not think this affects safety or quality3.16 (SD 0.04)
E: Info inc a disclosure that the investigator's institution has an investment in the drug company plus a statement that ethics committee does not think this affects safety or quality3.28 (SD 0.04)
Welton et al (UK)59Parallel groupPrimary care (multicentre, n=10)Verbal info about a trial of HRT, comparing oestrogen only, with combined oestrogen and progestogen, with placeboVerbal info about a trial of HRT, comparing oestrogen only with combined oestrogen and progestogenWomen aged 45–64 who had not had a hysterectomy65/218 (29.8%)85/218 (39.0%)CConsidered willingness to take part in a hypothetical trial; between-group difference was not statistically significant (p=0.06)
Weston et al (Canada)60Parallel groupSecondary care (multicentre)Written study information followed by viewing of Term Prelabour Rupture of the Membranes (Term PROM) videoWritten study information onlyWomen attending for antenatal visits26/42 (61.9%) initially; 23/41 (56.1%) at 2–4 weeks17/48 (35.4%) initially; 17/44 (38.6%) at 2–4 weeksBBetween-group difference was statistically significant (p=0.01)

  • *Risk of bias: A, low; B, moderate; C, high.

  • †Includes difference in outcomes as reported by the authors.

  • RCT, randomised controlled trial.