Effects of different regimens to lower blood pressure on major cardiovascular events in older and younger adults: meta-analysis of randomised trials

doi:10.1136/bmj.39548.738368.BE

BMJ 2008;336:1121-1123 (17 May), doi:10.1136/bmj.39548.738368.BE (published 14 May 2008)

Research

Effects of different regimens to lower blood pressure on major cardiovascular events in older and younger adults: meta-analysis of randomised trials

Blood Pressure Lowering Treatment Trialists’ Collaboration

Correspondence to: F Turnbull, Blood Pressure Lowering Treatment Trialists’ Collaboration, George Institute for International Health, University of Sydney, PO Box M201, Sydney, NSW 2050, Australia fturnbull{at}george.org.au

Abstract

Objective To quantify the relative risk reductions achievedwith different regimens to lower blood pressure in younger andolder adults.

Design Meta-analyses and meta-regression analyses used to comparethe effects on the primary outcome between two age groups (<65v $≥$ 65 years). Evidence for an interaction between age and theeffects of treatment sought by fitting age as a continuous variableand estimating overall effects across trials.

Main outcome measures Primary outcome: total major cardiovascularevents.

Results 31 trials, with 190 606 participants, were included.The meta-analyses showed no clear difference between age groupsin the effects of lowering blood pressure or any differencebetween the effects of the drug classes on major cardiovascularevents (all P $≥$ 0.24). Neither was there any significant interactionbetween age and treatment when age was fitted as a continuousvariable (all P>0.09). The meta-regressions also showed nodifference in effects between the two age groups for the outcomeof major cardiovascular events (<65 v $≥$ 65; P=0.38).

Conclusions Reduction of blood pressure produces benefits inyounger (<65 years) and older ( $≥$ 65 years) adults, with nostrong evidence that protection against major vascular eventsafforded by different drug classes varies substantially withage.

Introduction

Observational studies have shown that blood pressure levelsare strongly and directly related to the relative risks of strokeand heart disease¹ but that the strength of the associationdeclines with increasing age.² A recent large overview foundthat for each 20 mm Hg lower usual systolic blood pressure,the risk of stroke was 33% lower in those aged 80-89 but 62%lower in those aged 50-59.³ While many trials with broad entrycriteria for age have investigated the effects of lowering bloodpressure on major vascular events, consistently larger reductionsin relative risk have not been reported for younger participants.This might reflect true comparability of the effects of reducingblood pressure in older and younger people but might also bea consequence of the limited power of the individual trialsto detect differences in effectiveness between age groups. Likewise,there is a paucity of evidence about the effects of differentdrug classes in older compared with younger patients. Some guidelinesadvocate the selective use of particular drug regimens basedon patients’ age,⁴ ⁵ though systematic reviews quantifyingthe comparative effects of regimens on major vascular outcomeshave not been done.

With the global population rapidly ageing⁶ and guidelines recommendingtreatment to lower blood pressure for an increasing proportionof the elderly population, we need clear evidence about theeffects of such treatments in older compared with younger adults.The Blood Pressure Lowering Treatment Trialists’ Collaborationwas established to perform a prespecified series of overviewsof trials investigating the effects of drugs to lower bloodpressure on cardiovascular mortality and morbidity, includingassessments of the comparative effects of regimens between majorsubgroups of patients. We compared the proportionate risk reductionsachieved with different classes of drugs in younger and olderadults.

Methods

Trials included
Trials were eligible for inclusion if they randomised patientsbetween a drug to lower blood pressure and control (placeboor less intensive blood pressure treatment) or randomised patientsbetween regimens based on different classes of drug to lowerblood pressure. Trials had to have a minimum of 1000 patientyears of planned follow-up in each randomised group and mustnot have presented or published their main results before wefinalised our protocol in July 1995.⁷ We included in our analysestrials for which data had been obtained by September 2006. Whena trial included more than two treatment arms, we calculatedestimates of effect for all possible comparisons except whenearly termination of one arm made such estimates impossible.⁸Data were accepted as data on individual patients (25 studies)or as tabular data by using prespecified categories (six studies).The data requested included participants’ characteristicsrecorded at screening or randomisation, selected measurementsmade during follow-up, and details of the occurrence of alloutcomes during the scheduled follow-up period.

Age groups
The age groups predefined in the original overview protocolwere <65 and $≥$ 65 years at the time of entry into the trial,henceforth referred to as "younger" and "older" adults. Thesecut offs were chosen because most participating trials usedthe same categories in their own subgroup analyses.

Outcomes
Our primary outcome was total major cardiovascular events, comprisingstroke (non-fatal stroke or death from cerebrovascular disease),coronary heart disease (non-fatal myocardial infarction or deathfrom coronary heart disease including sudden death) and heartfailure (causing death or resulting in admission to hospital).Secondary outcomes were stroke, coronary heart disease, heartfailure, cardiovascular death, and total mortality. All outcomeswere prespecified in the original study protocol.⁷

Comparisons
The seven comparisons of treatment were those reported in thesecond main cycle of overviews⁹: (a) angiotensin convertingenzyme inhibitor versus placebo, (b) calcium antagonist versusplacebo, (c) more intensive versus less intensive regimens tolower blood pressure, (d) angiotensin receptor blocker versuscontrol regimen, (e) angiotensin converting enzyme inhibitorversus diuretics/β blockers, (f) calcium antagonist versusdiuretics/β blockers, and (g) angiotensin converting enzymeinhibitor versus calcium antagonists. Additional comparisonsexamined the separate effects of diuretics and β blockersin different age groups as some recent guidelines have madespecific recommendations about the use of these treatments inolder and younger adults.⁴ ⁵ These additional comparisons were(a) angiotensin converting enzyme inhibitor or calcium antagonistversus β blockers and (b) angiotensin converting enzymeinhibitor or calcium antagonist versus diuretics.

Statistical analyses
We calculated the reduction in blood pressure in each trialarm as the mean of the differences between each participant’smean blood pressure during follow-up and their blood pressureat baseline. We then calculated the mean difference in bloodpressure between randomised groups by subtracting the valuesfor the arms compared. Mean levels of baseline characteristicsand the mean difference in blood pressure between randomisedgroups were calculated separately for younger and older adultsfor each trial. Overall estimates were obtained by weightingthe estimates from each individual study in proportion to thenumber of older and younger adults in that study.

We performed three sets of analyses to explore the impact ofage on the proportional risk reduction achieved with loweringblood pressure.

Firstly, we carried out meta-analyses of subgroups of participantsdefined according to age. For each trial and each outcome wecalculated the relative risk and its variance separately foreach of the two age groups according to the principle of intentionto treat. Each participant could contribute only the first eventin any category to the calculation for each outcome but mightcontribute an event to analyses of several outcomes. Overallestimates of effect and 95% confidence intervals were calculatedseparately for each age group by using a random effects modeland inverse variance weighting (that is, weighting by the precisionof the estimate for each age group in each trial). The "meta"routine in STATA (release 9.0; Stata Corporation, College Station,TX, USA) evaluated effects of randomised treatments. Consistencyof treatment effects across the age groups was tested with ${chi}$ ²tests of homogeneity.

Secondly, we investigated interactions between treatment tolower blood pressure and age taken as a continuous variableby fitting Cox’s regression models including treatment,continuous age, and their interaction. The regression ("β")coefficient for the latter term estimates the log ratio of relativerisks, comparing the treatments, where each relative risk isthe effect of a unit (here taken as 10 years) increase in agewith one of the two treatments. Twenty four trials contributingdata on individual participants were included in these analyses,with no comparisons being made for regimens based on angiotensinreceptor blockers because data were available from only onetrial. We pooled the log ratios of relative risks using inversevariance weighted random effects meta-analysis. The pooled summarywas exponentiated to arrive at the overall estimated ratio ofrelative risks for a 10 year difference in age for each outcome.

Thirdly, we carried out meta-regression analyses to explorethe association between the difference in systolic blood pressureat follow-up between randomised groups and the log relativerisk for cardiovascular events in each age group. This was investigatedacross trials with random effects meta-regression models withinverse variance weighting.¹⁰ Analyses were carried out usingthe metareg routine in STATA. We fitted separate regressionlines for each age group and compared the slopes of these linesto test for a differential effect of reduction in blood pressureon risk reduction between age groups for each outcome. The modelincluded an interaction term between age group and systolicblood pressure.¹⁰ Assumptions of linear associations betweendifferences in blood pressure at follow-up and log relativerisks were tested with standard graphical methods. As trialparticipants could contribute only once to a given meta-regressionanalysis, for factorial trials that included randomisation todifferent intensities of blood pressure lowering and randomisationto different drug treatments^w1-w5 we included only the resultsof the randomisation to different intensities of blood pressurelowering. For similar reasons, trials with randomisation tothree treatment arms^w6-w8 contributed results from only twoof the possible three treatment comparisons, with the controlarm participants divided between the two comparisons. We carriedout sensitivity analyses to examine the impact of removing thethree trials that contributed participants’ data exclusivelyto older age groups ( $≥$ 65 years)^{w7 w9 w10} and the impact of removingthe six trials for which data on individual participants werenot available.^{w1 w9 w11-w14} In every analysis P<0.05 indicatedthat a result was possibly not due to chance, although eachcase required careful interpretation, given the large numbersof comparisons.

Results

Characteristics of trials and patients included
Of the 37 eligible trials,^w1-w38 we included 31 (190 606 individuals)in these analyses (see table A on bmj.com). For the six remainingtrials^w33-w38 we could not extract data according to criteriaspecified in the original study protocol.⁷ There were 96 466individuals aged <65 and 94 140 aged $≥$ 65 at baseline who contributedto the primary analyses (table 1).

The mean age in the two groupswas 57 and 72 and the proportion of men was 58% and 51%, respectively.Mean baseline blood pressure was higher in the older age groups,as was the proportion of primary outcome events that comprisedstroke (table 2).

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Table 1 Mean baseline characteristics and differences in blood pressure at follow-up between randomised groups in subgroups of younger and older adults

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Table 2 Numbers (percentages) of individuals with stroke, coronary heart disease, and heart failure by age

Meta-analyses of effects of treatments in different age groups
For the primary outcome, total major cardiovascular events,in the trials that examined blood pressure lowering regimenscompared with placebo or less active control, there was no evidenceof any difference in reductions in relative risk in differentage groups (all P>0.2 for heterogeneity) (fig 1).

Likewise,in the overviews of trials comparing blood pressure loweringregimens based on different drug classes there was no differencein the proportional reductions in total major cardiovascularevents observed between age groups for any comparison (all P>0.3for heterogeneity) (figs 2 and 3).

While there was some variationin the reductions in blood pressure with the randomised treatmentsbetween age groups, there was no systematic pattern. Among the35 comparisons between age groups made for the secondary outcomesthere were two with P $≤$ 0.05 (www.thegeorgeinstitute.org/bplttc),and these are likely to have arisen by chance. Sensitivity analysesin which we excluded the three trials^{w7 w9 w10} that contributedpatients to only one age group ( $≥$ 65 years) from the meta-analysesdid not make any material difference to the findings. Similarly,there was no difference in the findings when we repeated theanalyses on the subset of 25 trials for which data on individualparticipants were available.

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Fig 1 Comparison of blood pressure lowering regimens against placebo or less intensive control. SBP/DBP difference=overall difference in mean blood pressure during follow-up between treatment groups (actively treated group versus control group), calculated by weighting difference observed in each contributing trial by number of individuals in trial. Negative blood pressure values indicate lower mean follow-up blood pressure in first listed than in second listed groups

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Fig 2 Comparison of angiotensin receptor blocker based regimens with control regimens. SBP/DBP difference=overall difference in mean blood pressure during follow-up between treatment groups (angiotensin receptor blocker treated group versus control group), calculated by weighting difference observed in each contributing trial by number of individuals in trial. Negative blood pressure values indicate lower mean follow-up blood pressure in first listed than in second listed groups

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Fig 3 Blood pressure lowering regimens based on different drug classes for the outcome total major cardiovascular events and age groups <65 versus $≥$ 65. SBP/DBP difference=overall difference in mean blood pressure during follow-up between treatment groups (group assigned first listed treatment versus group assigned second listed treatment), calculated by weighting difference observed in each contributing trial by number of individuals in trial. Negative blood pressure values indicate lower mean follow-up blood pressure in first listed than in second listed groups

We used data from eight trials^{w1 w5 w6 w10 w27-w29 w31} in subsidiaryanalyses to examine the separate effects of regimens based onβ blockers and on diuretics compared with other drug classes(angiotensin converting enzyme inhibitors and calcium antagonistcombined) according to patients’ age. In these analyses,there was no evidence of a difference in the proportional riskreduction for major cardiovascular events between younger andolder adults for either comparison (all P>0.3) (fig 4).

Weconducted similar subsidiary analyses to examine the effectsof including eligible trials for which only published data wereavailable.^{w36 w38} In these analyses, there was no evidence ofdifference between treatment regimens according to patients’age (all P>0.22).

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Fig 4 Regimens based on diuretics and β blockers versus other active agents for total major cardiovascular events according to age. SBP/DBP difference=overall difference in mean blood pressure during follow-up between group assigned first listed treatment versus group assigned diuretic or β blocker, calculated by weighting difference observed in each contributing trial by number of individuals in trial. Negative blood pressure values indicate lower mean follow-up blood pressure in first listed than in second listed groups

Effects of age on blood pressure lowering with age fitted as continuous variable
We found no evidence of an interaction between age and the effectsof treatment on the primary outcome of major cardiovascularevents for any blood pressure lowering treatments compared withcontrol (all P>0.09) (fig 5).

The same was true for the comparisonsof different active agents (all P>0.2). For the secondaryoutcomes there was one significant interaction (P=0.02) amongthe 30 analyses, and this is most likely to have arisen by chance(www.thegeorgeinstitute.org/bplttc).

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Fig 5 Proportionate increase in relative risk of major cardiovascular events, first listed v second listed, for every extra 10 years of age

Meta-regressions of effects of blood pressure lowering in different age groups
There was no difference in the risk reduction achieved per unitreduction in blood pressure for individuals aged <65 comparedwith $≥$ 65 for the primary outcome of total major cardiovascularevents (P=0.38) (fig 6)

nor for any of the secondary outcomes(all P $≥$ 0.18) (available from author (www.thegeorgeinstitute.org/bplttc).

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Fig 6 Associations of reduction in blood pressure with risk reduction for total major cardiovascular events for adults aged <65 and $≥$ 65. Area of each circle is proportional to inverse variance of log odds ratio. Fitted lines represent summary meta-regressions for total major cardiovascular events

Discussion

Principal findings
These analyses provide strong support for the use of drugs tolower blood pressure in older and younger adults, with no strongevidence for the selective use of specific classes of drug accordingto age. While some current management guidelines advocate theuse of particular types of drug according to age on the basisof possible differences in effects on major cardiovascular events,⁴⁵ ¹¹ factors such as tolerability and cost are probably reasonablebases for choice of drug so long as effective blood pressurereduction is achieved.¹² ¹³ ¹⁴ In particular, for these agegroups there was no evidence of differences between the effectsof β blockers and other classes of drugs in older comparedwith younger adults for any outcome studied, and the same wastrue for all other drug comparisons.

Findings in context of observational studies
We might expect variation in the effect of lowering blood pressurebecause observational data have shown less strong proportionalassociations of blood pressure levels with risk in older comparedwith younger adults.³ The analyses prespecified in the originaloverview protocol⁷ identified no attenuation of risk reductionwith age but were not especially well powered to detect sucheffects. Each of the subsidiary analyses provided better statisticalpower, and there were some comparisons that showed evidenceof different effects of blood pressure lowering between agegroups or interactions between age and particular drug regimens.It is important, however, that the "statistically significant"subsidiary analyses are interpreted in light of their post hocnature, the multiple comparisons made, and, in the case of themeta-regressions, the non-randomised nature of the evaluations.So, our results do not completely exclude the possibility ofdifferences in the proportional effects of blood pressure loweringregimens between age groups but they do suggest that any suchdifferences are likely to be small.

Clinical implications
As the magnitude of the proportional risk reduction achievedwith blood pressure lowering does not seem to decline with age,our findings provide strong support for the use of blood pressurelowering in elderly people. Among the older age group therewas, in almost every analysis and for almost every outcome,an estimate of effect suggesting benefit from blood pressurelowering, and in no case was there evidence of harm. The muchgreater absolute risk in elderly people means that even if proportionalreductions were attenuated in this group, the protection affordedwould still translate into large numbers of serious vascularevents prevented. These data also provide considerable reassurancethat current approaches to the use of blood pressure loweringtreatments based on absolute risk, that assume constant proportionalrisk reductions across age groups,⁵ ¹¹ ¹² ¹³ ¹⁴ are an appropriatemeans of quantifying the likely absolute benefit to be gainedfrom lowering blood pressure.³

Strengths and weaknesses
Our analyses included thousands of major cardiovascular eventsand provided reasonably precise estimates of the effects ofthe different regimens in older and younger adults for mostoutcomes. They are, however, subject to several limitationsand need to be interpreted with these in mind. Firstly, thedifference in mean age between the older and younger participantswas not large—only about 15 years. The observational datasuggest that proportional differences in risk reduction wouldbe modest for age differences of this magnitude, and it is possiblethat these overviews could have failed to detect real differencesin the effectiveness of blood pressure lowering between agegroups. That said, the analyses with age fitted as a continuousvariable had much better statistical power to detect interactionsbetween age and treatment to lower blood pressure and providereassurance that moderate or large effects have not been missed.Secondly, because most patients in the trials fell within afairly limited age range, the analyses were unable to definethe effects of blood pressure lowering agents in very elderlypeople. Although particular concerns about the safety and efficacyof treatment to lower blood pressure in this group have previouslybeen raised,¹⁵ recent results from the HYVET study¹⁶ have largelyaddressed uncertainty around the benefits of lowering bloodpressure in patients aged $≥$ 80. In the same way that the limitedage range of patients in our analyses could not define the effectsin the very elderly, postulated differences between the effectsof drug regimens in younger age groups¹⁷ cannot be excluded.Thirdly, although there was reasonable comparability in thebaseline characteristics of younger and older patients it ispossible that different levels of baseline blood pressure, theproportion of men, and possibly other comorbidities might havehad an effect on the potential to detect differences betweenthe age groups. Fourthly, the overviews defined only the shortto medium term effects of the regimens studied and cannot excludethe evolution of differences between the effects in each agegroup in the longer term. Fifthly, the ability of these analysesto detect differences between regimens would have been diminishedby incomplete adherence to randomised treatments and the extensiveuse of add-on therapies. Similarly, the a priori definitionof a "conventional group" that combines two different drug classes(diuretics and β blockers) represents an additional challenge,although subsidiary analyses were not able to detect differenceswhen β blockers and diuretics were considered separately.Sixthly, data defined by the prespecified criteria were notavailable for all eligible trials, but limited subsidiary analysesincluding published data from those studies did not change theoverall study conclusions.

Finally, the primary analyses were based on the composite outcomeof major cardiovascular events, and this outcome might underestimateany real difference in the proportional effects of blood pressurelowering between age groups. The reason for this is that thecomposition of major cardiovascular events varies between agegroups, with the proportion of strokes, which are more stronglyaffected by lowering blood pressure, being larger in the olderage groups. This would tend to inflate the magnitude of theproportional reduction achieved for major cardiovascular eventsin the older compared with the younger group. The secondaryanalyses of the separate major cause-specific outcomes do not,however, suggest that this has been a major cause of confounding.

Conclusions
Our results confirm the benefits of effective control of bloodpressure in older and younger adults. They also provide substantialreassurance that, within the age range studied, the benefitsof regimens to lower blood pressure based on different drugclasses are largely comparable across age groups, although thereis a relative paucity of data for those under 50 and over 80.None the less, these findings should greatly simplify decisionmaking for millions of clinicians around the world.

What is already known on this topic

In observational studiesthe proportional reductions in the risks of vascular diseaseassociated with lower blood pressure levels decline with increasingage, suggesting that the relative effects of blood pressurelowering drugs might be smaller among elderly people

Some bloodpressure management guidelines recommend specific classes ofblood pressure lowering treatment for particular age groups

Whatthis study adds

Blood pressure reduction produces similar proportionalreductions in the risks of vascular events in younger (<65years) and older ( $≥$ 65 years) adults

The absolute benefits oftreatment are likely to be particularly large among older individualsbecause of their higher average risk

There was no clear evidenceto support recommendations for particular drug classes in olderor younger adults

Members of the Blood Pressure Lowering Treatment Trialists’Collaboration: L Agodoa (National Institute of Diabetes andDigestive and Kidney Diseases, National Institutes of Health,Bethesda, Maryland, US); C Anderson, J Chalmers, S MacMahon,B Neal (George Institute, Sydney, Australia); F W Asselbergs,W H van Gilst (University of Groningen, Groningen, Netherlands);C Baigent, R Collins (Clinical Trial Service Unit, Universityof Oxford); H Black (New York University School of Medicine,New York, US); B Brenner, M Pfeffer (Brigham and Women’sHospital, Boston, US); C Bulpitt, P Poole-Wilson (Imperial College,London); R Byington (Wake Forest University, Winston-Salem,US); J Cutler (National Heart, Lung and Blood Institute, Bethesda,US); B Davis (University of Texas School of Public Health, Houston,US); D de Zeeuw (University Medical Center Groningen, Groningen,Netherlands); J Dens (University Hospital Gasthuisberg, Leuven,Belgium); R Estacio (University of Colorado Health SciencesCenter, Denver, US); R Fagard (University of Leuven, K U Leuven,Belgium); K Fox (Royal Brompton Hospital and Imperial College,London); T Fukui (St Luke’s International Hospital, Tokyo,Japan); L Hansson (deceased), R Holman (Oxford Centre for Diabetes,Endocrinology and Metabolism, University of Oxford); Y Imai,T Ohkubo (Tohoku University Graduate School of PharmaceuticalSciences and Medicine, Sendai, Japan); M Ishii (Yokohama Seamen’sInsurance Hospital, Yokohama, Japan); Y Kanno, H Suzuki (SaitamaMedical University, Saitama, Japan); J Kostis (UMDNJ-RobertWood Johnson Medical School, New Brunswick, US); K Kuramoto(Tokyo Metropolitian Geriatric Hospital, Tokyo, Japan); E Lewis(Rush University Medical Center, Chicago, US); M Lièvre(Louis Pradel Hospital Université Claude Bernard-Lyon1, Lyon, France); L H Lindholm (Department of Public Healthand Clinical Medicine, Umeå University, Sweden); L Liu(Fu Wai Hospital and Cardiovascular Institute, Beijing, China);J Lubsen (SOCAR Research S.A, Nyon, Switzerland); S Lueders,J Schrader (St Josefs Hospital, Cloppenburg, Germany); E Malacco(Ospedale L. Sacco, University of Milan, Italy); G Mancia (Universityof Milano-Bicocca, Department of Clinical Medicine and Prevention,San Gerardo Hospital, Milan, Italy); M Matsuzaki (YamaguchiUniversity Hospital, Yamaguchi, Japan); S Nissen (ClevelandClinic, Cleveland, US); T Ogihara (Osaka University GraduateSchool of Medicine, Osaka, Japan); C Pepine (University of Florida,Gainsville, US); B Pitt (University of Michigan School of Medicine,Ann Arbor, US); M Rahman (University Hospitals of ClevelandCase Medical Center, Cleveland, US); W Remme (Sticares CardiovascularResearch Institute, Rhoon, Netherlands); G Remuzzi, P Ruggenenti(Mario Negri Institute for Pharmacological Research and OspedaliRiuniti di Bergamo, Bergamo, Italy); A Rodgers (Clinical TrialsResearch Unit, University of Auckland, New Zealand); T Saruta(Keio University School of Medicine, Tokyo, Japan);, R Schrier(University of Colorado School of Medicine, Denver, US); P Sleight(University of Oxford and John Radcliffe Hospital, Oxford);J Staessen (University of Leuven, Leuven, Belgium); K Teo (McMasterUniversity Medical Centre, Ontario, Canada); G Viberti (King’sCollege London, Guy’s Hospital, London); J Wang (RuijinHospital, Shanghai, China); P Whelton (Loyola University MedicalCenter, Maywood, US); L Wing (Flinders University, Adelaide,Australia); Y Yui (Kyoto University Hospital, Kyoto, Japan);S Yusuf (Hamilton General Hospital, Ontario, Canada); A Zanchetti(University of Milan and Instituto Auxologico Italiano, Milan,Italy).

Collaboration Coordinating Centre (George Institute for InternationalHealth, Sydney, Australia): F Barzi, J Chalmers, S Heritier,N Li, S MacMahon, B Neal, T Ninomiya, V Perkovic, F Turnbull,M Woodward.

Writing committee: F Turnbull, B Neal, T Ninomiya, C Algert,H Arima, F Barzi, C Bulpitt, J Chalmers, R Fagard, A Gleason,S Heritier, N Li, V Perkovic, M Woodward, S MacMahon.

Contributors: FT is guarantor.

Funding: National Health and Medical Research Council of Australia.B Neal was supported by a fellowship awarded by the NationalHeart Foundation of Australia. T Ninomiya was supported by afellowship awarded by the Banyu Life Science Foundation andby an International Society of Hypertension visiting postdoctoralfellowship awarded by the Foundation for High Blood PressureResearch Council of Australia. V Perkovic was supported by apostdoctoral fellowship awarded by the National Heart Foundationof Australia.

Competing interests: Of the members of the writing committee, FT, BN, TN, HA, CB, JC, VP, MW, and SM have received travelexpenses, payment for speaking at meetings, or research fundingfrom one or more agencies that sponsored trials included inthis collaboration.

Ethical approval: Not required.

Provenance and peer review: Not commissioned; externally peerreviewed.

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(Accepted 4 April 2008)

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Rapid Responses:

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drug choice and efficacy may depend on the aims of treatment: oscar,m jolobe
bmj.com, 17 May 2008 [Full text]
No difference between different antihypertensives in reducing cardiovascular mortality?: Ian KC Fok
bmj.com, 20 May 2008 [Full text]