Title: Second Australian National Blood Pressure Study
1Second Australian National Blood Pressure Study
ANBP2
Conducted by the High Blood Pressure Research
Council of Australia in conjunction with
Australias General Practitioners
2Background
- Treatment of hypertension based on diuretics
and/or beta blockers provides a definite outcome
benefit - Additional benefit beyond that resulting from
blood pressure reduction may result with therapy
based on agents inhibiting the renin-angiotensin
system
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New Engl J Med, 2003348583-92.
3Antihypertensive Drug Use in Australia
4Background
- No outcome data with ACE inhibitor based regimens
- Potential benefits include
- Reduction in LVH
- Improved survival with cardiac failure
- Enhanced insulin sensitivity
- Lipid neutrality
- Will outcome be the same better or worse than
those of published studies?
5Main Aim
- To determine in hypertensive patients aged 65-84
years whether there is any difference in total
cardiovascular events (fatal and non-fatal) over
a 5 year treatment period between treatment with
either a diuretic-based regimen or an ACE
inhibitor-based regimen
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New Engl J Med, 2003348583-92.
6Study Design
- P prospective
- R randomised
- O open label
- B blinded
- E endpoints
- Features
- Intention to treat
- General practice based
- 600 practices
- 6000 patients
- Recruitment 2.5 years
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New Engl J Med, 2003348583-92.
7Study Organisation
ANBP2
8Study Subjects
- Inclusion Criteria
- Men and women 65 - 84 years
- Previously treated or newly diagnosed
hypertensives - Untreated sitting SBP gt 160 and/or DBP gt 90 mmHg
- Able to give consent and to attend GP practice
- No recent cardiovascular morbidity
- Exclusion Criteria
- Any cardiovascular end-point in the past 6 months
- Dementia
- Plasma creatinine gt 0.2 mmol/L
- Any life threatening illness (unlikely to survive
5 years) - Unwillingness of GP to enter subject into study
- Unable to attend GP practice
- Absolute contraindication to ACE or diuretic
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New Engl J Med, 2003348583-92.
9Study Protocol
- Blood Pressure Screening
- 3 visits conducted by Study Nurses
- 3 measurements (average of 2nd and 3rd)
- Mercury sphygmomanometer
- Entry BP - average of 2nd and 3rd visit readings
- Randomisation
- Central - Data Management Centre (Adelaide)
- Stratified for age (gt or ? 75)
- Follow-Up
- GP manages patient according to usual practice
- Conform (where possible) to randomisation arm
- Achieve subject goal BP
- At least 2 visits per year
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10Study Drug Treatments
- ACE Inhibitor Group
- Step 1. ACE Inhibitor (enalapril recommended)
- Step 2. Beta or alpha blocker or calcium
antagonist - Step 3. Drug from class not used in Step 2 or
diuretic - Step 4. Drug from class not used in step 2 or 3
- Diuretic Group
- Step 1. Thiazide type diuretic (low dose)
- Step 2. Beta or alpha blocker or calcium
antagonist - Step 3. Drug from class not used in Step 2
- Step 4. Drug from class not used in step 2 or 3
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11Study End-points
- Obtained by study nurses from GP case notes,
hospital case records and death certificates - End-point Committee (blinded to treatment
allocation) evaluated all data relating to
potential study end-points
- Primary Outcome All cardiovascular events
(initial and subsequent) or death from any cause
total burden of cardiovascular disease - Any first event or death event-free survival
- Cause-specific first events
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New Engl J Med, 2003348583-92.
12End-points
- myocardial infarction (fatal and non-fatal)
- sudden or rapid or other cardiac death
- coronary events resulting in coronary therapeutic
procedures - cardiac failure (fatal or non-fatal)
- stroke (fatal or non-fatal)
- transient cerebral ischaemic attacks
- acute non-coronary or non-cerebral vascular
occlusion - other vascular deaths
- dissecting or ruptured aortic aneurysm
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New Engl J Med, 2003348583-92.
13Data Analysis
- Multivariate proportional hazards (Cox) models
incorporating - Wei-Lin-Weissfeld method for multiple failure
time data - Li-Lagakos application of WLW method to analyse
recurrent event data with a terminating event - Robust variance estimation
- Validation by simulation
- Proportional hazards (Cox) models for
cause-specific first events
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New Engl J Med, 2003348583-92.
14GP Involvement in ANBP2
2681 - GPs 1594 - Practices
500 299
472 224
361 200
390 270
958 601
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15ANBP2 Subject Recruitment
Screened - 54288 Randomised - 6083 Rate
- 11
16Study profile
54288 screened
25805 ineligible 16899 unwilling to
participate 5501 did not meet inclusion criteria
3 yrs
6083 randomised
ACE 3044
Diuretic 3039
ITT analysis
Observation Time Median 4.1
yrs Patient yrs 24702
0 No Vital Status
2
ACE 3044
Diuretic 3037
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Intention to treat
New Engl J Med, 2003348583-92.
17Baseline data
ACE Diuretic (3044) (3039) Male
Female 5050 4852 Age (yr) 72.0 71.9 B
lood Pressure (mmHg) 167 13 168 13
91 8 91 8 Previously Treated 62 62 B
ody Mass Index (kg/m2) 27 4 27 4 Current
Smokers 7 7 Physically Active 78 76
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New Engl J Med, 2003348583-92.
18Baseline data
ACE Diuretic (3044) (3039) Coronary
Heart Disease 8 8 Cerebrovascular
Disease 5 5 Diabetes Mellitus 8 7 Hyper
cholesterolaemia 38 36 - lipid lowering
drugs 13 13
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New Engl J Med, 2003348583-92.
19Drug treatments
At Randomisation At Study End ACE
Diuretic ACE Diuretic (3044) (3039)
(3044) (3039) Allocated Therapy 83
83 58 62 Monotherapy 82 82 65
67 ? 3 agents 6 5 No
drugs 16 15 4 3
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New Engl J Med, 2003348583-92.
20Antihypertensive Medication Use at Study End
- ACE Diuretic
- ACE 58 18
- Beta Blocker 11 14
- Ca Blocker 23 25
- Diuretic 24 62
- Single Drug 65 67
- 2 Drugs 25 25
- 3 Drugs 6 5
Data represent
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New Engl J Med, 2003348583-92.
21In-study blood pressure
-26 mmHg
-12 mmHg
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New Engl J Med, 2003348583-92.
22Primary Result
ACE Diuretic Event n
Rate n Rate HR (95CI) p All
cardiovascular 692 55.8 732 59.5 0.89
(0.79,1.00) 0.05 events or any death First
cardiovascular 490 41.9 529 45.7 0.89
(0.79,1.01) 0.06 event or death Death 195
15.7 210 17.1 0.90 (0.75,1.09) 0.27
Rate per 1000 patient years Adjusted for age,
gender
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New Engl J Med, 2003348583-92.
23Primary Result
Rate per 1000 patient years Adjusted for age,
gender
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24Cause-specific first events
All subjects - first any events
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New Engl J Med, 2003348583-92.
25Cause-specific fatal events
All subjects - fatal events
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New Engl J Med, 2003348583-92.
26Cause-specific non-fatal events
All subjects - first non-fatal events
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New Engl J Med, 2003348583-92.
27Summary
- 11 reduction in total cardiovascular events (or
death from any cause) with ACE inhibitor
treatment - 11 reduction in first events with ACE inhibitor
treatment - 17 reduction in total events in males and no
effect in females
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New Engl J Med, 2003348583-92.
28Summary
- No difference between treatments
- total or cardiovascular mortality
- all cerebrovascular events
- all coronary events
- With ACE inhibitor treatment
- reduction in first non-fatal cardiovascular
events (HR 0.86) - reduction in non-fatal myocardial infarctions
(HR 0.68) - increase in fatal strokes (HR 1.91)
- cause-specific effects only in males
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New Engl J Med, 2003348583-92.
29Conclusion
- Initiation of antihypertensive treatment in older
patients with an ACE inhibitor particularly in
males has a modest but definite outcome advantage
over a diuretic despite a similar reduction in
blood pressure
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New Engl J Med, 2003348583-92.
30Acknowledgments
- Australian Commonwealth Department of Health and
Ageing - National Health and Medical Research Council of
Australia - Study staff
- Australias General Practitioners
- Merck Sharp Dohme (Australia) Pty Ltd
ANBP2
31Acknowledgments
- Prof L. Wing (SA - Chairperson)
- Dr C. Reid (Vic - Study Director)
- Dr P. Ryan (SA - Statistician)
- Prof G. Jennings (Vic)
- Prof J. McNeil (Vic)
- Prof M. Brown (NSW)
- Prof C. Johnston (Vic)
- Prof T. Morgan ( Vic)
- Prof J. Marley (SA)
- Prof L. Beilin (WA)
- Prof M. West (Qld)
- Prof G. MacDonald (NSW)
-
ANBP2 Management Committee
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32Acknowledgments
- Regional Co-ordinating Centres
- Mark Nelson, Anne Bruce, Paul Beckinsale, Jill
Thompson, Marilyn McMurchie, - Glenda Fraser, David Gleave, Vicki Cope, Fred
DeLooze, Sue Moore, - Cathy Dibben, Jonathon Newbury
- Data Management and National Coordinating
Centres - Helen Miles, Brian McDermott, Kristyn Willson,
Carol Bear - Genetic Sub-Committee
- Malcolm West, Stephen Harrap, Colin Johnston,
Lawrie Beilin, Philip Ryan, - Lindon Wing, Christopher Reid
- Ambulatory Blood Pressure Monitoring
Sub-Committee - Lawrie Beilin, Mark Brown, Philip Ryan, Lindon
Wing, Christopher Reid - LVH Sub-Committee
- Garry Jennings, Peter Fletcher, Michael Feneley,
Elizabeth Dewar, Lindon Wing, - Christopher Reid
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33Acknowledgments
- Data Audit Sub-Committee
- John McNeil, Lindon Wing, John Marley,
Christopher Reid - Finance Sub-Committee
- Colin Johnston, Garry Jennings, Lindon Wing,
Christopher Reid - Health Economic/Quality of Life Sub-Committee
- John Marley, John Moss, Penny Webb, Paul
Glasziou, Fran Boyle, John Primrose, - Lindon Wing, Christopher Reid
- GP Advisory Committee Ian Steven, Leon
Piterman, Fred De Looze, - Jim Dickinson, John Gambrill, Peter Joseph,
Christopher Reid - End-point Committee David Hunt, Geoff Donnan,
Lindon Wing, Trefor Morgan - Independent Data Audit Sub-Committee John
Chalmers, - Judith Whitworth, Stephen MacMahon, Chris Silagy
(Decd)
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